Re: 요산의 항산화 기능, 고요산 혈증과 관련된 질환들..... 2024 nature

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Hyperuricemia and its related diseases: mechanisms and advances in therapy

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• Review Article
• Open access
• Published: 28 August 2024

Hyperuricemia and its related diseases: mechanisms and advances in therapy

• Lin Du, 
• Yao Zong, 
• Haorui Li, 
• Qiyue Wang, 
• Lei Xie, 
• Bo Yang, 
• Yidan Pang, 
• Changqing Zhang, 
• Zhigang Zhong & 
• Junjie Gao 

Signal Transduction and Targeted Therapy volume 9, Article number: 212 (2024) Cite this article

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Abstract

Hyperuricemia, characterized by elevated levels of serum uric acid (SUA), is linked to a spectrum of commodities such as gout, cardiovascular diseases, renal disorders, metabolic syndrome, and diabetes, etc. Significantly impairing the quality of life for those affected, the preval‎ence of hyperuricemia is an upward trend globally, especially in most developed countries. UA possesses a multifaceted role, such as antioxidant, pro-oxidative, pro-inflammatory, nitric oxide modulating, anti-aging, and immune effects, which are significant in both physiological and pathological contexts. The equilibrium of circulating urate levels hinges on the interplay between production and excretion, a delicate balance orchestrated by urate transporter functions across various epithelial tissues and cell types. While existing research has identified hyperuricemia involvement in numerous biological processes and signaling pathways, the precise mechanisms connecting elevated UA levels to disease etiology remain to be fully elucidated. In addition, the influence of genetic susceptibilities and environmental determinants on hyperuricemia calls for a detailed and nuanced examination. This review compiles data from global epidemiological studies and clinical practices, exploring the physiological processes and the genetic foundations of urate transporters in depth. Furthermore, we uncover the complex mechanisms by which the UA induced inflammation influences metabolic processes in individuals with hyperuricemia and the association with its relative disease, offering a foundation for innovative therapeutic approaches and advanced pharmacological strategies.

혈청 요산(SUA) 수치 상승을 특징으로 하는 고요산혈증은 

통풍, 심혈관 질환, 신장 질환, 대사증후군, 당뇨병 등과 같은 

다양한 질환과 관련이 있습니다. 

고요산혈증 환자의 삶의 질을 크게 저하시키는 고요산혈증의 유병률은 

전 세계적으로, 특히 대부분의 선진국에서 증가하는 추세입니다. 

요산은 

항산화,

pro-oxidative,

항염증,

산화질소 조절,

노화 방지,

면역 효과 등

다각적인 역할을 하며 생리적 및 병리학적 맥락에서 모두 중요한 역할을 합니다. 

UA possesses a multifaceted role, such as antioxidant, pro-oxidative, pro-inflammatory, nitric oxide modulating, anti-aging, and immune effects,

고요산혈증은 심혈관 및 대사증후군과 관련이 있으며, 신장 질환의 초기 증상 및 신장 기능 악화 진행과 관련이 있는 것으로 알려져 있습니다. 그러나, 높은 요산 수치는 일반적으로 진정한 원인이나 매개체로 간주되지 않고, 이러한 질병의 지표로 간주됩니다. 요산은 최근에 심장 혈관 및 신장 질환에서 고요산혈증이 원인이 된다는 것을 시사하는 새로운 데이터에 근거하여 임상적 관심과 인기를 다시 얻고 있습니다. 실험 데이터에 따르면, 요산에 노출된 혈관, 신장, 간세포 및 지방세포에서 산화 스트레스가 가장 먼저 관찰되는 현상 중 하나입니다. 요산은 혈장 내 주요 항산화제 중 하나로서, 자유 라디칼 제거제 및 전이 금속 이온의 킬레이트제로 작용하기 때문에, 요산에 의한 산화 스트레스는 역설적으로 보입니다. 고요산혈증의 임상적 의미에 관한 데이터는 더욱 혼란스럽습니다. 고요산혈증을 일상적인 추적 관찰에서 배제해야 할 쓸모없는 변수로 정의하거나 치료의 주요 위험 요인으로 정의합니다. 실험적, 역학적 데이터를 검토한 결과, 우리 몸의 여러 구획에서 요산의 항산화 또는 산화 촉진제로서의 역할을 조절하는 분자 스위치가 존재한다는 사실이 밝혀졌습니다. 이는 요산의 역설적인 역할에 대한 이해를 돕고 “요산 논쟁”을 해결하는 데 도움이 될 수 있습니다.

고요산혈증은 전 세계적으로 공중 보건 문제로 인식되고 있습니다. 이 연구는 중년 및 고령 인구 집단의 혈청 구리(Cu) 농도와 고요산혈증의 유병률 사이의 연관성을 조사하기 위해 실시되었습니다. 혈청 Cu 농도는 Roche 모듈러 P800을 사용하여 PAESA 방법을 통해 측정되었습니다. 혈청 요산(UA) 농도는 Beckman Coulter AU 5800을 통해 검출되었습니다. 고요산혈증의 유병률은 남성의 경우 혈청 UA ≥ 416 μmol/L, 여성의 경우 ≥ 360 μmol/L로 정의되었습니다. 혈청 Cu 농도와 고요산혈증의 유병률 사이의 연관성은 로지스틱 회귀분석을 통해 평가되었습니다. 본 연구에서 고요산혈증의 유병률은 17.6%(n=6,212)였습니다. 최하위 25%에 비해, 연령과 성별을 고려한 고요산혈증의 상대적 위험도는 1.38(95% CI: 1.12~1.70), 1.34(95% CI: 1.07~1.66), 1.53(95% CI: 1.23~1.91)로 나타났습니다. 혈청 Cu 농도 5분위수(추세에 대한 P < 0.001). 비슷한 결과가 남녀 하위 그룹에서 모두 발견되었습니다. 추가적인 잠재적 교란 요인을 조정해도 발견된 결과는 실질적으로 변하지 않았습니다. 결론적으로, 이 인구 기반 단면 연구에서 혈청 Cu 농도는 고요산혈증의 유병률과 양의 상관관계가 있었습니다.

https://www.frontiersin.org/journals/psychiatry/articles/10.3389/fpsyt.2022.828476/full

순환 요산 수치의 균형은 

다양한 상피 조직과 세포 유형에 걸쳐 

요산 수송체 기능에 의해 조율되는 섬세한 균형인 

요산 생산과 배설 사이의 상호작용에 달려 있습니다. 

기존 연구에서 

고요산혈증이 수많은 생물학적 과정과 신호 전달 경로에 관여한다는 사실이 밝혀졌지만, 

요산 수치 상승과 질병 발병을 연결하는 정확한 메커니즘은 

아직 완전히 규명되지 않았습니다. 

또한 

고요산혈증에 대한 유전적 감수성 및 환경적 결정 요인의 영향은 

세밀하고 미묘한 조사가 필요합니다. 

이 리뷰에서는 

전 세계 역학 연구 및 임상 사례의 데이터를 수집하여 

요산 운반체의 생리적 과정과 

유전적 기초를 심도 있게 탐구합니다. 

또한, 

요산으로 인한 염증이 

고요산혈증 환자의 대사 과정에 영향을 미치는 

복잡한 메커니즘과 관련 질환과의 연관성을 밝혀내어 

혁신적인 치료 접근법과 첨단 약리학 전략의 토대를 제공합니다.

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Introduction

Hyperuricemia is a metabolic disorder marked by elevated serum uric acid concentrations in both extracellular fluids and tissues, coupled with impaired uric acid excretion.1 The definition of hyperuricemia is SUA level ≥ 7.0 mg/dl (416.0 μmol/L) in males or ≥ 6.0 mg/dl (357.0 μmol/L) in females.2 Hyperuricemia is associated with various risk factors, including a high-purine diet, alcohol consumption, medication usage, hypertension, hypothyroidism, and obesity. Additionally, social factors such as higher socioeconomic status, as well as a history of smoking and alcohol use, further contribute to the heightened risk of developing this condition.1,3,4 UA plays a double-edged sword role in humans.5 Uric acid possesses antioxidant capabilities that combat free radicals and reactive oxygen species, thus preventing oxidative stress.6,7,8 The antioxidant effect of uric acid can be manifested in the inhibition of cell death to protect nerves as well as profile support of NO-mediated vasodilation.9 However, uric acid will be transformed into a pro-oxidant and pro-inflammatory molecule that exacerbates oxidative stress when the UA levels are increased.10,11,12 

UA, mediates the innate immune response, which can release inflammatory mediators and activate the renin-angiotensin system,13 inflammatory responses, oxidative stress, vascular endothelial dysfunction and insulin resistance.14,15,16 Mendelian randomization studies have demonstrated no causal relationship between elevated uric acid levels and the risks of diabetes, coronary heart disease, ischemic stroke, heart failure, body mass index, bone mineral density, coronary artery disease, blood pressure, metabolic syndrome, blood glucose levels, triglyceride levels, diabetes mellitus, serum creatinine levels, glomerular filtration rate, and Parkinson’s disease.17,18,19,20,21 The only phenotypes that were causally associated with HU were gout and kidney disease.22 However, epidemiological and clinical studies have linked hyperuricemia to the development of various conditions, including chronic kidney disease, fatty liver, metabolic syndrome, hypertension, insulin resistance, obesity, type 2 diabetes, and cardiovascular and cerebrovascular disorders.1,23,24,25 In this article, we review the complex physiological roles and metabolism of uric acid and the interconnections of mechanisms between hyperuricemia and potential diseases. Furthermore, we summarize the novel therapeutic interventions for hyperuricemia by examining its common comorbidities, underlying mechanisms, phenotypes, and pathogenesis.

소개

고요산혈증은

세포 외액과 조직 모두에서 혈청 요산 농도가 상승하고

요산 배설 장애가 동반되는 대사 장애입니다.1

https://www.nature.com/articles/s41598-024-55809-9

요산에 의한 관상 손상을 막기 위해 요산 재흡수를 억제하는 것이 신장을 보호할 수 있습니다. 그러나 이 접근법은 특히 산성화된 소변에서 신장에 독성을 일으킬 수 있는 관상 요산 결정화를 촉진할 수 있습니다. 관상 요산 처리가 신장 결과에 어떤 영향을 미치는지 평가하기 위해, 우리는 사구체 여과율(eGFR)이 15-60 mL/min/1.73 m2인 1042명의 환자를 대상으로 후향적 코호트 연구를 실시했습니다. 노출은 부분 요산 배설(FEUA)과 요산 대 크레아티닌 비율(UUCR)이었습니다. 신장 결과는 기준선에서 eGFR이 절반으로 감소하거나 신장 대체 요법을 시작하는 것으로 정의되었습니다. FEUA와 UUCR의 중앙값은 각각 7.2%와 0.33g/gCre였습니다. 1.9년의 중앙값 추적 기간 동안 314건의 신장 결과가 발생했습니다. 다변량 Cox 모델에서 최저 FEUA 사분위수 집단은 최고 FEUA 사분위수 집단보다 신장 결과 비율이 1.68배 더 높았습니다(95% 신뢰 구간, 1.13-2.50; P=0.01). 마찬가지로, 낮은 UUCR은 신장 결과 비율과 관련이 있었습니다. 특히, FEUA와 UUCR이 가장 높은 사분위수인 환자들은 산뇨증 환자들 중에서도 신장 결과의 위험이 가장 낮았습니다. 결론적으로, FEUA와 UUCR이 낮을수록 신부전 위험이 높다는 것을 의미하며, 요산 재흡수 증가가 신장에 해롭다는 것을 시사합니다.

고요산혈증의 정의는

남성의 경우 SUA 수치가 7.0 mg/dl(416.0 μmol/L) 이상,

여성의 경우 6.0 mg/dl(357.0 μmol/L) 이상입니다.2

고요산혈증은

고퓨린 식단, 알코올 섭취, 약물 사용, 고혈압, 갑상선 기능 저하증 및 비만을 포함한

다양한 위험 인자와 연관되어 있습니다.

또한,

높은 사회경제적 지위, 흡연 및 음주 병력과 같은

사회적 요인도 이 질환의 발병 위험을 높이는 데 기여합니다.1,3,4

요산은

인간에게 양날의 검 역할을 합니다.5

요산은

활성산소 및 활성 산소 종과 싸우는 항산화 기능을 가지고 있어

산화 스트레스를 예방합니다.6,7,8

요산의 항산화 효과는

신경을 보호하기 위한 세포 사멸 억제와

NO 매개 혈관 확장의 프로파일 지원으로 나타날 수 있습니다.9

그러나

요산은 UA 수치가 증가하면

산화 스트레스를 악화시키는 친산화 및 친염증성 분자로 전환됩니다.10,11,12

UA는

선천성 면역 반응을 매개하여 염증 매개체를 방출하고

레닌-안지오텐신 시스템,13

염증 반응,

산화 스트레스,

혈관 내피 기능 장애 및 인슐린 저항성을 활성화할 수 있습니다.14,15,16

멘델리안 무작위 배정 연구에 따르면

요산 수치 상승과 당뇨병, 관상동맥질환, 허혈성 뇌졸중, 심부전,

체질량지수, 골밀도, 관상동맥질환, 혈압, 대사증후군, 혈당 수치, 중성지방 수치, 당뇨병,

혈청 크레아티닌 수치, 사구체 여과율 및 파킨슨병 위험 사이에 인과 관계가 없음이 입증되었습니다.17,18,19,20,21

고요산혈증과 인과적으로 연관된 유일한 표현형은

통풍과 신장 질환이었습니다.22

그러나

역학 및 임상 연구에 따르면

고요산혈증은

만성 신장 질환, 지방간, 대사 증후군, 고혈압, 인슐린 저항성, 비만, 제2형 당뇨병, 심혈관 및 뇌혈관 장애 등

다양한 질환의 발병과 관련이 있습니다.1,23,24,25

이 기사에서는 요산의 복잡한 생리적 역할 및 대사와 고요산혈증과 잠재적 질환 사이의 메커니즘 상호 연결에 대해 검토합니다. 또한 고요산혈증의 일반적인 동반 질환, 근본적인 메커니즘, 표현형 및 병인을 조사하여 고요산혈증에 대한 새로운 치료 개입을 요약합니다.

The timescale and preval‎ence of hyperuricemia

Among history, Podagra first developed and identified by Hippocrates, which called “unwalkable illness” in 400 BC. with the definition podagra as a style called “arthritis of the rich.” Over 2000 years ago, Colchicine, initially used as a purgative in ancient Greece, which was later recognized by Alexander of Tralles in the sixth century AD for its specific therapeutic effects on arthritis.26 By 1200, gout was dubbed the ‘disease of kings’ due to its association with a luxurious lifestyle. In 1679, Antonie van Leeuwenhoek, a pioneer in microbiology, first observed crystals from tophi in gout patients. The chemical composition of uric acid was identified by a Swedish chemist in 1797, and by 1940, the understanding of uric acid metabolism, including its excretion and overproduction was established.27,28,29,30 The role of genetic factors in hyperuricemia preval‎ence was discovered in the 1960s. In 1963, the introduction of Allopurinol, an inhibitor of xanthine oxidase, marked a significant advancement in treating hyperuricemia. More recently, in 2010, uricase enzymes like Pegloticase and Rasburicase were approved for the management of persistent arthritis in patients with comorbidities and joint deformities.31,32,33 Currently, the emerging drugs and some advanced treatments such as uricosuric compounds, antidyslipidemic drugs or gut microbiota, can reduce the concentration of serum uric acid to address resistant hyperuricemia (Fig. 1).

고요산혈증의 발생 시기 및 유병률

역사적으로 포다그라는 기원전 400년 히포크라테스가 “걸을 수 없는 병”이라고 정의한 “부자들의 관절염”이라는 뜻으로 처음 개발 및 확인되었습니다. 2000여 년 전 고대 그리스에서 연옥으로 사용되던 콜히친은 서기 6세기 트랄레스의 알렉산더에 의해 관절염에 대한 특별한 치료 효과가 인정되었습니다.26 1200년에 통풍은 호화로운 생활 방식과 연관되어 '왕의 질병'으로 불렸습니다.

1679년 미생물학의 선구자인 안토니 반 리우벤후크는

통풍 환자에서

토피의 결정을 처음으로 관찰했습니다.

1797년 스웨덴 화학자에 의해 요산의 화학 성분이 밝혀졌고, 1940년 요산의 배설과 과잉 생산을 포함한 요산 대사에 대한 이해가 확립되었습니다.27,28,29,30 고요산혈증 유병률에서 유전적 요인의 역할은 1960년대에 밝혀졌습니다. '

1963년,

크산틴 산화효소 억제제인 알로퓨리놀의 도입으로

고요산혈증 치료에 획기적인 발전이 이루어졌습니다.

Allopurinol, an inhibitor of xanthine oxidase

최근에는 2010년에 동반 질환과 관절 기형이 있는 환자의 지속적인 관절염 관리를 위해

페글로티카제 및 라스부리카제와 같은

요산분해효소가 승인되었습니다.31,32,33

현재 요산 화합물, 항지질 약물 또는 장내 미생물과 같은

새로운 약물과 일부 첨단 치료법은

혈청 요산 농도를 감소시켜

내성 고요산혈증을 해결할 수 있습니다(그림 1).

Fig. 1

The timescale and historical development of hyperuricemia (depicted in light red) and hyperuricemia treatment (depicted in dark red) from 1944 to June 2024, along with the volume of published literature, have been analyzed using data extracted from PubMed. The search criteria included “hyperuricemia*“ in conjunction with terms such as “history”, “medicine”, “treatment”, “therapy”, “drug”, “mechanism”, “genetic”, and “uric acid”

Full size image

Hyperuricemia is a globally preval‎ent condition, particularly in high- and middle-income countries. Its preval‎ence varies significantly due to factors such as geographic location, regional differences, ethnicity, dietary habits, and economic conditions. Recent trends indicate an increase in the preval‎ence of hyperuricemia.2,3 The global preval‎ence rate has been reported to be ranging from 2.6% to 36% in different populations.34 The U.S. National Health and Nutrition Examination Survey (NHANES) indicates that approximately 21% of adults, or 43 million individuals, have been diagnosed with hyperuricemia.35 Comparative preval‎ence rates are as follows: 16.6% in Australia,36 48% in Finland with a gender-specific breakdown of 60% in males and 31% in females,37 17.0% in New Zealand with 27.8% in males and 8.8% in females,38 24.5% in Ireland with 25.0% in males and 24.1% in females,39 9.9% in Croatia,40 16.8% in Russia,41 12.1% in Turkey with 19.0% in male and 5.8% in female,42 21.2% in Qatar.43 Likewise, among developing countries, the Korea NHANES reported that the preval‎ence of hyperuricemia in Korea was 11.4% with 17.0% in male and 5.9% in female.44 In addition, it is 20.6% in Mexico,45 17.2% in Niger with 25.0% in male and 13.7% in female,46 71.6% in French Polynesia,47 9.9% in Croatia,40 44.6% in India,48 28.1% in Jordan,49 31.8% in sub-Saharan African,50 10.6% in Thailand with 18.4% in male and 7.8% in female,51 8.4% in Saudi Arabia52 and approximately 9.3% in Bangladesh.53 (Table 1)

As expected, the preval‎ence of hyperuricemia found in our study is higher in most developed countries. Interestingly, the preval‎ence of hyperuricemia is higher in coastal areas and countries than in landlocked countries, especially for countries surrounded by sea and in developing. China, with its large population, exhibits significant demographic diversity and regional differences. The preval‎ence of hyperuricemia was 6.4% in Chinese adults according to a study covering 13 provinces.2 Geographically, the preval‎ence of hyperuricemia is highest in southern China (9.1%) and lowest in northern China (3.2%). The majority of affected individuals (71.0%) reside in urban areas, with a substantial proportion (44.7%) living in coastal cities. The preval‎ence is notably higher in urban regions (8.0%) compared to rural areas (5.0%). By 2014, the overall preval‎ence of hyperuricemia in mainland China had reached 13.3%,54 and this gradually increased to 17.7% in 2017. The preval‎ence was higher in the elderly population, and the rate was higher in male (23.5%) than in female (11.7%).55

고요산혈증은 특히 고소득 및 중산층 국가에서 전 세계적으로 널리 퍼져 있는 질환입니다. 고요산혈증은 지리적 위치, 지역적 차이, 인종, 식습관, 경제 상황 등의 요인으로 인해 유병률이 크게 달라집니다. 최근 고요산혈증 유병률이 증가하는 추세입니다.2,3

전 세계 유병률은 인구 집단에 따라 2.6%에서 36%까지 보고되었습니다.34

미국 국민건강영양조사(NHANES)에 따르면 성인의 약 21%인 4,300만 명이 고요산혈증 진단을 받은 것으로 나타났습니다.35 비교 유병률을 보면 다음과 같습니다: 호주 16.6%,36 핀란드 48%(남성 60%, 여성 31%),37 뉴질랜드 17.0%(남성 27.8%, 여성 8.8%),38 아일랜드 24.5%(남성 25.0%, 여성 24.1%),39 크로아티아 9.9%,40 러시아 16.8%,41 터키 12.1%(남성 19.0%, 여성 5.8%),42 카타르 21.2%입니다.43 마찬가지로 개발도상국 중 한국의 고요산혈증 유병률은 11.4%로 남성 17.0%, 여성 5.9%로 한국 국민건강영양조사(NHANES)에서 보고한 바 있습니다.44 또한 멕시코 20.6%,45 니제르 17.2%(남성 25.0%, 여성 13.7%),46 프랑스령 폴리네시아 71.6%,47 크로아티아 9.9%,40 인도 44.6%,48 요르단 28.1%,49 사하라 이남 아프리카 31.8%,50 태국 10.6%(남성 18.4%, 여성 7.8%),51 사우디아라비아 8.4%,52 방글라데시 약 9.3%이다 (표 1).

예상대로, 본 연구에서 발견된 고요산혈증 유병률은 대부분의 선진국에서 더 높았습니다.

흥미롭게도

고요산혈증 유병률은

내륙 국가보다 해안 지역과 국가,

특히 바다로 둘러싸인 국가와 개발도상국에서 더 높았습니다.

인구가 많은 중국은 인구학적 다양성과 지역적 차이가 매우 큽니다. 13개 성을 대상으로 한 연구에 따르면 중국 성인의 고요산혈증 유병률은 6.4%였습니다.2 지리적으로 고요산혈증 유병률은 중국 남부(9.1%)에서 가장 높고 북부(3.2%)에서 가장 낮습니다. 고요산혈증 환자의 대부분(71.0%)이 도시 지역에 거주하며, 상당수(44.7%)가 연안 도시에 거주하고 있습니다. 유병률은 농촌 지역(5.0%)에 비해 도시 지역(8.0%)에서 현저히 높습니다. 2014년까지 중국 본토의 전체 고요산혈증 유병률은 13.3%에달했으며54 2017년에는 17.7%로 점차 증가했습니다. 유병률은 노인 인구에서 더 높았으며, 여성(11.7%)보다 남성(23.5%)에서 더 높았습니다.55

Table 1 Diagnostic criteria and preval‎ence for hyperuricemia in each country/area

Full size table

Physiological role of uric acid

Uric acid is the final product of the catabolism of purine nucleotides. UA is a weak diprotic acid with one dis-sociable H+ at physiologic pH values. The concentrations of UA range from 3.5 to 7.2 mg/dL (210–430 μmol/L) in males and 2.6–6.0 mg/dL (155–360 μmol/L) in premenopausal females.2,35 In addition to its role as a byproduct of purine metabolism, uric acid is recognized for its multifaceted effects, which include antioxidant, pro-oxidant, pro-inflammatory, nitric oxide regulation, immune system interactions, and anti-aging properties.7,56

요산의 생리적 역할

요산은 퓨린 뉴클레오타이드의 이화 작용의 최종 산물입니다. 요산은 생리적 pH 값에서 비사회성 H+가 하나 있는 약한 이염기성 산입니다. 요산의 농도는 남성의 경우 3.5-7.2mg/dL(210-430 μmol/L), 폐경 전 여성의 경우 2.6-6.0 mg/dL(155-360 μmol/L)입니다.2,35 요산은 퓨린 대사의 부산물로서의 역할 외에도 항산화, 항산화, 항염증, 산화 질소 조절, 면역 체계 상호작용, 항노화 특성 등 다면적 효과로 인정받고 있습니다.7,56

Antioxidant and Pro-oxidant

Uric acid is a natural byproduct of purine metabolism, arising from the enzymatic degradation of hypoxanthine to xanthine, which is subsequently converted by xanthine oxidase.57 In the process in which uric acid is produced, ROS, particularly superoxide anions and hydrogen peroxide (H2O2), are generated as byproducts.58,59,60,61 Uric acid functions as a powerful antioxidant, effectively neutralizing singlet oxygen molecules, oxygen radicals, and peroxynitrite (ONOO-) molecules, due to its ability to provide electrons and act as a powerful reducing agent.27,28,29,62,63,64,65 It can easily provide a hydrogen atom to free radicals, thereby stabilizing them and preventing further oxidative damage.66 Therefore, uric acid has remarkable antioxidant properties that effectively combat oxidative stress induced by free radicals and reactive oxygen species (ROS).7 Free radicals are highly reactive entities that can cause oxidative stress and cellular damage and contribute to the development of various diseases.67 Nevertheless, uric acid has a highly reducing structure that effectively neutralizes free radicals and mitigates their harmful effects. Additionally, uric acid acts as an inhibitor of the oxidative chain reaction through a dual mechanism.68,69 It captures and neutralizes free radicals, forming stable intermediates and thereby impeding the transmission of the oxidative reaction.66 Furthermore, the complex formed by uric acid and free iron ions acts as a chelating agent, effectively inhibiting the formation of free radicals from iron ions and enhancing the antioxidant effect.67 

Uric acid regulates the inflammatory response by inhibiting the production of inflammatory mediators, which significantly reduces the formation of free radicals.57 One of the most interesting aspects of the antioxidant function of uric acid is its potential role in neuroprotection.60,61,62 Uric acid and purines, including adenosine and adenosine triphosphate, have been implicated in regulating central nervous system functions such as convulsive threshold, memory, cognition, sleep, activity, appetite, mood, social interaction, drive, impulsivity, and intelligence.70,71,72 Some studies have found that patients with neurodegenerative diseases, like Parkinson’s disease, Alzheimer’s disease, and amyotrophic lateral sclerosis (ALS), tend to have lower serum uric acid levels, suggesting a potential neuroprotective effect of uric acid.73 Patients with major depression and anxiety disorders had lower plasma uric acid levels and increased UA levels after treatment, further suggesting that UA may have a neuroprotective effect.70 The antioxidant properties of UA and its ability to inhibit oxidative stress may attenuate inflammatory damage to the nervous system and contribute to the maintenance of neuron number and function by inhibiting programmed apoptosis of neuronal cells, which protects against excessive neuronal cell damage. The capacity of uric acid to neutralize reactive oxygen species (ROS) and shield neurons from oxidative damage may underlie its observed neuroprotective effects. Furthermore, the antioxidant properties of uric acid have significant implications for cardiovascular health.66 

The ability of uric acid to scavenge ROS and reduce oxidative stress may have protective effects on the cardiovascular system. Studies illustrated that uric acid may indirectly support NO-mediated vasodilation by preventing nitric oxide degradation by superoxide radicals. This finding implies that uric acid may play a role in maintaining vascular health and regulating blood pressure.74 The antioxidant function of serum uric acid reflects the multifaceted and complex nature of its physiological role. The ability of uric acid to neutralize free radicals and protect against oxidative stress has implications for all aspects of health.67,75 Interestingly, a level of uric acid that is either too high or too low disrupts the delicate balance of oxidative stress regulation and may lead to excessive oxidative damage or impaired antioxidant defense. At higher intracellular concentrations, uric acid can function as a pro-oxidant molecule.76 Studies have shown that within various cell types, including vascular smooth muscle cells, endothelial cells, adipocytes, hepatocytes, pancreatic islet cells, and renal tubular cells, uric acid can activate NADPH oxidase, a crucial enzyme involved in the generation of reactive oxygen species.57,76 Moreover, in certain cell types, NADPH oxidase may translocate to the mitochondria, further exacerbating oxidative stress.77,78 The effects of soluble urate on mononuclear cells are multifaceted. Some studies suggest that priming peripheral blood mononuclear cells (PBMCs) with urate enhances the release of interleukin-1β (IL-1β) in response to lipopolysaccharide (LPS), indicating a potential pro-inflammatory effect.79 While it was found no significant effects of urate on IL-1β release, superoxide dismutase 2 (SOD2) gene transcription, or the total antioxidant capacity of the cell.80

항산화 및 항산화제

요산은 퓨린 대사의 자연적인 부산물로,

하이폭산틴이 효소적으로 분해되어

잔틴으로 전환된 후 잔틴 산화효소에 의해 생성됩니다.57

요산이 생성되는 과정에서

ROS, 특히 슈퍼옥사이드 음이온과 과산화수소(H2O2)가

부산물로 생성됩니다.58,59,60,61

요산은

전자를 제공하고 강력한 환원제로 작용하는 능력으로 인해

단일 산소 분자,

산소 라디칼 및 퍼옥시니트라이트 (ONOO-) 분자를

효과적으로 중화시키는 강력한 항산화제로 기능합니다 .27,28,29,62,63,64,65

요산은

활성산소에 수소 원자를 쉽게 제공하여 활성산소를 안정화시키고

추가적인 산화 손상을 방지할 수 있습니다.66

따라서

요산은

활성산소와 활성 산소종(ROS)에 의해 유발되는 산화 스트레스에 효과적으로 대항하는

뛰어난 항산화 특성을 가지고 있습니다.7

활성산소는

산화 스트레스와 세포 손상을 유발하고

다양한 질병의 발병에 기여할 수 있는 반응성이 높은 존재입니다.67

그럼에도

요산은 환원 구조가 매우 강하여

활성산소를 효과적으로 중화시키고

유해한 영향을 완화할 수 있는 특성을 가지고 있습니다.

또한

요산은 이중 메커니즘을 통해

산화 연쇄 반응의 억제제 역할을 합니다.68,69

요산은

자유 라디칼을 포획하고 중화하여 안정적인 중간체를 형성함으로써

산화 반응의 전달을 방해합니다.66

또한

요산과 유리 철 이온이 형성하는 복합체는 킬레이트 제 역할을 하여

철 이온으로부터 자유 라디칼의 생성을 효과적으로 억제하고

항산화 효과를 향상시킵니다.67

요산은

염증 매개체의 생성을 억제하여

염증 반응을 조절하여

자유 라디칼 형성을 현저히 감소시킵니다 .57

요산의 항산화 기능의 가장 흥미로운 측면 중 하나는

신경 보호에서의 잠재적 역할입니다 .60,61,62

아데노신과 아데노신 삼인산을 포함한 요산과 퓨린은

경련 역치, 기억, 인지, 수면, 활동, 식욕, 기분, 사회적 상호 작용, 추진력, 충동성, 지능과 같은

중추 신경계 기능을 조절하는 데 관여합니다.70,71,72

일부 연구에 따르면

파킨슨병, 알츠하이머병, 근위축성 측삭 경화증(ALS)과 같은

신경 퇴행성 질환 환자는 혈청 요산 수치가 낮은 경향이 있어

요산의 잠재적인 신경 보호 효과를 시사합니다.73

배경 산화 스트레스와 신경 염증을 비롯한 여러 위험 요소가 파킨슨병의 진행에 영향을 미칩니다. 역학 연구에 따르면 요산염 수치가 높을수록 파킨슨병 발병 위험이 낮아지는 것으로 밝혀졌습니다. 그러나 이러한 연관성에 대한 메커니즘적 근거는 아직 명확하지 않습니다. 요산염은 산화 스트레스로 인한 세포 사멸로부터 도파민 신경세포를 보호합니다. 여기에서는 지질 다당류(LPS)로 유도된 PD 모델에서 미세아교세포 활성화에서 요산염의 새로운 역할을 조사했습니다. 방법 우리는 신경염증을 검출하기 위해 Griess, ELISA, 실시간 PCR, 웨스턴 블롯, 면역조직화학 및 면역형광법을 활용했습니다. 그리스, ELISA, 웨스턴 블롯 및 면역 형광 분석의 경우, 폴리엘라이신(PLL)으로 사전 코팅된 6웰 플레이트에 세포를 시드하고 지정된 약물과 함께 24시간 동안 배양했습니다. 실시간 PCR 분석의 경우, PLL로 사전 코팅된 6웰 플레이트에 세포를 시드하고 표시된 약물과 함께 6시간 동안 배양했습니다. 동물 실험의 경우, 정위 수술 전후 5일 연속으로 매일 2회씩 요산 또는 그 운반체를 쥐에게 주사했습니다. 쥐를 사살하고 4주간의 LPS 주입 후 뇌 조직을 채취했습니다. 결과 배양된 BV2 세포와 쥐의 일차 미세아교세포에서 요산염은 염증성 사이토카인 생산과 유도성 사이클로옥시게나제 2 및 산화질소 합성효소 발현을 억제하여 활성화된 미세아교세포의 독성 영향으로부터 도파민 신경세포를 보호하는 것으로 나타났습니다. 요산염의 신경 보호 효과는 항염증제인 인터루킨 10 및 형질 전환 성장 인자 β1의 자극과도 관련이 있을 수 있습니다. 요산염과 LPS를 병용 처리하면 용량 의존적으로 세포 내 요산염 수치가 증가했으며, 이러한 효과는 포도당 수송체 9와 요산염 수송체 1(URAT1)의 억제제인 프로베네시드(PBN)로 전처리하면 제거되었습니다. 또한 PBN은 요산염의 항염증 효과도 없앴습니다. 이러한 시험관 내 관찰과 일관되게, LPS로 유도된 PD 쥐 모델에서 요산염 투여에 의해 티로신 하이드 록 실라 제 양성 뉴런의 수가 감소하고 운동 협응력의 손실이 역전되었습니다. 또한 혈장 요산염 수치가 증가하면 URAT1 발현 감소, 인터루킨-1β 발현 증가, 이온화 칼슘 결합 어댑터 분자 1 양성 미세아교세포의 수가 형태 변화와 함께 폐지되었습니다. 결론 요산염은 요산염 수송체 매개 세포 내 요산염 수준을 조절하여 미세아교세포 활성화에 의해 유발되는 세포 독성으로부터 신경세포를 보호합니다.

주요 우울증 및 불안 장애 환자는

치료 후 혈장 요산 수치가 낮아지고

UA 수치가 증가하여

UA가 신경 보호 효과를 가질 수 있음을 추가로 시사합니다.70

요산의 항산화 특성과 산화 스트레스를 억제하는 능력은

신경계의 염증성 손상을 약화시키고

신경 세포의 프로그램된 세포 사멸을 억제하여

과도한 신경 세포 손상으로부터 보호함으로써

신경 세포 수와 기능 유지에 기여할 수 있습니다.

요산이

활성산소종(ROS)을 중화시키고

뉴런을 산화적 손상으로부터 보호하는 능력은

관찰된 신경 보호 효과의 근간이 될 수 있습니다.

또한

요산의 항산화 특성은

심혈관 건강에도 중요한 영향을 미칩니다.66

요산이

ROS를 제거하고

산화 스트레스를 감소시키는 능력은

심혈관계에 보호 효과를 줄 수 있습니다.

연구에 따르면

요산은

과산화 라디칼에 의한 산화질소 분해를 방지하여

NO 매개 혈관 확장을 간접적으로 지원할 수 있는 것으로 나타났습니다.

이 발견은

요산이 혈관 건강 유지와 혈압 조절에 중요한 역할을 할 수 있음을 시사합니다.74

혈청 요산의 항산화 기능은

요산의 생리적 역할의 다면적이고 복잡한 특성을 반영합니다.

요산이 활성산소를 중화시키고

산화 스트레스로부터 보호하는 능력은 건강의 모든 측면에 영향을 미칩니다.67,75

흥미롭게도 요산 수치가 너무 높거나 낮으면

산화 스트레스 조절의 섬세한 균형이 깨지고

과도한 산화 손상이나 항산화 방어력 저하를 초래할 수 있습니다.

세포 내 농도가 높으면 요산이 항산화 분자로 작용할 수 있습니다.76 연구에 따르면 혈관 평활근 세포, 내피 세포, 지방 세포, 간세포, 췌장 섬 세포, 신장 관 세포 등 다양한 세포 유형에서 요산이 활성 산소 종 생성에 관여하는 중요한 효소인 NADPH 산화 효소를 활성화할 수 있습니다.57,76 또한 특정 세포 유형에서는 NADPH 산화 효소가 미토콘드리아로 이동하여 산화 스트레스를 더욱 악화시킬 수 있습니다.77,78 단핵 세포에 대한 용해성 요산염의 영향은 다방면에 걸쳐 있습니다. 일부 연구에 따르면 말초 혈액 단핵 세포(PBMC)에 요산염을 프라이밍하면 지질 다당류(LPS)에 반응하여 인터루킨-1β(IL-1β)의 방출이 증가하여 잠재적인 전 염증 효과를 나타냅니다.79 요산염이 IL-1β 방출, 슈퍼옥사이드 디스뮤타제 2(SOD2) 유전자 전사 또는 세포의 총 항산화 능력에 큰 영향을 주지 않는 것으로 밝혀졌지만.80

Pro-inflammatory

Uric acid acts as a danger signal, being naturally released by necrotic cells and subsequently initiating adaptive immune responses. Studies have indicated that uric acid crystals can engage with Toll-like receptors (TLRs), which are membrane-bound receptors integral to innate immunity, thereby inducing inflammation.10,11,81,82 Specifically, TLR-2, TLR-4, and the myeloid differentiation primary response protein 88 (MyD88) are crucial to the inflammatory reaction of macrophages to uric acid crystals. These crystals can directly interact with these receptors, initiating signal transduction pathways that ultimately activate NF-κB.83,84,85,86,87 NF-κB is a transcription factor responsible for improving the transcription of various inflammation-associated proteins, including pro-interleukin-1 (pro-IL-1), when secreted in the extracellular space.88 In recent years, studies have revealed that UA activates the TLR4-NLRP3 inflammatory complex, which is a multi-protein complex that plays a pivotal role in initiating the innate immune response to various danger signals, including MSU crystals. Upon recognition of MSU crystals, the NLRP3 inflammasome is activated, leading to the cleavage of pro-inflammatory cytokines, specifically interleukin-1β (IL-1β) and interleukin-18 (IL-18).89,90,91,92,93 These cytokines play a central role in orchestrating the inflammatory response by recruiting additional immune cells and amplifying the proinflammatory cascade.57 UA exerts its influence on the renin-angiotensin system through dual mechanisms involving the stimulation of plasma renin activity and renal renin expression‎. Additionally, UA contributes to the activation of the intrarenal angiotensin system.94 These immune inflammatory pathways, particularly those involving monocytes and macrophages, are upregulated in the presence of hyperuricemia.95,96 The pro-inflammatory function of uric acid is critical for revealing its role in various inflammatory conditions, such as gout, cardiovascular disease, and metabolic syndrome.82 UA was observed to reduce reactive oxygen species (ROS) and interleukin-6 (IL-6) production in macrophages while enhancing fatty acid oxidation (FAO) under inflammatory and hypoxic conditions in vitro.95 Although the antioxidant properties of uric acid have long been recognized, its pro-inflammatory effects complicate its physiological significance and clinical relevance.

Nitric oxide regulation

Nitric oxide (NO) is a vital signaling molecule produced by endothelial nitric oxide synthase (eNOS) within endothelial cells. It serves as a powerful vasodilator, modulating blood pressure by inducing relaxation in the smooth muscle cells of blood vessel walls.97 Hyperuricemia, by inducing oxidative stress and inflammation, diminishes the expression‎ of eNOS and the synthesis of NO, while elevating levels of inflammatory cytokines such as IL-6 and TNF-α, ultimately impairing endothelial function.98,99 In addition, NO is involved in inhibiting platelet aggregation, leukocyte adhesion, and inflammation. It also contributes to various signaling pathways that affect cardiac function, nerve conduction, and the immune response.100 The interaction between uric acid and NO is bidirectional. When concentrations are low, uric acid acts as a natural antioxidant that scavenges free radicals and prevents oxidative damage. Specifically, uric acid neutralizes peroxynitrite, a harmful molecule formed from the reaction between nitric oxide and superoxide radicals.101,102 This antioxidant effect of uric acid protects nitric oxide from degradation by superoxide radicals, thereby indirectly supporting nitric oxide bioavailability and potentially enhancing nitric oxide-mediated vasodilation.61,103 However, at higher concentrations, uric acid reduces NO bioavailability, impairs eNOS function, reduces NO production, and further exacerbates endothelial cell dysfunction. These complex interactions have important implications for cardiovascular health, renal function, and treatment of NO-related diseases.97,104,105 Uric acid has a protective effect against dementia and cognitive impairment related to senescence.72,106,107,108,109,110 UA endowed with hydrophilic antioxidant properties which can exert a protective influence against Alzheimer’s disease and Parkinson’s disease, while hyperuricemia could potentially worsen vascular dementia, encompassing conditions such as stroke and small vessel cerebrovascular disease.111

Aging and Anti-aging effects

Uric acid can influence cellular activities, such as cell proliferation, by modulating EGF/EGFR bioactivity. Hyperuricemia can downregulate the expression‎ of cell cycle proteins including D1, p-Rb, Ki67, and CDK4, inducing cellular senescence and consequently diminishing EGF/EGFR signaling. Increased levels of uric acid result in inflammation and oxidative stress, which serve as potential risk factors for cellular senescence, apoptosis, and disruptions in the cell cycle. Conversely, physiological concentrations of uric acid (5 mg/dl) exhibit anti-aging effects by enhancing growth factor activity in aging cells. However, at higher concentrations (10 mg/dl), uric acid promotes cellular senescence and downregulates EGF/EGFR signaling.112

Immune system interaction effects

The interaction of uric acid with the immune system involves the formation of monosodium urate (MSU) crystals. These uric acid crystals activate pattern recognition receptors (PRRs), including Toll-like receptors (TLRs), NOD-like receptors, and the NLRP3 inflammasome.113,114,115,116 Activation of these receptors initiates an inflammatory signaling cascade resulting in the secretion of pro-inflammatory cytokines and chemokines. These needle-shaped crystals can accumulate in diverse tissues, particularly in joints, eliciting an innate immune response. Consequently, immune cells, notably neutrophils and macrophages, are recruited to sites of crystal deposition.10 Moreover, neutrophils can phagocytose uric acid crystals and release various inflammatory mediators, such as interleukin-1β and ROS, further activating inflammation and amplifying the local inflammatory response.113 Studies have shown that UA also affects both T-cell populations and regulatory T-cell populations.117 UA-induced inflammation leads to the recruitment and activation of effector T cells at the site of crystal deposition, thereby exacerbating local inflammation.113,117

The physiology of Hyperuricemia

Hyperuricemia is characterized by an elevated level of uric acid in the bloodstream, often surpassing the normal physiological threshold. This metabolic state arises from a dysregulation between uric acid production and elimination, culminating in its accumulation in the bloodstream.118 The etiology of hyperuricemia is multifaceted and involves genetic predispositions, environmental factors, and complex metabolic pathways governing urate homeostasis.

Factors influencing uric acid

The risk of developing hyperuricemia is influenced by a combination of inherited genetic variants, environmental factors, gene-environment interactions, and intrinsic factors such as age, sex, and body weight.119 Research indicates that factors such as age, diet, alcohol consumption, fructose-rich intake, pharmacologic interventions and diseases, such as obesity, insulin resistance, Down syndrome, and kidney disease, contribute to the development of hyperuricemia120,121,122,123,124 (Fig. 2).

Fig. 2

Consumption of purine-rich meats such as beef, pork, lamb, and seafood like oysters, shrimp, and tuna, as well as dietary fructose, are known to elevate uric acid (UA) production. Additionally, alcohol metabolism from beer and distilled spirits, along with certain medical conditions such as tumor lysis syndrome and obesity, pose increased risks for hyperuricemia. Hepatic metabolism of uric acid involves the sequential processing of purine nucleotides, including adenosine monophosphate (AMP), guanosine monophosphate (GMP), and inosine monophosphate (IMP).66 IMP plays a pivotal role as a key intermediate in purine nucleotide biosynthesis, serving as a precursor for the synthesis of both adenosine monophosphate (AMP) and guanosine monophosphate (GMP). Moreover, IMP can be enzymatically deaminated by IMP dehydrogenase, leading to the formation of inosine. Inosine, in turn, can undergo phosphorylation to become hypoxanthine. Hypoxanthine undergoes oxidative reactions catalyzed by xanthine oxidase (XOD), resulting in the production of xanthine. Xanthine can further undergo oxidation reactions, also catalyzed by XOD, ultimately leading to the formation of uric acid from xanthine.118 However, xanthine oxidase inhibitors, such as allopurinol, febuxostat, and topiroxostat, serve as first-line therapies by effectively reducing the production of uric acid from both endogenous and dietary purine sources. In the final step of purine metabolism, the enzyme uricase converts uric acid into allantoin, a highly soluble compound. While humans lack the uricase enzyme, animals naturally possess it. The therapeutic agents pegloticase and rasburicase are recombinant forms of uricase, designed to facilitate the breakdown of uric acid in humans

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Dietary

Dietary selections abundant in purine, particularly nucleic acids, notably contribute to the production of uric acid. Beverages like beer, which contains purine-rich yeast, along with the consumption of foods such as bacon, beef, lamb, turkey, veal, venison, organ meats, and certain types of fish and shellfish (including anchovies, cod, tuna, sardines, shrimp, scallops, trout, and haddock), are implicated in elevating uric acid levels.101,125 Beer contains high amounts of guanosine, and ethanol increases the degradation of ATP. Alcohol and dietary purines (meat, seafood) may be risk factors for gout, which has traditionally been considered a disease of affluence. Sugar (sucrose) is a disaccharide composed of glucose and fructose.126 Among middle-aged Chinese men, a direct and notable association exists between seafood consumption and the occurrence of hyperuricemia. Conversely, protein intake from either animal or plant sources demonstrated a contrasting impact on the preval‎ence of hyperuricemia. Nevertheless, comprehensive data on the precise purine content of foods remains limited, primarily due to various factors such as food processing techniques, which can influence purine levels.121 According to the NHANES, dietary folate intake reduces the risk of hyperuricemia in female, while vitamin B12 and folate intake are associated with a reduced risk of hyperuricemia in men.127

Fructose metabolism

Fructose metabolism, particularly through the aldolase reductase pathway in the liver, results in increased UA levels.128 Fructose is transported into cells via SLC2A5 (Glut5) and undergoes metabolism to fructose 1-phosphate catalyzed by ketohexokinase (KHK), a process requiring ATP. This metabolic pathway primarily occurs in the liver, leading to a transient reduction in intracellular ATP and phosphate levels. Subsequently, activation of adenosine monophosphate (AMP) deaminase occurs, with AMP generated from fructose metabolism entering the purine catabolic pathway, ultimately resulting in the production of uric acid.129

Purine metabolism

Uric acid originates from the breakdown of purines catalyzed by the oxidized and reduced forms of xanthine oxidoreductase (XOR) and xanthine dehydrogenase (XDH). Purines are essential nucleotide components of DNA and RNA, crucial for cell division and metabolism.101 Both endogenous purine metabolism and dietary intake contribute to uric acid production. Increased cellular catabolism, heightened endogenous purine synthesis, and a diet rich in purines can elevate urate levels. Although basal XOR expression‎ is typically low in humans, various factors such as hypoxia, ischemia-reperfusion injury, interleukin-1 (IL-1), interleukin-6 (IL-6), tumor necrosis factor-alpha (TNF-α), and corticosteroid treatment can markedly enhance XOR transcription. Additionally, the conversion of XDH to XO is expedited under hypoxic conditions.101 Purine metabolism occurs primarily in the liver and in tissues where xanthine oxidase is widely distributed. Approximately 65% of uric acid is excreted from the kidneys, and the rest is excreted mainly into the intestine.130 Due to the absence of the uricase enzyme responsible for converting uric acid into allantoin and allantoic acid, UA remains the terminal metabolic product in humans. The majority of uric acid is filtered in its free form, with approximately 90% of the filtered UA being reabsorbed.131 Hyperuricemia can be triggered by inadequate excretion due to reduced glomerular filtration, impaired tubular secretion and improved tubular reabsorption.39,40 Elevated phosphoribosyl pyrophosphate (PRPP) synthetase activity and deficiency in hypoxanthine phosphoribosyl transferase (HPRT) not only enhance endogenous purine synthesis but also result in excessive production and buildup of uric acid.132,133

Disease

Cellular turnover processes like tumor lysis, rhabdomyolysis, and hemolysis contribute to increased urate production. Additionally, various transporters in the intestinal mucosa and salivary glands, diverse medications, extracellular fluid volume depletion, and organic acids that facilitate transport can influence uric acid metabolism. Thus, both intrinsic and extrinsic factors play roles in urate production.134

Uric acid regulation

UA levels are contingent on the dynamic equilibrium among purine-rich food intake, endogenous urate synthesis, and urate excretion through various routes, including urine and the gastrointestinal tract. Disruptions to this balance can impact serum uric acid (SUA) levels.135,136,137 The transport of uric acid entails multiple genes and proteins, collectively participating in the complex mechanisms of uric acid reabsorption and secretion. At a genome-wide significant level, three loci (ABCG2, SLC2A9, and CUX2) have been identified in association with renal urate overload, whereas four loci (ABCG2, SLC2A9, CUX2, and GCKR) have been linked to renal urate underexcretion.138,139 The main transporter genes are SLC22A12 (URAT1), SLC2A9 (GLUT9), and ABCG2 (BCRP).140(Table 2) It is increasingly recognized that disturbances in urate transport, both in the gastrointestinal tract and kidneys, are pivotal in the pathogenesis of diseases associated with hyperuricemia. Investigating these transporters and their genetic loci is essential for regulating and achieving target serum urate levels. Moreover, alterations in gut microbiota structure or imbalance can contribute to metabolic disorders, influencing the synthesis of purine-metabolizing enzymes and the release of inflammatory cytokines. This relationship is closely linked to the onset and progression of hyperuricemia and gout, which are metabolic immune disorders.141,142

Table 2 Urate transporters and their characteristics related to launched therapies for hyperuricemia

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Gut microbiota

UA serves as both an antioxidant and an immune modulator, exerting significant influence on the composition of the gut microbiota. Notably, the gastrointestinal tract plays a pivotal role as a pathway for uric acid excretion, with the microbial ecosystem within the gut intricately involved in this metabolic process.143 Transporters for uric acid located in intestinal epithelial cells facilitate the translocation of uric acid from the bloodstream into the intestinal lumen.144,145,146,147,148,149,150,151,152 Once in the intestinal lumen, UA can either be directly excreted or metabolized by the gut microbiota.153 Specific bacteria, such as Lactobacillus and Pseudomonas, participate in the degradation and elimination of uric acid in the intestine through the production of short-chain fatty acids (SCFAs).154 Moreover, the activities of enzymes involved in uric acid metabolism are intricately connected to the gut microbiota.155,156,157 Uricase, an enzyme responsible for converting UA into allantoin and urea, is found in various bacterial species including Bacillus pasteurii, Proteus mirabilis, and E. coli. Certain strains of Lactobacillus, such as Lactobacillus sp. OL-5, Lactobacillus plantarum Mut-7, and Lactobacillus plantarum Dad-13, have been found to exhibit higher intracellular uricase activity, further emphasizing the role of gut microbiota in UA metabolism.143,149,154 An imbalance in the gut microbiota can elevate uric acid concentrations, thereby exacerbating the chronic deposition of UA crystals in joints, characteristic of gout. This dysbiosis typically involves a proliferation of opportunistic pathogens alongside a reduction in beneficial bacteria known to stimulate the synthesis of anti-inflammatory cytokines.145,158,159 The exploration of intestinal flora metabolism represents a promising frontier in clinical research pertaining to hyperuricemia and gout. Metabolic research has established a correlation between hyperuricemia and disruptions in the primary bile acid pathway or intestinal metabolism, suggested that targeting the gut microbiome could offer innovative therapeutic approaches for managing hyperuricemia and its associated complications. Future studies will concentrate on unraveling the intricate mechanisms through which gut microbiota modulates metabolic processes in these patient populations.

Genetics of urate control

Hyperuricemia and hyperuricosuria have been shown to cluster in families, indicating a familial transmission pattern. Studies in South American ethnic groups have demonstrated heritability rates ranging from 39% to 45%.160,161,162,163,164,165 Both adults and children have been found to exhibit genetic mutations that affect baseline renal urate excretion levels. In a genome-wide association study (GWAS) involving more than 140,000 individuals of European descent, uric acid receptors encoded by twenty-eight chromosomal genes were discovered to impact plasma uric acid levels. Genetic variants associated with uric acid levels mainly include purine metabolism (e.g., XDH, HPRT1), urate transporters (e.g., SLC2A9, SLC22A12), and renal urate processing regulators (e.g., ABCG2).119,166,167 Single nucleotide polymorphisms (SNPs) within or near these genes have consistently shown associations with variations in uric acid levels across diverse populations.168 Genome-wide association studies (GWAS) have identified key loci housing urate transporters crucial for uric acid excretion in both renal and gastrointestinal pathways.167,169 Through functional insights and expression‎ quantitative trait loci (eQTL) analyses, several loci have identified probable causal genes, such as SLC2A9, ABCG2, PDKZ1, SLC22A11 (OAT4), and INHBB.166 Additionally, numerous other loci have strong candidate genes identified, including GCKR, RREB1, SLC17A1 to SLC17A4, SLC22A12, MAF, MLXIPL, PRKAG2, HNF4G, A1CF, IGFR1, and HLF.166,170 (Fig. 3) The primary physiological regulation of serum uric acid levels occurs through renal excretion.171 GWAS in major populations consistently highlight urate transporter genes as pivotal loci influencing serum uric acid levels,138,139 notably SLC2A9 (GLUT9) and SLC22A12 (URAT1), involved in urate reabsorption from urinary filtrates.172,173 For instance, the primary effect of SLC2A9 (rs12498742) explains 2% to 3% of serum uric acid level variance in Europeans, which is substantial for a complex phenotype.174,175 Variation in ABCG2 (BCRP) is also noteworthy across European and East Asian populations.176,177,178 Notably, in individuals of European ancestry, the genetic control of SLC2A9a and SLC2A9b isoforms, situated at basolateral and apical membranes respectively, constitutes a prominent genetic signal.172,174 Thus, we concluded several key genes have been identified with significant associations with SUA levels. Among these genes, ABCG2 stands out as one of the most crucial and strongly linked to SU levels to the risk of hyperuricemia.167,171,179,180 A specific polymorphism (rs2231142) within ABCG2 has been identified, which reduces urate efflux activity and increases the susceptibility to both HU and gout.181 Notably, this variant is more preval‎ent in Asian populations compared to Europeans.180,182 Another important gene, SLC2A9, encodes a urate transporter and exerts a significant influence on SUA levels. A specific polymorphism (rs734553) within SLC2A9 has been associated with an elevated risk of hyperuricemia.119,166 Interestingly, the preval‎ence of this variant varies among different populations, with higher frequencies observed in Asian populations. Research indicates that the rs1967017 variant in PDZK1 creates a binding site for the transcription factor hepatocyte nuclear factor 4α (HNF4α) within an enhancer region upstream of the PDZK1 transcription start site.170 This binding increases PDZK1 expression‎, potentially leading to reduced urate excretion. Another prominent genetic variant associated with serum urate levels is rs1263026 at GCKR.183 The Leu allele of this variant induces relaxation of glucokinase inhibition, resulting in heightened glucose phosphorylation. This process diminishes the ATP pool and augments urate production through ADP catabolism.184 However, other loci with more modest effects have not consistently replicated in subsequent studies examining their correlation with serum urate levels.

Fig. 3

In East Asian populations, four loci have demonstrated a significant association with serum urate levels: SLC2A9, ABCG2, SLC22A12, and MAF. Similarly, in African American populations, three loci have been identified: SLC2A9, SLC22A12, and SLC2A12. In contrast, the European population predominantly shows an association with only one locus, SLC2A9. Australian studies have identified 28 loci, encompassing all but one (SLC2A12) of those found in African American and East Asian populations. Among these diverse populations, certain loci, such as SLC2A9, ABCG2, GCKR, and SLC17A1-SLC17A4 (also known as NPT1-NPT4), exhibit stronger effects and have been consistently replicated in multiple studies

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URAT1

URAT1, located in the membrane of renal tubular epithelial cells, serves as a uric acid transporter protein. It plays a crucial role in mediating UA reabsorption, a process in which approximately 90% of uric acid is typically reabsorbed following glomerular filtration.175 URAT1 belongs to the organic anion transporter (OAT) subgroup within the broader gene family. Other subcategories within this family include organic cation transporters, as well as novel type/carnitine transporters. Moreover, additional genetic alterations in hyperuricemia and gout associated with PDZK1 likely occurs through its modulation of the apical membrane localization of URAT1.55 Research has shown that individuals with renal hypouricemia and loss-of-function mutations in URAT1 demonstrate incomplete responses to both pyrazinamide and uricosurics, resulting in average concentrations reaching 0.93 mg/dL.185

GLUT9

GLUT9 functions as the principal transporter for urate efflux across the basolateral membrane of the proximal tubule in the kidney, facilitating transepithelial urate absorption.186 The pronounced lack of renal reabsorption of filtered urate in hypouricemic patients with GLUT9 loss-of-function mutations provides compelling evidence of the critical role this protein plays in renal tubular urate reabsorption. In these individuals, the fractional excretion of urate approaches 150%, highlighting the predominant mechanism of tubular urate secretion in the absence of reabsorption.134

BCRP

BCRP is an efflux pump that is driven by ATP on the apical membrane proximal renal tubule and intestinal epithelial cells and is critical for UA excretion. Mutated or dysfunctional ABCG2 may lead to significantly reduced excretion, moderate hyperuricemia and metabolic syndrome.139 Initially, it was hypothesized that the loss or reduction of ABCG2-mediated renal urate secretion would result in increased renal urate reabsorption, as diminished renal excretion is typically considered the primary mechanism of hyperuricemia in most gout patients. However, hyperuricemic patients with varying degrees of ABCG2 dysfunction, categorized by genotypes of dysfunctional SNPs, exhibit hyperuricemia characterized by urate overproduction. This is evidenced by elevated urinary urate excretion and a fractional excretion exceeding 5.5%. Additionally, ABCG2 dysfunction appears to contribute to renal underexcretion of urate in patients with milder functional impairments, also classified by genotype.136

OAT1, OAT3 and OAT4

OAT1 and OAT3, located on the basolateral membrane of the proximal tubule, function as urate/dicarboxylate exchangers responsible for uric acid excretion. Additionally, OAT4 participates in the transport of high-affinity binding steroids such as estrone sulfate (ES).187 This transporter operates as a chloride-ion-dependent exchanger for both ES and uric acid. Physiologically, OAT4 facilitates uric acid excretion in the proximal tubule by orchestrating ion exchange processes such as PAH/Cl-, PAH/ES, and potentially PAH/UA interactions. Its interplay with NHE3 and sodium dicarboxylate transporter 1 contributes to the regulation of intracellular α-ketoglutarate levels.134

NPT1 and NPT4

NPT1, which exhibits a weak to moderate correlation with altered uric acid levels, facilitates both the absorption and efflux of urate. It functions as a chloride-dependent urate transporter, which is involved in sodium/phosphate cotransport activities.188 NPT4 is crucial in urate excretion, working synergistically with basolateral organic anion transporters 1 and 3 (OAT1/OAT3). Uric acid was absorbed by OAT1 and OAT3 into tubular cells, which is subsequently transported into the urinary lumen by NPT4.189

PDZK

Polyvalent PDZ domain 1 (PDZK1) is a multidomain protein with four PDZ domains, primarily located at the apical membrane of kidney proximal tubule cells. It is abundantly expressed in this region and engages directly with several apical transporters, such as URAT1 and NPT1.134 As a scaffold protein, PDZK1 significantly regulates the activity of various transport proteins within the proximal tubules. Additionally, PDZK1 is proposed as a potential upstream regulator of ABCG2, impacting its function in the small intestine. Specifically, the upregulation of ABCG2 expression‎ and function in response to soluble uric acid in intestinal cell lines is dependent on PDZK1 at the transcriptional level.188

These genes are specifically expressed on the apical membrane of renal proximal tubule cells, which are crucial for the secretion of uric acid into the glomerular filtrate, as depicted in Fig. 4. Beyond the genes that encode for these transporter proteins, over a hundred genetic loci have been associated with hyperuricemia. Genome-wide association studies provide a comprehensive and unbiased method for pinpointing genetic factors linked to urate regulation and metabolism.190

Fig. 4

Uric acid undergoes a dynamic process of elimination and reabsorption, primarily orchestrated by the kidneys (two-thirds) and the intestines (one-third). In the nephron, filtration of water and solutes occurs within the glomerular capsule, followed by tubular reabsorption, predominantly mediated by the proximal convoluted tubule. Concurrently, tubular secretions extract uric acid from peritubular capillaries, secreting it into the tubular fluid for urinary excretion. Urate transporters in renal proximal tubule epithelial cells actively mediate the secretion and reabsorption of urate, thus determining the net excretion levels from the kidney. In the renal proximal tubule, SLC22A12 (URAT1), SLC17A1 (NPT1), and SLC22A11 (OAT4) located on the apical membrane facilitate reabsorption. SLC2A9 (GLUT9), found in both the apical and basolateral membrane tubules, is a long isoform that mediates the basolateral efflux of urate back into circulation. For excretion, SLC22A6 (OAT1) and SLC22A8 (OAT3) on the basolateral membrane facilitate urate entry into the renal tubules. ABCG2 (BCRP) and SLC17A3 (NPT4), positioned on the apical side, contribute to the secretory transport of urate into the tubule lumen for urinary excretion. In intestinal metabolism, uric acid is actively secreted into the intestinal lumen primarily by the transporter ABCG2, underscoring the role of the intestines in urate homeostasis

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Hyperuricemia and diseases

An elevated uric acid concentration above physiological levels can pose a potential risk factor for several diseases closely associated with metabolic disorders. Numerous epidemiological studies have suggested that hyperuricemia may correlate with hypertension, metabolic syndrome, insulin resistance, dyslipidemia, type II diabetes, kidney disease, and cardiovascular events including coronary heart disease and cerebrovascular disease.191,192,193,194,195,196,197,198,199 Studies have demonstrated that serum uric acid levels can also predict the onset of hypertension, diabetes, obesity, and renal disorders74,200,201 (Table 3).

Table 3 The mechanisms of conditions caused by hyperuricemia

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Mendelian randomized studies

A significant biomedical question is whether hyperuricemia is causally associated with related comorbid conditions such as gout, hypertension, cardiac and kidney disease, etc.202,203,204,205,206,207,208,209 Utilizing data from observational epidemiologic studies in conjunction with experimental evidence from in vitro and animal model investigations, elevated serum urate levels have been suggested as being potentially linked to concurrent metabolic disorders.210 The principles of Mendelian randomization, which leverages genetic variants influencing exposures (e.g., UA levels), can serve as a natural randomization method to study the causal effects of these exposures on disease outcomes.21,211,212 To investigate the association between elevated serum urate concentrations and comorbid metabolic conditions, Mendelian randomized studies were conducted using genetic variants linked to increased serum urate levels.213,214,215 These genetic variants act as proxies for prolonged urate exposure, assuming they remain unconfounded by other factors.18,22,206,216 The pioneering Mendelian randomization studies leveraged specific genetic variants with substantial impacts on serum uric acid levels as instrumental variables. The objective of their research was to investigate the associations between uric acid concentrations and various health conditions, including body mass index, bone mineral density, coronary artery disease, blood pressure, metabolic syndrome, blood glucose levels, triglyceride levels, diabetes mellitus, serum creatinine levels, estimated glomerular filtration rate, Parkinson’s disease, memory, and gout.207,212,217,218,219,220 However, over the past three years, Mendelian randomization studies have utilized genetic variants associated with serum uric acid levels, identified through genome-wide association studies (GWAS), to construct genetic risk scores. These investigations consistently indicate a lack of evidence supporting a causal relationship between elevated serum urate levels and the risk of developing type 2 diabetes mellitus, coronary heart disease, ischemic stroke, and heart failure.17,221,222,223 Li et al.22,169 conducted a comprehensive analysis of 107 Mendelian randomization studies, included a median of 7,158 participants and 2,225 cases, with serum uric acid level as the exposure variable for various health outcomes. The instrumental variables utilized in these studies explained 2% to 6% of the variability in serum uric acid levels. The results indicated a significant association between serum uric acid levels and four health outcomes: diabetic macrovascular disease, arterial stiffness, renal events, and gout. Particularly noteworthy was the robust association observed with gout. However, the study did not find significant associations with several common cardiac and metabolic disorders, including type 2 diabetes, hypertension, chronic kidney disease, ischemic heart disease, and congestive heart failure.224,225,226,227,228,229,230,231,232,233,234,235,236,237,238 These findings suggest that while elevated serum uric acid levels may be associated with certain health outcomes such as gout and renal diseases, the evidence does not strongly support a causal relationship with other metabolic disorders. Additional analyses have shown consistent results across most outcomes examined, which included a variety of cardiovascular diseases, such as incidence of atrial fibrillation,239 coronary heart disease, incidence of hypertension,216 and incidence of stroke,71 diabetes,240 chronic kidney disease,222 mild cognitive impairment, Parkinson’s disease,241 and multiple sclerosis.21 However, statistical significance was inconsistent in the two outcomes of diabetic neuropathy5,218 and Alzheimer’s disease.242 In particular, the role of genetic variants, such as those within the SLC2A9 gene, in influencing cardiovascular and metabolic outcomes remains subject to debate.6,191,223,243,244 Recent research has delved into the causal relationship between variants of the URAT1 transporter gene (SLC22A12) and obesity and metabolic syndrome.245,246 In a randomized controlled trial involving patients with essential hypertension, specific SLC22A12 single nucleotide polymorphisms (SNPs), such as rs11602903, were associated with higher body mass index (BMI), larger waist circumference, higher HDL cholesterol levels, and the presence of metabolic syndrome in individuals of European descent.247,248,249 However, these associations were not observed in non-European populations, underscoring potential ethnic differences in genetic susceptibility to hyperuricemia-related metabolic abnormalities.250,251,252

UA induced inflammation and relative mechanism

Uric acid signaling triggers the activation of several transcription factors, such as NF-κB or AP-1, through the activation of MAPK p38 and ERK pathways, resulting in the production of reactive oxygen species (ROS) under the conditions of hyperuricemia.78 The NLRP3 inflammasome, part of the nucleotide-binding domain and leucine-rich repeat protein family complex, is essential in the development of numerous infections and inflammatory disorders.116,253,254,255,256 The expression‎ of NLRP3 is induced by NF-κB activation, leading to the assembly of a complex with the adaptor protein ASC and procaspase-1.85,91,114,257 Subsequently, procaspase-1 transforms into its mature form, caspase-1. This enzyme then activates pro-IL-1β and pro-IL-18, converting them into their mature forms, IL-1β and IL-18, respectively. This process coincides with the initiation of pyroptosis, facilitating the release of IL-1β into the extracellular environment.258,259 In gout, the activation of the NLRP3 inflammasome by monosodium urate (MSU) crystals stimulates the release of IL-1β, which contributes to the progression of arthritis. This activation mechanism involves phagocytic cells such as macrophages and neutrophils.260,261,262,263,264 This cascade of events leads to enhanced transcription of innate cytokines in various cell types including vascular endothelial cells, smooth muscle cells, and adipocytes. The activation is linked to the generation of vasoconstrictive agents, including MCP-1, (pro)renin receptor, endothelin, and angiotensin II, while concomitantly diminishing vasodilatory compounds like nitric oxide, which may contribute to the development of hypertension and lead to decreased viability of cardiomyocytes and myocardial damage.94,265,266,267 Moreover, in vascular cells, upregulation of growth factors like PDGF has been noted, which can promote smooth muscle cell proliferation and atherosclerosis.268 In vascular smooth muscle cells, uric acid-induced activation of MAPKs promotes the expression‎ of MCP-1, an important chemokine involved in atherosclerosis progression. In pancreatic β-cells, uric acid triggers ERK activation, resulting in reduced cell viability, apoptosis, and the production of reactive oxygen species.78,269,270 Treatment with a URAT1 inhibitor suppresses the ERK pathway and mitigates uric acid-induced cell damage, underscoring the involvement of intracellular uric acid in MAPK activity.271,272,273,274 Additionally, uric acid regulates MAPK through phosphatase activity that inhibits the MAPK pathway.275,276 Monosodium urate crystals are ingested by monocytes via phagocytosis, engaging Toll-like receptors (TLRs) such as TLR2 and TLR4. This interaction prompts the recruitment of the adaptor protein ASC to the NLRP3 inflammasome complex. Subsequently, caspase-1 is drawn to the ASC assembly, where it oligomerizes along the ASC filaments. This oligomerization triggers the autoproteolytic maturation of caspase-1, activating its inflammatory caspase function.183,277 Active caspase-1 then catalyzes the proteolytic cleavage and maturation of proIL-1β into the biologically active IL-1β, which leads to acute flares of gouty arthritis.183 In neutrophils, uric acid activates the ERK/p38 signaling pathway while inhibiting the Nrf2 pathway. Additionally, monosodium urate crystals induce the translocation of Nrf2 into the nucleus and modulate intracellular reactive oxygen species levels, thereby promoting the activation of the NLRP3 inflammasome. This ROS-induced injury can lead to apoptosis, disruptions in ion regulation, and mitochondrial dysfunction, further exacerbating the inflammatory response and tissue damage.67,278 Furthermore, resolution of gout flares involves the formation of neutrophil extracellular traps, which capture monosodium urate crystals. Uric acid can modulate cytokine production and inflammatory outcomes through various pathways.253,279,280 Uric acid can enhance AKT phosphorylation, which subsequently leads to PRAS40 phosphorylation with the activation of mTOR,281 resulting in the inhibition of autophagy, as well as inhibiting AMPK phosphorylation.282 When UA levels are elevated, RAGE signaling is stimulated, leading to the activation of nuclear factor-kappa B (NF-κB). NF-κB activation triggers the transcription and release of pro-inflammatory cytokines within endothelial cells. Additionally, UA-induced activation of RAGE promotes the expression‎ and extracellular release of high mobility group box 1 protein (HMGB1) by endothelial cells, lymphocytes, monocyte-derived macrophages, and vascular smooth muscle cells.87,283,284 The interaction between HMGB1 and RAGE amplifies the inflammatory cascade, contributing to cell apoptosis and endothelial dysfunction, resulted to CVD or CKD.277,285 This dysregulation of the HMGB1-RAGE pathway further diminishes NO availability, exacerbating inflammation. Moreover, UA-induced inflammation and oxidative stress can also trigger endoplasmic reticulum (ER) stress, decreased nitric oxide bioavailability and produce peroxynitrite (ONOO-), a very powerful radical, which contributing to cellular dysfunction and apoptosis.61,103,270,282 Uric acid diminishes nitric oxide levels through several mechanisms, including the consumption of NO due to excessive reactive oxygen species production and direct inhibition of NO synthesis. UA-induced dephosphorylation of endothelial NO synthase (eNOS) via uric acid transporters reduces NO production in human umbilical vein endothelial cells. Moreover, the HMGB1-receptor for advanced glycation end products pathway regulates eNOS production14,98,286,287 (Fig. 5).

Fig. 5

The role of uric acid in the pathogenesis of hyperuricemia and its associated diseases involves complex intracellular signaling mechanisms. Elevated intracellular uric acid levels stimulate the production of reactive oxygen species and activate multiple inflammatory signaling pathways. XO xanthine oxidase, eNOS endothelial nitric oxide synthase, MSU monosodium urate, Nrf2 Nuclear factor-erythroid 2-related factor 2, mTOR mammalian target of rapamycin complex, ERK extracellular signal-regulated kinase, AMPK AMP-activated protein kinase, IL-1β interleukin-1β, MAPK mitogen-activated protein kinases, PRAS40 Proline-Rich AKT Substrate, NF-κB nuclear factor κB, TLR Toll-like receptors, NLRP3, NOD-, LRR- and pyrin domain-containing 3, PKC Protein Kinase C, RAGE Receptor for Advanced Glycation End Products pathway

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Biomarkers of hyperurceimia and its relative disease

Recent advances in proteomics have shed light on the biochemical underpinnings of hyperuricemia. Notably, Liu’s288 research indicated elevated serum levels of complement C3, haptoglobin, complement C4, and apolipoprotein A1 (apo A1) in Uyghur patients with hyperuricemia. This suggests a correlation between hyperuricemia and high-density lipoprotein (HDL) components, with apo A-I implicated in cholesterol transport and anti-atherosclerotic properties.289,290,291 Furthermore, HDL’s role in lipid metabolism regulation and its influence on cardiovascular disease and diabetes development cannot be overlooked.292 The inhibition of apo A-I may be linked to atherosclerosis progression through chronic inflammation pathways. Moreover, the complement system’s activation in response to hyperuricemia has been implicated in the pathogenesis of various inflammatory conditions, including gout, renal injury, and type 2 diabetes (T2DM).144 The NLRP3 inflammasome’s activation and its interplay with the complement and coagulation systems are of particular interest. Component C5a of the complement system, recognized for its potent pro-inflammatory effects, can amplify monocyte and neutrophil activation. MSU crystals have been shown to trigger IL-1β production and inflammatory cytokine release through C5a activation, highlighting the potential of complement antagonists in managing gout inflammation. In the realm of urine proteomics, Huo et al.293 conducted a comparative study between healthy individuals and those with hyperuricemia, revealing differentially expressed proteins that hint at pathways involved in insulin receptor recycling and lipid metabolism. The study pinpointed the V-type proton ATPase subunit B kidney isoform and Complex Factor D (CFAD or adipsin) as key factors impacting insulin regulation in hyperuricemia patients.

Cardiovascular metabolic mechanisms and diseases

In recent years, numerous studies have reinforced the strong association between hyperuricemia and cardiovascular events. Research has demonstrated that serum uric acid levels are positively correlated with hypertension.265,294,295 The proposed mechanisms involve the activation of the renin-angiotensin system, inflammatory responses, oxidative stress, vascular smooth muscle cell proliferation, and insulin resistance.57,69,78,94,296 The ONATA study showed a negative correlation between serum uric acid levels and insulin sensitivity, suggesting a potential link between uric acid, insulin sensitivity, and the risk of developing hypertension.105,212 Hyperuricemia frequently coexists with insulin resistance, which can elevate the activity of the renin-angiotensin-aldosterone system and the sympathetic nervous system. This interaction leads to sodium retention, increased blood volume, and subsequent hypertension.297,298 In patients with hyperuricemia, elevated serum levels of high-sensitivity C-reactive protein (hs-CRP) are closely linked to inflammation and oxidative stress, which may exacerbate hypertension.299 Soluble urate may further exacerbate vascular inflammation and oxidative stress by promoting LDL oxidation, lipid peroxidation, and elevating hs-CRP levels. Moreover, hs-CRP can contribute to vascular endothelial injury by activating the complement system.99,287 Furthermore, elevated uric acid levels have been implicated in causing inflammation in endothelial cells via the activation of the receptor for advanced glycation end products (RAGE) signaling pathway.285 When UA levels are increased, RAGE signaling becomes activated, that ultimately lead to endothelial dysfunction, is a key feature of various cardiovascular diseases. Specifically, the activation of RAGE triggers the nuclear factor-kappa B pathway, resulting in the transcription and release of proinflammatory cytokines within endothelial cells.277,285 To mitigate UA-induced endothelial dysfunction and inflammation, targeting the RAGE signaling pathway offers a promising therapeutic strategy. Employing anti-RAGE antibodies to inhibit RAGE activity can suppress the HMGB1/RAGE signaling axis, thereby alleviating endothelial dysfunction and diminishing inflammation within endothelial cells.285,300,301(Fig. 5) By modulating this pathway, it may be possible to alleviate the detrimental effects of elevated UA levels on endothelial function and reduce associated cardiovascular risks.105,265,302

Elevated serum uric acid levels heighten the risk of cardiovascular disease (CVD) mortality, potentially due to mechanisms by which hyperuricemia activates the renin-angiotensin system and induces hypertension. Additionally, uric acid has been detected in atherosclerotic plaques.102,201 A recent study conducted in the Japanese revealed that even among healthy, lean, normotensive individuals, the presence of hyperuricemia is associated with an elevated risk of cardiometabolic disease.191 Kleber et al. reported a significant association between each 1 mg/dL increase in genetically predicted uric acid concentration and the risk of cardiovascular death and sudden cardiac death.207 Emerging evidence has linked elevated serum uric acid levels to cardiovascular diseases, particularly atherosclerosis and hypertension. Chronic low-grade inflammation is a hallmark of atherosclerosis, and UA-induced IL-1β release may contribute to this inflammatory milieu.69,90,239,303 Additionally, uric acid has been associated with endothelial dysfunction, which further exacerbates vascular inflammation and contributes to hypertension.237,304,305,306,307,308 Endothelial dysfunction characterized by impaired nitrogen oxide-mediated vasodilatation is a key event in the development of atherosclerosis.94 Experimental and clinical research has substantiated that elevated uric acid levels exert detrimental effects on cardiovascular health, with increased oxidative stress being a key mechanism implicated in these adverse outcomes,6,66 decreased nitric oxide availability, endothelial dysfunction, the promotion of local and systemic inflammation, vasoconstriction, vascular smooth muscle cell proliferation, insulin resistance309 and metabolic disorder.51,124 Additionally, endothelial dysfunction associated with elevated serum uric acid levels leads to a low-grade inflammatory state and vascular activation of the angiotensin system. As estrogen production declines with age in females, its cardio-protective effects may diminish, thereby increasing susceptibility to elevated uric acid levels.307

Renal metabolic mechanisms and diseases

Emerging evidence increasingly supports the pathogenic role of hyperuricemia in both the onset and progression of chronic kidney disease (CKD). Untreated hyperuricemia is notably acknowledged as a risk factor for the development of CKD. In China, the preval‎ence of hyperuricemia among CKD patients varies from 36.6% to 50%, with a notable rise observed as CKD progresses.310 The mechanisms by which hyperuricemia contributes to chronic kidney disease include renal inflammation, endothelial dysfunction, and activation of the renin-angiotensin system.13 Hyperuricemia is known to stimulate the renin-angiotensin system and impair endothelial nitric oxide release, which collectively lead to renal vasoconstriction and increased blood pressure.100 Nitric oxide (NO) plays a crucial role in regulating vascular endothelial cell relaxation, maintaining stable renal vascular tone, and influencing renal blood flow, renin secretion, and tubuloglomerular feedback mechanisms.105,311 However, hyperuricemia inhibits nitric oxide synthase, leading to reduced nitric oxide levels.312 Furthermore, endothelial cells respond to hyperuricemia by upregulating angiotensin-converting enzyme activity, which enhances angiotensin II and superoxide anion production. This cascade promotes vasoconstriction and hypertension.102,313 Uric acid directly affects endothelial cells by reducing nitric oxide levels, influencing processes such as vascular smooth muscle cell proliferation, extracellular matrix deposition, and the adhesion and migration of macrophages.102,227,228,314,315,316,317 These effects lead to arterial resistance and remodeling, ultimately contributing to renal dysfunction and fibrosis.6,318 However, the evidence supporting the treatment of asymptomatic hyperuricemia in hypertensive patients with chronic kidney disease is limited. Observational studies have produced inconsistent findings, and there is a notable absence of large-scale randomized controlled trials to validate the efficacy of lowering uric acid levels. Despite these limitations, the majority of existing studies suggest that therapies aimed at reducing uric acid levels may potentially attenuate the progression of CKD.102,319,320,321 A single-center double-blind, randomized, parallel placebo-controlled study found that uric acid reduction slowed the decline of glomerular filtration rate in patients with stage 3 and 4 CKD.322 Another study by Jeong et al. demonstrated that febuxostat treatment to reduce serum uric acid levels tended to reduce renal functional deterioration in patients with both CKD and hyperuricemia.323 These findings suggest that reducing uric acid levels could potentially improve renal function. However, ongoing debate centers on whether the benefits of uric acid-lowering therapy stem from decreased uric acid levels or the inhibition of XO activity.319,324,325 Further investigations have shown that medications like benzbromarone and febuxostat can mitigate the advancement of chronic kidney disease and decrease serum uric acid levels in CKD patients, highlighting the potential advantages of treatments aimed at lowering uric acid levels.319,326,327,328

Increased uric acid levels are linked to kidney inflammation and the progression of kidney diseases, especially in the presence of hyperuricemia. Gout has been identified as an independent risk factor for chronic kidney disease, nephrolithiasis and acute kidney injury, wherein uric acid excretion by the kidneys participate in facilitating crystal-induced direct tubular toxicity.310 This finding underscores the close interconnection between uric acid and nitric oxide regulation in this particular clinical context.329 Kidney damage mediated by UA involves the stimulation of the renin-angiotensin-aldosterone system. In the medulla, an elevated UA concentration results in the deposition of urate precipitates and the activation of the Nod-like receptor protein 3 (NLRP3) inflammasome.96 Activation of these pathways leads to chronic interstitial inflammation and tubular damage, ultimately contributing to kidney fibrosis. Additionally, in the renal cortex, hyperuricemia amplifies the activity of the renin-angiotensin-aldosterone (RAA) system, fostering sustained vasoconstriction of the afferent arterioles.130 In turn, leads to glomerular damage and the development of glomerulosclerosis.330 CKD is characterized by endothelial dysfunction and NO deficiency; thus, uric acid is a potential contributor to CKD progression. It is primarily driven by the development of hypertrophy in the afferent arteriole, which compromises autoregulation and facilitates heightened transmission of systemic blood pressure to the glomerulus.310 The kidney’s susceptibility to oxidative stress stems from various sources including the mitochondrial respiratory complex, NADPH oxidases, endothelial nitric oxide synthase (eNOS), myeloperoxidase, and xanthine oxidoreductase (XOR), all of which contribute to the advancement of chronic kidney disease and its related complications.331 Oxidative stress is a characteristic feature of chronic kidney disease, initiating inflammation and endothelial dysfunction, which accelerates arteriosclerosis. This sequence plays a role in glomerular injury, leading to albuminuria and eventual glomerulosclerosis. Hyperuricemia exacerbates oxidative stress, thereby intensifying inflammation and endothelial dysfunction within this context.332

Gout and its mechanism

Gout is one of the most common forms of chronic degenerative disease of the joints.333,334 It is defined by recurring episodes of inflammatory arthritis affecting joints and specific soft tissues, including cartilage, synovial bursae, and tendons, particularly in the lower extremities, due to the deposition of uric acid in the form of monosodium urate crystals.34 The painful pathological state of gout is mainly induced by hyperuricemia with the concentration of more than 6.8 mg/dL under physiological conditions (37 ◦C, pH 7.4).333,334 When uric acid levels increase to such concentration, crystals form in the joints, triggering an inflammatory response. MSU crystals display a triclinic structure composed of stacked sheets of purine rings, forming needle-shaped crystals observable under microscopy. The exposed, charged surfaces of these crystals are thought to promote interactions with phospholipid membranes and serum factors, thereby contributing to the inflammatory response mediated by these crystals.335 MSUs serve as the primary stimuli for initiating, amplifying, and sustaining the innate immune response. They are phagocytosed by macrophages as foreign particles and recognized by Toll-like receptors 2 and 4 (TLR2/TLR4), which subsequently activate and oligomerize the NLRP3 complex.336 The NLRP3 complex, a multiprotein assembly with proteolytic activity, facilitates the conversion of the pre-IL-1β into its active form, IL-1β. Subsequently, IL-1β is released into the extracellular milieu, initiating acute inflammation.337 The MSU crystals are initially engulfed by macrophages, which then facilitate the assembly and activation of the NLRP3 inflammasome, preceded by priming through pathways that activate NF-κB, such as those initiated by the engagement of Toll-like receptors (TLRs) within the TLR family.338,339,340 Inflammasomes are intracellular multiprotein complexes that trigger inflammatory responses. These structures emerge as intracellular pattern recognition receptors (PRRs) like NLRP3 detect signals that have infiltrated the cell’s cytosol.341 The recognition triggers the PRR to oligomerize and associate with a complex comprising adaptor proteins and effector enzymes.342,343,344 The formation of the NLRP3 inflammasome involves the recruitment of the adaptor protein ASC, which is then followed by the recruitment of caspase-1.345 Following initial oligomerization within the inflammasome structure, ASC monomers can subsequently polymerize into high-molecular-weight aggregates.341,346 The recruitment and oligomerization of caspase-1 by this complex initiate the activation and proteolytic cleavage of its substrates. Caspase-1 activates proinflammatory cytokines such as IL-1β by cleaving their respective precursor proteins and proIL-1β.262 In gout, the release of IL-1β mediated by inflammasomes triggers a significant inflammatory response characterized by vasodilation and rapid recruitment of neutrophils to the site of crystal deposition, thereby driving acute inflammatory episodes.347,348,349 Similarly, MSU promotes the expression‎ of other cytokines, such as interleukin-6 (IL-6), tumor necrosis factor-α (TNF-α), and interferon gamma (IFN-γ), and chemokines, such as monocyte chemotactic protein-1 (MCP-1). MCP-1 induces the recruitment of innate immune cells and indirectly affects gout progression.214 Flare resolution involves the capture of MSU crystals by neutrophil extracellular traps.350

Diabete and its mechanism

Chronic hyperuricemia is associated with pancreatic β-cell dysfunction, which is a critical component of type 2 diabetes.4 Research indicates that the likelihood of developing diabetes rises by 6% with each 1 mg/dL increment in uric acid concentration.240 Uric acid has been observed to adversely affect β-cells, resulting in impaired insulin secretion and decreased functional β-cell mass. This contributes to an insufficient compensatory response to insulin resistance and gluconeogenesis, mediated by the inhibition of hepatic AMP-activated protein kinase, thereby promoting the progression towards overt diabetes.351 Uric acid can promote oxidative stress, generating reactive oxygen species that cause cellular damage.122 Oxidative stress is closely associated with insulin resistance and β-cell dysfunction. The increased oxidative load in hyperuricemia may impair insulin sensitivity and exacerbate the metabolic disorders observed in diabetes.309 Moreover, hyperuricemia frequently coincides with low-grade inflammation. Increased uric acid concentrations have been implicated in the release of inflammatory cytokines, thereby contributing to systemic inflammation. Inflammation is a well-recognized contributor to the pathogenesis of insulin resistance and type 2 diabetes. This inflammatory environment disrupts insulin signaling pathways and exacerbates glucose intolerance. Elevated insulin levels, stemming from insulin resistance and β-cell dysfunction, may enhance the renal reabsorption of uric acid. Consequently, this cycle potentially reinforces higher serum uric acid levels, establishing a feedback mechanism in the interplay between hyperinsulinemia and hyperuricemia.352 Additionally, research has shown that elevated uric acid levels inhibit insulin-induced glucose uptake in cardiomyocytes. This effect is primarily mediated by an increase in the phosphorylation of insulin receptor substrate 1 (IRS1) and a concomitant inhibition of Akt phosphorylation, a crucial component of the insulin signaling pathway.353 Moreover, clinical research has identified a correlation between hyperuricemia and diabetes, although the causal relationship remains controversial. While high UA may accelerate the development of diabetes and impair glucose tolerance, it is insufficient to solely induce diabetes.19,351,354

Metabolic syndrome (MetS) and its mechanism

Metabolic syndrome is characterized by a cluster of conditions, including obesity, insulin resistance, and dyslipidemia, and is intimately linked to chronic inflammation.355 The preval‎ence of metabolic syndrome rises by approximately 5% in men and 9% in female with each 1 mg/dL increase in serum uric acid concentration.356 Elevated serum uric acid levels have been shown to impair insulin sensitivity, thereby contributing to the development of insulin resistance. In response to increased insulin resistance, the pancreas compensates by secreting higher levels of insulin, resulting in hyperinsulinemia.357 The preval‎ence of metabolic syndrome components, including hyperglycemia, hypertriglyceridemia, low HDL cholesterol, and hypertension, shows a rising trend with increasing serum uric acid levels. Interestingly, central obesity appeared to decrease slightly in individuals with exceptionally high serum uric acid concentrations.200 Uric acid is implicated in the pathogenesis of metabolic syndrome through its ability to induce insulin resistance and promote low-grade inflammation, underscoring its proinflammatory role.51 In addition, hyperuricemia is frequently accompanied by dyslipidemia, another hallmark of metabolic syndrome. Studies have demonstrated an association between elevated serum uric acid levels and alterations in lipid profiles, including increased triglycerides and decreased high-density lipoprotein cholesterol (HDL-C) levels.358 These lipid abnormalities contribute to the dyslipidemia pattern often observed in individuals with metabolic syndrome. There is evidence to suggest that hyperuricemia may promote weight gain and central obesity, both of which are integral components of metabolic syndrome. Uric acid has been shown to influence adipogenesis and fat accumulation, potentially exacerbating obesity in individuals with MetS.200

Hypertension and its mechanism

Hyperuricemia may acutely influence blood pressure through a renin-dependent pathophysiological mechanism. Additionally, it is postulated that hyperuricemia exacerbates hypertension by promoting systemic endothelial dysfunction and oxidative stress.201 Epidemiological studies consistently demonstrate a robust association between hyperuricemia and the incidence of hypertension. Each 1 mg/dL rise in serum uric acid is linked to a 13–15% increase in hypertension risk.299 Elevated serum uric acid levels constitute a substantial risk factor for both the onset and progression of hypertension. The precise mechanisms by which elevated uric acid concentrations lead to hypertension are not entirely understood but likely involve complex processes related to cardiovascular disease pathogenesis. The increase in blood pressure in hyperuricemic individuals is predominantly attributed to oxidative stress and intracellular urate activity, mediated chiefly by xanthine oxidoreductase (XOR).299 Uric acid deposition-induced inflammation, resulting in endothelial dysfunction and vascular damage (referred to as vascular gout), can occur at serum uric acid levels exceeding 6.5 mg/dL. This threshold is notably higher than those typically linked with hypertension and cardiovascular disease.201 Uric acid-lowering therapy effectively reduces both systolic and diastolic blood pressure in pediatric and adolescent patients newly diagnosed with essential hypertension, particularly in young individuals with a short duration of hypertension and preserved renal function.200

Intervertebral degeneration (IVD) and its mechanism

Several studies have confirmed that the oxidative properties of physiological levels of UA can eliminate 60% of ROS in the body.359 This reduction in ROS can inhibit autophagy in IVDs and reduce the apoptosis of myeloid cells caused by oxidative stress, maintaining the stability of the structure of IVD.94 However, high concentrations of UA can promote oxidative stress and mitochondrial dysfunction. The induction of XO can promote the production of ROS, thus promoting oxidative stress in IVD and exacerbating IDD. Moreover, high osmolality induced by high uric acid levels may inhibit PDGF- and IGF-I-mediated DNA synthesis in the medulla oblongata.268 Additionally, MSU crystals may accumulate in IVD under high uric acid conditions and cause damage to cone endplates.360 MSU crystals cause cellular damage and mediate inflammatory responses, such as prostaglandin, bradykinin, IL-1, IL-6, and TNF-a.337 The accumulation of inflammation and bone destruction affect the ability of cartilage endplates to provide nutrients to IVD, exacerbating IDD.361

Therapy approaches for hyperuricemia

Hyperuricemia can manifest either asymptomatically or symptomatically, leading to distinct management approaches.95 Thus, the management strategies for hyperuricemia typically involve two primary modalities: non-pharmacological interventions and pharmacological therapy. These approaches are tailored based on the clinical presentation and individual patient factors, aiming to mitigate the risk of complications.362

Treatment of asymptomatic hyperuricemia

Non-pharmacological interventions play a crucial role in managing hyperuricemia, particularly in asymptomatic individuals.363,364 Dietary modifications, such as adherence to a low-purine diet and avoidance of alcohol, particularly beer and spirits, sugar-sweetened beverages, heavy meals, and excessive intake of meat and seafood, have demonstrated efficacy in reducing uric acid levels by approximately 10-15%.365 Furthermore, incorporating cherries, coffee, and low-fat dairy products into the diet can confer beneficial effects. Consumption of fructose-rich beverages should be minimized. Protein-rich vegetables like nuts, legumes, beans, spinach, cauliflower, and mushrooms can be consumed in moderation due to their low bioavailability of urate and high fiber content, which are less likely to elevate serum uric acid levels.324,366,367,368,369 However, complete prohibition of purine intake is not recommended due to its limited effect on serum uric acid levels (approximately 1 mg/dL) and the significant burden it imposes on patients.1 Instead, supplementation with vitamins such as ascorbic acid (vitamin C) and folic acid can help lower serum urate concentrations. Vitamin C, administered in doses ranging from 500 to 1000 mg/day, exhibits mild uricosuric properties and can complement dietary and lifestyle modifications. Similarly, folic acid supplementation has been shown to effectively reduce serum urate levels.9,127,370,371 Of note, non-pharmacological interventions represent valuable adjunctive measures for all individuals with gout, encompassing weight management and avoidance of excessive consumption of purine-rich foods, alcoholic beverages, and fructose-rich beverages. However, complete elimination of purine intake is not recommended due to its limited impact on serum uric acid levels, typically resulting in a reduction of approximately 1 mg/dL. Nonetheless, exceptional cases may require pharmacotherapy even in asymptomatic individuals with elevated serum uric acid levels.372 For instance, patients undergoing radiotherapy or chemotherapy for malignancies are at risk of uric acid nephropathy and may require preventive therapy with intravenous hydration and xanthine oxidase inhibitors.330,373,374 Xanthine oxidase inhibitors are typically used in such case. In Japan, treatment of asymptomatic hyperuricemia is recommended to mitigate the risk of chronic diseases such as hypertension, coronary artery disease (CAD), and chronic kidney disease (CKD).191 However, the decision to initiate pharmacotherapy for asymptomatic hyperuricemia remains debatable and should be based on individual risk factors and considerations. While recent studies suggest a potential association among hyperuricemia, cardiovascular and renal diseases, further research is needed to elucidate the mechanisms and clinical benefits of urate-lowering therapy in these populations.102,320,375

Treatment of hyperuricemia with commodities

An analysis of twenty-two guidance documents revealed a consensus on target serum uric acid levels for long-term control, with 6.0 mg/dL (or 360 μmol/L) as the predominant recommendation.362 Uric acid-lowering drugs can be broadly classified into three major groups: drugs that reduce uric acid synthesis (xanthine oxidase inhibitors), drugs that promote uric acid excretion (reabsorption inhibitors), and drugs that regulate uric acid metabolic hydrolysis (uricase inhibitors).1 Irrespective of the specific urate-lowering therapy (ULT) selected, fundamental principles entail commencing treatment concurrently with prophylaxis and initiating with a conservative dosage, followed by systematic monitoring of serum uric acid levels and subsequent dose adjustment until the therapeutic target is attained.310 For symptomatic hyperuricemia, the common pharmacological interventions for urate-lowering therapy (ULT) are illustrated in Fig. 4. Xanthine oxidase (XO) plays a central role in purine metabolism by catalyzing the conversion of hypoxanthine to xanthine and further to uric acid (UA). Concurrently, XO contributes to the production of reactive oxygen species (ROS).372 Allopurinol, categorized as a purine-like XO inhibitor, and febuxostat and topiroxostat, classified as non-purine XO inhibitors, constitute the primary pharmacological approach for ULT.326,376,377 By inhibiting XO activity, these agents demonstrate antioxidant properties by reducing ROS production associated with purine metabolism as well as remain the cornerstone of hyperuricemia treatment.139 Uricosuric agents represent a secondary or alternative therapeutic option, with recent guidelines advocating their use in combination with XO inhibitors when monotherapy proves ineffective.378 However, it is crucial to acknowledge that the predominant cause of hyperuricemia in most patients which is impaired renal clearance of uric acid. This impairment may be influenced by inherited renal transport factors or a reduced estimated glomerular filtration rate (eGFR).102,189,320,330 In patients with lower eGFR levels, uricosuric agents may not be as effective, necessitating the use of alternative agents with different mechanisms of action.379,380,381 Benzbromarone, another potent uricosuric drug, acts by inhibiting URAT1 and GLUT9.328,382 Emerging evidence linking hyperuricemia to cardiovascular and metabolic comorbidities has spurred the development of novel agents. Lesinurad and arhalofenate, inhibitors of URAT1 and OAT4, respectively, offer promising therapeutic avenues.383,384 Dotinurad, a selective urate reabsorption inhibitor available in Japan, inhibits URAT1 with high selectivity, demonstrating non-inferiority to febuxostat in lowering serum UA levels with no significant safety concerns385 (Table 4).

Table 4 Update on the therapies for the treatment of hyperuricemia

Full size table

Xanthine oxidase inhibitors (XOIs)

Xanthine oxidase catalyzes the conversion of purine metabolites to uric acid (UA). Therefore, xanthine oxidase inhibitors reduce UA production from both endogenous and dietary purine sources, making them the first-line therapies for managing hyperuricemia.23,55

Allopurinol

Allopurinol is an inhibitory agent that interferes with xanthine oxidase-mediated purine synthesis; allopurinol undergoes metabolic conversion to alloxanthine, which is a potent xanthine oxidase enzyme inhibitor.386 The dual action of allopurinol and its metabolite, alloxanthine, inhibits xanthine oxidase, effectively catalyzing the conversion of hypoxanthine to xanthine and its subsequent conversion to uric acid. Allopurinol is crucial for promoting the secondary utilization of hypoxanthine and xanthine through a metabolic pathway intricately linked with hypoxanthine-guanine phosphoribosyl transferase. This metabolic cascade contributes to the synthesis of nucleic acids and nucleotides, elucidating the multifaceted impact of allopurinol on purine metabolism.358 This metabolic process results in an increased concentration of nucleotides, triggering feedback mechanisms that suppress the synthesis of purines. Consequently, the reduced levels of uric acid in both urine and serum contribute to a reduction in the occurrence of hyperuricemia.383 The initial dose of 50 mg was given 1 ~ 2 times a day, and each time, the dose was increased by 50 ~ 100 mg. The general dose was 200 ~ 300 mg/d, divided into 2 ~ 3 doses, for a maximum daily dose of 600 mg.387 Notably, the CKD-FIX study and the PERL trials demonstrated that allopurinol did not significantly slow the deterioration of estimated glomerular filtration rate (eGFR) in chronic kidney disease patients compared to placebo, over a span of 2 and 3 years, respectively.388,389 However, a contrasting outcome was observed in a pediatric study where allopurinol treatment over four months led to an improvement in renal function in children with CKD.390 The ALL-HEART trial, which included patients over the age of 60 with ischemic heart disease but without a history of gout, found that allopurinol did not reduce the incidence of non-fatal myocardial infarction, non-fatal stroke, or cardiovascular death over an average follow-up period of 4.8 years when compared to standard care.391 Conversely, a smaller study involving 82 heart failure patients indicated that long-term allopurinol administration was associated with an improvement in left ventricular function.392 However, an algorithm was developed to theoretically mitigate the risk of allopurinol hypersensitivity syndrome (AHS), which occurs in 2–8% of patients.393 Allopurinol can cause severe cutaneous adverse reactions (SCARs), which is a primary concern associated with allopurinol use. SCARs are strongly correlated with the HLA B*5801 allele and include drug rash accompanied by eosinophilia and systemic symptoms, Stevens–Johnson syndrome, and toxic epidermal necrosis.394 In certain regions, a precautionary measure involves tailoring the allopurinol dosage based on creatinine clearance, aiming to mitigate the risk associated with SCARs, particularly considering renal failure as a predisposing factor for these adverse reactions. Notably, when allopurinol doses are less than 300 mg daily, less than half of patients achieve the therapeutic target of a serum uric acid (SU) concentration less than 6.0 mg/dL.395 Intriguingly, even in instances where allopurinol is not adjusted according to the estimated glomerular filtration rate (eGFR), approximately one-third of patients fail to attain SU levels below the designated threshold of 6.0 mg/dL. Nonetheless, a significant portion of patients receiving allopurinol fail to reach the target serum urate concentrations.396 Notably, the ABCG2 Arg141Lys variant has been consistently linked with poor response to allopurinol across multiple independent cohorts.397

Febuxostat

Febuxostat, a nonpurine xanthine oxidase inhibitor, effectively reduces serum uric acid levels without impeding the enzymes involved in pyrimidine and purine metabolism and synthesis. Its biotransformation is facilitated by uridine diphosphate glucuronosyltransferase (UGT) enzymes. Notably, patients treated with febuxostat demonstrate a slightly reduced risk of heart failure exacerbation compared to those receiving allopurinol.398 In China, febuxostat is recommended as a urate-lowering therapy and is prescribed at a daily dosage of 20–40 mg, contrasting with the global recommendation of 80-120 mg/day. In the United States, febuxostat is tolerated at doses of 40 and 80 mg per day, while in Europe it is 120 mg per day, and in Japan it is 10–60 mg per day.336 The CONFIRM‎S trial provided evidence that a daily dosage of 80 mg of febuxostat is more efficacious in lowering serum uric acid levels than a 300 mg daily dose of allopurinol.399 This nonpurine xanthine oxidase inhibitor is considered a viable alternative for individuals with allopurinol allergies. Notably, in scenarios of renal impairment, febuxostat is deemed more potent than allopurinol.326 Approximately 65% of patients achieved serum uric acid levels less than 6.0 mg/dL, although concerns have been raised regarding the cardiac safety profile of febuxostat.400 Common side effects of febuxostat encompass muscle pain, gastrointestinal discomfort, skin rashes, diarrhea, and a slight elevation in liver enzymes. Notably, the incidence of skin rashes is comparable to that observed with allopurinol. The manufacturer advises careful monitoring of liver function at the commencement of therapy and in the presence of any symptom’s indicative of liver injury. Importantly, the incidence of adverse effects associated with febuxostat remains low unless the daily dosage exceeds 120 mg.376 In the PRIZE trial, a cohort of 483 individuals with asymptomatic hyperuricemia was randomly assigned to either a two-year treatment with febuxostat or a control group that received lifestyle modifications. The study found that febuxostat did not correlate with a slowed progression of carotid intima-media thickness.401 However, a detailed sub-analysis revealed that the febuxostat group experienced a greater reduction in arterial stiffness parameters compared to the control group.402 Additionally, another sub-analysis indicated that patients on febuxostat treatment exhibited improved diastolic function.403 The FREED trial, involving 1070 elderly patients with hyperuricemia and cardiovascular risk factors, randomized participants to receive either febuxostat or non-febuxostat treatment. The results demonstrated that febuxostat was linked to a significantly reduced risk of the primary composite endpoint, encompassing cerebral, cardiovascular, renal events, and all-cause mortality.404

Topiroxostat

Topiroxostat, a nonpurine xanthine oxidase inhibitor, interacts with multiple amino acid residues within the solvent channel and forms covalent bonds with the molybdenum ion. This interaction produces a hydroxylated 2-pyridine metabolite that effectively inhibits xanthine oxidase, a critical enzyme in uric acid metabolism. Additionally, topiroxostat inhibits the ATP-binding cassette transporter G2 (ABCG2), which plays a key role in renal uric acid reabsorption and the secretion of uric acid from the intestines.394 However, topiroxostat has not received approval for use in the United States and Europe, although it is utilized in Japan. The medication is available in oral tablets of 20, 40, and 60 mg. The standard recommendation is to initiate treatment with a 20 mg dose administered twice daily, with a maximum approved dosage of 80 mg twice daily.387 The literature on topiroxostat reports certain adverse effects, including polyarthritis, nasopharyngitis, and an increase in liver enzymes. Notably, the majority of these adverse effects are generally classified as mild to moderate in severity.377 A study demonstrated a marked enhancement (≥150%) of warfarin activity in 32% of patients with cardiovascular disease and hyperuricemia who were treated with topiroxostat.405 A prospective, randomized, blinded study compared the effects of topiroxostat with allopurinol and suggested that topiroxostat may lead to a reduction in left ventricular end-diastolic pressure, indicating a potential benefit for cardiac function.406 Additionally, the study hinted at nephroprotective properties of topiroxostat compared to allopurinol. As for nephroprotection, an RCT on the use of febuxostat vs topiroxostat show none improvement in urinary protein/creatinine ratio.407

Advanced therapy

Hyperuricemia can arise due to either overproduction or underexcretion of uric acid, with the latter being the predominant form as mentioned. The underexcretion of uric acid is primarily attributed to diminished renal clearance.138,139 During renal filtration, uric acid is extensively handled by proximal tubular cells. Approximately 90% of the filtered uric acid is reabsorbed via the apical transporters URAT1 and OAT4, as well as the basolateral GLUT9. Conversely, a portion of uric acid is secreted back into the proximal tubular lumen through various apical transporters, including ABCG2, NPT1, NPT4, and GLUT9, along with the basolateral transporters OAT1 and OAT3.138,139 Uricosuric agents act on the proximal tubule of the kidney by inhibiting the reabsorption of uric acid or enhancing its excretion. These medications are considered second-line treatments for hyperuricemia, particularly in cases unresponsive to standard therapies. They are often used in conjunction with xanthine oxidase (XO) inhibitors or prescribed for patients who cannot tolerate XO inhibitors. Additionally, certain antihypertensive and lipid-lowering drugs, such as losartan, simvastatin, atorvastatin, and fenofibrate, have been shown to reduce serum uric acid levels, potentially exhibiting a synergistic effect when used alongside standard hypouricemic treatments.81,408

Probenecid

Probenecid is a quintessential uricosuric agent with multifaceted effects on renal function, significantly influencing the elimination of organic anions and tubular reabsorption of urate. Its therapeutic potential extends beyond managing hyperuricemia, demonstrating efficacy as a URAT1 and GLUT9 inhibitor, especially in cases of renal impairment. Probenecid exerts its uricosuric effects by inhibiting renal organic anion elimination and disrupting tubular urate reabsorption. This dual action enhances urinary uric acid excretion, thereby reducing serum urate concentrations. Additionally, probenecid may modulate urate binding by plasma proteins and influence uric acid secretion within the renal tubules.397 The comprehensive use of probenecid is not without consideration of adverse reactions, as it spans various organ systems. Gastrointestinal, dermatologic, hematologic, renal, and immunologic manifestations have been reported.409 Approximately 5% of users experience manifestations such as rash, gastrointestinal complaints, and hypersensitivity reactions. While serious toxicity is infrequently reported, a notable proportion of patients, approximately one-third, may exhibit intolerance, necessitating discontinuation of probenecid.410

Benzbromarone

Benzbromarone, recognized as a uricosuric agent, exhibits notable in vitro inhibitory effects on urate transport facilitated by URAT1 and GLUT-9. Its approval for clinical use comes with cautious considerations, particularly in terms of dosing and associated hepatotoxicity. The recommended starting dosages of benzbromarone range from 12.5 mg to 50 mg daily, a regimen predominantly observed in Europe and Asia.79,83,411 As novel URAT1 inhibitor uricosuric therapies gain momentum in clinical trials, particularly among Western populations, the application of benzbromarone warrants meticulous consideration. Patient selection for clinical trials should reflect the pathophysiologic subtype of hyperuricemia, existing comorbidities, and concurrent use of urine alkalization agents such as potassium citrate. This comprehensive approach facilitates a thorough eval‎uation of benzbromarone’s efficacy and safety across diverse patient cohorts, ultimately refining uricosuric therapy regimens.55 The risk of hepatotoxicity is especially increased in individuals administered high doses of 300 mg daily of benzbromarone. However, findings from a comprehensive systematic review indicates that, when juxtaposed with probenecid, benzbromarone is associated with a reduced frequency of adverse effects.378 Certain scholars posit that the removal of benzbromarone from the market may not align with the best interests of patients with gout, with the argument that conceivable toxicity could be mitigated through a cautious approach involving gradual dosage escalation coupled with vigilant monitoring of liver function.327 Importantly, similar to those treated with febuxostat, patients on benzbromarone exhibited a significantly reduced risk of advancing to end-stage renal disease.412 In an additional study, benzbromarone demonstrated a lower risk of experiencing the initial gout flare and developing type 2 diabetes when contrasted with allopurinol.413 A randomized, open-label, crossover study comparing benzbromarone and febuxostat in hyperuricemia patients indicated that benzbromarone was associated with diminished endothelial dysfunction and an increase in adiponectin levels.414

Emerging drugs and uricosuric compounds

Given the advancements in drug delivery systems and a deeper understanding of renal mechanisms and urate transporters, numerous novel therapeutic agents for managing hyperuricemia are currently in various stages of clinical development.372,415,416 Emerging pharmacological agents for hyperuricemia management are currently undergoing various stages of clinical development, ranging from preclinical to early clinical trials. Notable candidates in Phase II/III trials include arhalofenate (MBX102), AC201, the RDEA group (including lesinurad), tranilast, and ulodesine (BCX4208). Additionally, Phase I trials are eval‎uating drugs such as levotofisopam and Marine Active. The primary goal of these innovative therapies is to improve serum uric acid control in patients with symptomatic hyperuricemia, particularly those with comorbid conditions. These new agents aim to offer enhanced tolerability and minimize adverse events compared to traditional treatments. However, it is important to acknowledge that uricosuric agents and emerging therapies that increase renal clearance of uric acid may also raise the risk of renal adverse events.188

Lesinurad (RDEA594)

Lesinurad is a common URAT1 inhibitor that influences the serum uric acid concentration through the inhibition of URAT1 and OAT4.394 Lesinurad is metabolized and eliminated predominantly by the liver (75%) and to a lesser extent by the kidneys (25%), with a half-life of approximately 9 to 10 h. The primary treatment-emergent adverse events reported with its use include serious cardiovascular events and potential nephrotoxicity. Nonetheless, clinical studies have demonstrated that lesinurad at a dosage of 200 mg once daily does not elevate the risk of renal, cardiovascular, or other adverse events beyond those associated with xanthine oxidase (XO) inhibitors alone, with the exception of transient increases in serum creatinine levels.417 Nephrotoxicity emerges as the primary adverse effect associated with lesinurad, with its incidence being dose dependent. A recent Phase III clinical trial focused on gout patients who were intolerant or contraindicated to xanthine oxidase inhibitors (XOIs) revealed that lesinurad monotherapy at a dosage of 400 mg led to a significant incidence of elevated serum creatinine. Additionally, the trial reported renal-related adverse events, including serious adverse events, at a higher rate compared to the placebo group.383 However, Lesinurad is a relatively new pharmaceutical agent, currently lacks data regarding its potential impact on cardiovascular and renal outcomes.

Arhalofenate (MBX-102)

Arhalofenate (MBX-102) is a uricosuric compound that has been investigated for its potential in the treatment of gout and hyperuricemia. It acts as a dual-acting agent, combining the properties of a uricosuric and a nonsteroidal anti-inflammatory drug (NSAID). By inhibiting URAT1, arhalofenate promotes the excretion of uric acid in the urine, reducing serum uric acid levels.384 Furthermore, arhalofenate has anti-inflammatory properties, which can be beneficial in the context of gout, where inflammation plays a significant role in joint symptoms. However, clinical trials of arhalofenate have been conducted to assess its efficacy and safety in the treatment of gout and hyperuricemia. These trials aimed to eval‎uate its ability to lower serum uric acid levels, reduce gout flares, and provide anti-inflammatory effects.418 Arhalofenate is available for oral administration in daily dosages are 200, 400, or 600 mg once. The U.S. Food and Drug Administration (FDA) and the European Medicines Agency (EMA) respectively concurred with a pharmaceutical company on the efficacy endpoints for two distinct clinical indications of arhalofenate in 2017. Currently, three Phase III trials are in progress, designed to assess the comparative efficacy of a combination therapy consisting of arhalofenate plus febuxostat 40 mg versus febuxostat monotherapy at 80 mg. These trials aim to eval‎uate the reduction in serum uric acid levels and the incidence of gout flares.419

Dotinurad

Dotinurad represents a novel and selective urate reabsorption inhibitor that has received approval for clinical application in Japan. This medication potently inhibits the URAT1 transporter to a lesser extent, which also affects ABCG2, OAT1, and OAT3.420 Phase III clinical trials have substantiated the non-inferiority of dotinurad in comparison to both febuxostat and benzbromaron.421 Notably, dotinurad has demonstrated safety in patients with an estimated glomerular filtration rate (eGFR) between 60 ml/min and 30 ml/min, without necessitating any dosage adjustments. In terms of adverse drug reactions, aggregated data from phase II and III studies indicate that while dotinurad can potentially cause liver-related adverse reactions, such as hepatic steatosis and abnormal liver function tests, which the incidence is lower compared to benzbromarone.420

Tranilast

Tranilast, is recognized as an anti-inflammatory agent initially designed for treating allergic conditions such as asthma and allergic rhinitist.422,423,424 Recent research has shed light on its efficacy in lowering urate levels by inhibiting renal transporters URAT1 and Glucose Transporter 9 (GLUT9).425 In two separate preclinical trials, tranilast exhibited promising urate-lowering effects along with a reduction in inflammation associated with urate crystal deposition. Following the administration of a single dose of tranilast, a mean reduction in serum uric acid levels of 0.17 mg/dL at 4 h and 0.24 mg/dL at 24 h was observed. Headache was notably identified as the predominant adverse effect associated with tranilast. Furthermore, tranilast has been investigated in Phase II clinical trials in combination with allopurinol for patients experiencing moderate-to-severe gouty arthritis.418

Ulodesine (BCX4208)

Ulodesine, an inhibitor of purine nucleoside phosphorylase (PNP), operates upstream of xanthine oxidase (XO) in the purine metabolism pathway. By blocking PNP activity, ulodesine diminishes the substrates available for XO, thereby reducing uric acid production.426 Currently, this drug is in development for managing hyperuricemia in chronic gout. Promising results have been observed in two Phase II clinical trials, eval‎uating ulodesine both as a monotherapy and in combination with allopurinol. In a 24-week extension study, the treatment response rates for 5 mg, 10 mg, and 20 mg doses were 40%, 50%, and 45%, respectively, compared to a 25% response rate for the placebo.427,428 Interestingly, no significant adverse events were documented compared to the placebo group. Ulodesine displays no interactions with CYP450 isoforms and undergoes no hepatic metabolism, thereby minimizing anticipated drug interactions. However, there are concerns regarding its potential effects on T cells. Deficiency of purine nucleoside phosphorylase (PNP) has been linked to immunodeficiency and autoimmune disorders.243

Uricase

Uricase, facilitating enhanced uric acid excretion involves the administration of exogenous urate oxidase, is an enzyme which not endogenously expressed in humans. Uricases are employed in the treatment of refractory gout and are capable of achieving a rapid reduction in hyperuricemia, significant resolution of tophi, alleviation of chronic joint pain, and enhancement of overall quality of life.387 Urate oxidase catalyzes the breakdown of uric acid into 5-hydroxyisourate, which subsequently undergoes spontaneous degradation to allantoin without enzymatic assistance. The heightened solubility of allantoin, surpassing that of uric acid by 5-10-fold, facilitates its more efficient renal excretion.429 Addressing this constraint, the development of a recombinant urate oxidase, rasburicase and pegloticase has shown superior efficacy in rapidly reducing uric acid plasma concentrations compared to allopurinol.387 Pegloticase, a recombinant urate oxidase conjugated to polyethylene glycol (PEG), has been introduced to reduce immunogenicity and extend the half-life of rasburicase. Nevertheless, recent concerns regarding the development of antibodies against PEG in healthy blood donors prompt further exploration of potential implications for the efficacy of PEGylated pharmaceuticals. However, the main side effects include serious cardiovascular events and infusion reactions.1 Rasburicase is approved for managing hyperuricemia linked to chemotherapy in cancer patients. It is known for its immunogenicity and infusion-related reactions, like pegloticase. Unlike pegloticase, however, rasburicase is not PEGylated and has a shorter half-life of 8 hours.430 Rasburicase is predominantly employed in the management of tumor lysis syndrome owing to its rapid onset of action and short treatment duration. However, it is associated with significant incidences of infusion reactions, anaphylaxis, methemoglobinemia, and hemolysis, particularly in patients with glucose-6-phosphate dehydrogenase (G6PD) deficiency.431 However, the application of uricases has been constrained by factors such as availability, cost, and immunogenicity. Despite these limitations, uricases have the potential to become a primary therapeutic option for severe and challenging cases of hyperuricemia. They may be utilized as induction or debulking therapy to lower the urate pool, followed by maintenance with urate-lowering therapy (ULT).

Therapy frame and future considerations

Per the 2020 American College of Rheumatology guidelines, allopurinol is recommended as the initial therapeutic approach for symptomatic hyperuricemia, aiming to achieve a target serum uric acid level below 6 mg/dl.432 Epidemiological studies suggest that maintaining a serum uric acid level below 5.5 mg/dl may offer enhanced cardiovascular and renal protection compared to target levels of 6 mg/dl or higher.433 Maintaining urate levels at or below 360 μmol/L through urate-lowering therapy is deemed safe and crucial for the prevention and reversal of joint, cardiovascular and renal damages.308,362,363,372,434,435,436 Additionally, EULAR guidelines recommend losartan for patients with hypertension and fenofibrate for those with hyperlipidemia, both of which have mild uricosuric effects.336,437 Additionally, the British Society for Rheumatology advocates for a lower target serum uric acid level of less than 5 mg/dl.438 Similarly, the Japanese Society of Gout and Nucleic Acid Metabolism endorses allopurinol as the primary therapy for hyperuricemia, with a target serum uric acid level of less than 6 mg/dl. Furthermore, they suggest initiating treatment for hyperuricemia when the serum uric acid level exceeds 8 mg/dl with at least one complication, or above 9 mg/dl without any complications.439,440 Concurrently, the development of novel uricosuric compounds aims to address resistant hyperuricemia while maintaining a favorable safety profile. The uricosuric agents targeting the URAT1 transporter, such as lesinurad and dotinurad, along with the formulation of oral combination therapies comprising xanthine oxidase inhibitors and uricosuric agents, is poised to improve the attainment of the target serum uric acid level of less than 6 mg/dL.387 In conclusion, navigating the intricacies of hyperuricemia treatment requires a tailored approach. To mitigate acute arthritis attacks and associated complications, early initiation of pharmacotherapeutic interventions is advisable. The dynamic landscape, characterized by established agents and novel contenders, necessitates ongoing research to optimize therapeutic strategies, ensuring efficacy while mitigating potential risks.441

Conclusion and perspective

Among the history of hyperuricemia development, uric acid accumulation in serum characterizes hyperuricemia, a condition with diverse physiological roles ranging from antioxidant processes, pro-oxidative activities, pro-inflammatory activities, nitric oxide regulation, anti-aging effects and innate immune response.14,15,16 Understanding its multifaceted functions and mechanisms is crucial for deciphering its implications in health and disease. Furthermore, circulating urate levels are intricately regulated by the balance between urate production and excretion, and the kidney plays a pivotal role in maintaining this homeostasis.186,187 Urate transporters contribute to this delicate equilibrium. Genetic factors, particularly variations in urate transporter genes, significantly influence individual susceptibility to hyperuricemia.245,442 Altered urate transport mechanisms, both in the gastrointestinal tract and kidneys, are implicated in the pathogenesis of diseases associated with hyperuricemia.(Fig. 4) Future genome-wide association studies should aim to broaden their scope by encompassing diverse ethnic groups and varied patient populations. Furthermore, investigations into comorbidities linked with hyperuricemia need expansion to better elucidate the role of transporter gene mutations in disease pathogenesis.303,443 In the meantime, by utilizing the results of GWAS studies, clinicians can identify individuals at risk for adverse drug reactions better, thereby improving safety and treatment compliance.150 Furthermore, redefining hyperuricemia as a dynamic variable rather than a static biochemical parameter may offer novel perspectives on its role in disease progression. As our understanding advances, the intricate nature of hyperuricemia-related diseases necessitates ongoing exploration, emphasizing the importance of innovative personalized medicine approaches and a nuanced perspective to unravel these complexities. Dysmetabolic intestinal flora potentially contributes to gout-related metabolic and inflammatory symptoms by promoting Th17 infiltration. The identification of probiotic strains, such as DM9218, capable of lowering uric acid levels represents a novel therapeutic avenue. Currently, the modulation of intestinal microbiota through microecological therapies, including probiotics, prebiotics, and fecal microbiota transplantation, is a prominent area of clinical investigation for preventing and managing hyperuricemia and gout. These interventions aim to restore intestinal microecological balance, increasingly recognized as pivotal in the pathophysiology of these conditions. By targeting the gut microbiome, these therapies offer a novel and potentially effective strategy for mitigating the risks and progression of hyperuricemia and gout, thereby contributing to a more holistic and personalized treatment approach in clinical practice.143,444 Furthermore, identifying the distinct phenotypes is crucial, as hyperuricemia stemming from increased XO activity may have a different correlation with cardiovascular disease compared to that caused by renal underexcretion. Moreover, patients with the underexcretion phenotype might respond more favorably to uricosuric agents than to XO inhibitors. We suspect that biases in patient population selection could account for the inconsistent findings regarding the cardio and nephroprotective effects of hypouricemic agents in clinical trials. Differentiating between gout and asymptomatic hyperuricemia can be challenging, as gouty nephropathy may occur even in the absence of clinically apparent gout or with serum uric acid levels below the solubility threshold. There is an urgent need for future studies to delineate the effects of different classes of hypouricemic drugs on each hyperuricemia phenotypes.372

In addition, in terms of the major mechanism of hyperuricemia induced commodities, oxidative stress, inflammatory signaling pathway and immune response are involved in this process, which mainly lead to cell apoptosis and endothelial dysfunction.105,270,287(Fig. 5) While some associations have been observed, particularly with gout and renal diseases, evidence from Mendelian randomization studies did not consistently support a causal relationship between elevated serum urate levels and other metabolic or cardiovascular disorders. However, hyperuricemia plays a role in promoting inflammation, oxidative stress, and endothelial dysfunction underscores its potential contribution to disease pathogenesis.249,445,446,447,448,449 Uric acid exerts multifaceted effects on endothelial function and vascular health through its interactions with NO, ROS, and inflammatory pathways, highlighting its potential role in the pathogenesis of cardiovascular diseases like atherosclerosis.69,90,256 Targeting these pathways may offer therapeutic opportunities for mitigating the adverse vascular effects of hyperuricemia. However, the precise mechanisms by which NLRP3 is activated in response to monosodium urate crystals remain incompletely understood.91,114,263,423,450,451 The caspase-1-independent pathways of IL-1 production, including the specific proteases involved and the stimuli for their activation, are still not well-defined. Clarifying the stages at which these pathways contribute to the inflammatory phenotype and identifying the cell types orchestrating this inflammasome-independent response are crucial areas for further investigation.337,340,452 Moreover, a pivotal area of research concerns the mechanisms that precipitate gouty attacks in patients with sustained monosodium urate crystal deposits. It remains uncertain whether distinct initiation mechanisms trigger the inflammatory response by acting on priming signaling pathways, or if a reduction in the negative regulation of NLRP3 activation amplifies the inflammatory cascade.15,453,454 Current therapeutic approaches for hyperuricemia focus on mitigating associated complications and reducing serum UA levels with non-pharmacological interventions include dietary modifications and some environment factors.455 Besides, pharmacological interventions primarily involve urate-lowering drugs, uricosuric compounds and emerging agents.55 Traditional XO inhibitors and newer uricosuric compounds provide additional options for personalized treatment approaches. Newer uricosuric compounds, such as probenecid, lesinurad and arhalofenate, target different aspects of uric acid metabolism, providing additional options for personalized treatment approaches. Compared with XOIs, uricase, rasburicase and pegloticase convert UA to allantoin in adults with gout resistant to conventional therapy.429 Precision medicine guided by genetic insights holds promise for tailoring hyperuricemia management to individualized needs.410 Efforts are underway to develop novel therapies addressing unmet needs, such as alternative agents for long-term management of hyperuricemia.201,411,438,456 Integration of genetics into hyperuricemia research offers opportunities for advancing personalized medical approaches and improving patient outcomes. In the future, precision medicine, guided by genetic variants, represents a promising avenue for tailoring hyperuricemia management to individualized needs. Hyperuricemia continues to be inadequately managed, primarily due to factors such as ineffective dosing of urate-lowering therapy, patient noncompliance, and intolerance/adverse events associated with current treatment options.23,321,325,415,455 These limitations highlight the urgent needs for the creation of alternative treatment options capable of safely and effectively reducing serum uric acid levels for the long-term management of hyperuricemia. Acknowledging the growing need for better control of hyperuricemia, considerable research has been dedicated to the discovery and development of innovative therapies designed to meet these clinical challenges.

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