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beyond reason
Schematic representation of the influence of host Lf on immune cells.
(a) Promotes B- and T-lymphocyte maturation;
(b) Negative regulation of B-lymphocytes through LPS binding;
(c) B- and T-lymphocyte interaction;
(d) induces IgA and IgG secretion;
(e) promotes T-lymphocyte proliferation;
(f) decreases IL5 and IL10 secretion;
(g) down regulates NFκβ activation of monocytes;
(h) enhances the phagocytic activity of macrophages; and
(i) prevents the interaction between LPS and CD14 as a TLR4. B, B lymphocytes;
T, T lymphocytes; Mf, macrophages; Mon, Monocytes; Neu, Neutrophils.
Lactoferrin (Lf) is an iron-binding glycoprotein of the transferrin family, which is expressed in most biological fluids with particularly high levels in mammalian milk. Its multiple activities lie in its capacity to bind iron and to interact with the molecular and cellular components of hosts and pathogens. Lf can bind and sequester lipopolysaccharides, thus preventing pro-inflammatory pathway activation, sepsis and tissue damages. Lf is also considered a cell-secreted mediator that bridges the innate and adaptive immune responses. In the recent years much has been learned about the mechanisms by which Lf exerts its activities. This review summarizes the recent advances in understanding the mechanisms underlying the multifunctional roles of Lf, and provides a future perspective on its potential prophylactic and therapeutic applications.
Lactoferrin (Lf) is an iron-binding glycoprotein of the transferrin family, which is expressed in most biological fluids with particularly high levels in mammalian milk(saliva, tears 등). Its multiple activities lie in its capacity to bind iron and to interact with the molecular and cellular components of hosts and pathogens. Lf can bind and sequester lipopolysaccharides, thus preventing pro-inflammatory pathway activation, sepsis and tissue damages. Lf is also considered a cell-secreted mediator that bridges the innate and adaptive immune responses. In the recent years much has been learned about the mechanisms by which Lf exerts its activities. This review summarizes the recent advances in understanding the mechanisms underlying the multifunctional roles of Lf, and provides a future perspective on its potential prophylactic and therapeutic applications.
The first literature references to lactoferrin (Lf) refer to it as a “red protein from milk” and, from the time that it was first purified1,2, as an iron-binding protein. Lf is an 80-kDa glycosylated protein of approximately 700 amino acids with high homology among species that is considered a multifunctional glycoprotein that is widely distributed in colostrum and milk3 as well as in other secretions, such as tears and saliva4. It is released from neutrophils in the blood and inflamed tissues. Lf has a direct antimicrobial role, as it limits the proliferation and adhesion of microbes (eg, bacteria, viruses and parasites) and/or kills them5. This effect of Lf is the result of its ability to sequester iron in biological fluids and destabilize the membranes of microorganisms6. The metals that Lf binds are the Fe2+ or Fe3+ ions, but it can exist free of Fe3+ (apo-Lf). Human LF (hLF) is a polypeptide chain that is folded into two symmetrical lobes (N and C lobes) that are connected by a hinge region that contains parts of an α-helix (Figure 1).
It is known that Lf possesses antimicrobial activities, modulates the overall immune response and protects against viral infections, and its role against septic shock has already been well described5,6. In this respect, it is noteworthy that Lf concentrations are locally elevated in inflammatory disorders, including neurodegenerative diseases7, inflammatory disease, arthritis8 and allergic inflammation9. The cellular and molecular mechanisms responsible for the immunomodulatory effects of Lf are not fully elucidated, and in vitro and in vivo studies suggest the existence of multiple mechanisms that include modulation of cytokine/chemokine production, regulation of the production of reactive oxygen species and immune cell recruitment10.
Lf, which functions as a natural iron scavenger and an activator/modulator of signaling pathways, leads to the negative feedback of the inflammatory response, as shown by a decrease in the production of reactive oxygen species and various pro-inflammatory cytokines11,12.
Lf secretion dramatically increases during inflammation and neurodegenerative diseases, which leads to neutrophil degranulation and the activation of microglial cells13. The increase of Fe during hemorrhagic stroke in microglia is due to the uptake of the transferrin and lactoferrin receptors. Lactoferrin receptors (LfR; 105 kDa) on neurons are involved in the transferrin-independent pathway by transporting iron from iron-containing Lf across neuron membranes14. Future research on iron metabolism and its dysregulation may provide new insights into neurodegenerative diseases such as Alzheimer's, Parkinson's, and Friedrich's ataxia15.
Lf also acts as a first-line of defense by significantly impacting the development of adaptive immune responses. Iron sequestration by Lf reduces oxidative stress that alters the extension and production of cytokines16. Lf has a strong modulatory effect on the adaptive immune system by accelerating the maturation of T-cell precursors into competent helper cells and by the differentiation of immature B-cells into antigen-presenting cells17. Lf can also modulate innate and adaptive immunities because it binds to LPS and CD-14 and interferes with the formation of the CD14–LPS complex, resulting in attenuation of the LPS/CD-14/TLR-4 signaling pathway, which is essential for the pathogenesis of sepsis18. Lf may stimulate the immune system by binding to CD-14 and then activating the TLR-4-mediated pathway while preventing overexpression of LPS-induced inflammation19.
Lf blocks the signal transduction between LPS and the CD14–TLR complex that exists in the macrophages to prevent or treat septic shock. Lf promotes the maturation of B- and T-cells in function and phenotype to improve the immune response20. Thus, Lf may also protect infants from infections due to its large set of ability's against the direct interaction with microorganisms and through its immune modulatory effect.
Immunomodulators are biological or synthetic substances that are capable of altering the immune response by augmenting or reducing immune system components, including the innate and adaptive arms of the immune response21. The human body produces some peptides and small proteins with antimicrobial and immunomodulatory activities22. At first, it was thought that the function of these peptides was only to kill microorganisms; however, it is now known that these peptides also coordinate multiple immune system functions as a basic immunity mechanism23. These peptides are believed to contribute to the prevention or recovery of changes in the immune system by suppressing or enhancing the immune response24. Some immunomodulators, such as antibodies, react to unique antigens and may be specific to certain pathogens, but others can be nonspecific (eg, cytokines, antimicrobial peptides, drugs and even microorganisms used to generate a positive host response). A clear example of this is the use of probiotics to enhance the normal microbiome of the small intestine17. With this approach, immunomodulators may be classified as immunoadjuvants, immunosuppressants or immunostimulators.
Immunoadjuvants are substances that are required to elicit a maximal T-cell response to microbial antigens. They are commonly used in vaccine development to improve the response of the organism25,26. Immunosuppressants inhibit the normal functioning of the immune system; therefore, they are used in conjunction with drugs to treat autoimmune diseases and the immune response in transplantation27. Immunostimulators are agents that act through response-mediated innate and adaptive immunity. In healthy individuals, immunostimulators act as prophylactic agents to enhance the immune response to infection. In immunocompromised individuals, immunostimulators may act as natural therapy28.
Colostrum, the first milk produced by the mammary glands of mammals after giving birth, contains elements with immunomodulatory properties, and these elements have attracted the attention of some pharmaceutical and nutritional industries as a dietary supplement29. Lf is present in bovine colostrum at a concentration of 500 mg/100 g and is a GRAS (generally recognized as safe) product that is currently used in several countries as a supplement for infants. To date, no adverse effects regarding its use have been documented30. The first occurrence of an infant formula containing Lf was in Japan in 1986, and this product, which was called “BF-L dry milk”, was marketed by the Morigana Milk Industry. Currently, Lf can be found in various products, such as yogurt, pet food, cream, and milk and other beverages31.
The concentration of Lf in human colostrum is 5.3±1.9 mg/mL, and, after the first month of lactation, this value is approximately 1 mg/mL32. Colostrum is the pre-milk fluid in the mammary gland of female mammals immediately before giving birth. After the first instance of nursing, the fluid transforms to milk over a period of 2–3 d. In all non-human mammals, colostrum is crucial to the survival of the newborn because high concentrations of immune factors are transferred to the newborn via colostrum. In humans, some immunofactors are transferred through the placenta. Human colostrum is particularly beneficial; however, if a human newborn does not receive colostrum, death is not imminent as it is in other mammals. Like in other mammals, a newborn's first meal of colostrum significantly impacts its health and well-being, and the effect lasts the rest of its life. Because a newborn's immune system is not fully developed, it is highly susceptible to pathogens, antigens and allergens26. The colostrum that is found in breast milk contains all of the immune factors that are essential to activate and regulate the immune system response. Consequently, colostrum plays a crucial role in supporting a newborn's immune system while it develops. In trials, significant quantities of intact Lf was found in infant stools, even in babies of 4 months old, which suggests that Lf can survive being active in the small intestine. The values decline from 155 mg/24 h at 1 week of age to 20 mg/24 h at 14 weeks, whereas Lf intake from breast milk was 2.5 g/24 h at 1 week to 1.4 g/24 h at 14 weeks33.
Lf is the first line of defense for any entry point in the body. It is found in small quantities in most body fluids such as saliva, tears, nasal secretions and intestinal fluids (eg, bile), as well as in neutrophils (the secondary granules of white blood cells). Lf is synthesized by the mucosal lining (eg, in the mouth or intestinal tract) and neutrophils, and it is released in response to inflammatory stimuli. The low physiologic serum levels of Lf increase significantly upon host infection. The Lf receptor was studied and isolated from activated T- and B-cells, monocytes, intestinal brush border cells, platelets and neoplastic cells34. Lf inhibits neutrophil apoptosis via blockade of proximal apoptotic signaling events. Iron-unsaturated apo-lactoferrin inhibits spontaneous apoptosis in human neutrophils, depending upon the iron saturation status, and down regulates early events in the apoptosis process; moreover, its effect is evident in an established phase of rheumatic arthritis35.
Lactoferrin, amylase and lysozyme are detectable proteins during the early fetal stages of development. Only low levels of these secretory components are observed before week 29 of gestation, but their levels increase rapidly to adult levels one week after being born. Although the skin and gastrointestinal tracts are immunologically mature prior to birth, the respiratory tract is not36.
The first stage of human fetal hematopoiesis occurs in the mesoderm of the yolk sac and in the mesenchymal tissue. Totipotent erythroid and granulomacrophage progenitors can be found in human embryonic structures 3–4 weeks into gestation. These primitive cells can then be detected in circulation after 4 weeks of gestation, and they then migrate to the liver, which is known as the site of hematopoiesis. At approximately 5–10 weeks, the liver undergoes a dramatic increase in size as the number of nucleated cells rises. These early progenitors proliferate but undergo remarkably little differentiation. Hepatic hematopoiesis declines in the third trimester and ceases soon after birth36,37,38.
Lf expression can be detected at the 2- and 4-cell stages of embryonic development and throughout the blastocyst stage (prior to implantation). After implantation, Lf expression cannot be detected again until approximately halfway through gestation, when it can be found in neutrophils and epithelial cells of the developing reproductive and digestive systems39. The Lf plasma levels are higher during pregnancy than in either male or female adults, and these levels show a progressive increase leading up to week 29, at which point these levels remain high40. Several factors may explain this increase, such as pregnancy-associated leukocytosis, the selective increase of Lf in neutrophil granules or endometrial tissues or contribution from the decidua and mammary glands41. Lf acts as a growth factor activator and, when compared to epidermal growth factor, the effects of Lf alone on small intestine epithelial cells are more potent and can stimulate the proliferation of endometrium stromal cells39.
The principal stimuli that induce the postnatal maturation of the mammalian immune system are signals from the microbial environment, particularly the commensal microflora of the gastrointestinal tract, but infections in the gastrointestinal and respiratory tracts may also contribute to immune system development42. Lf is identified as an important defense component of colostrum and mature milk, which promotes the hypothesis that its function involves the protection of neonatal gut barriers. In concurrence with this finding, LfR were discovered in the small intestine during a study of iron delivery to the duodenal mucosa43. A recent study of LfR in the mouse small intestine suggests that LfR may act as the main iron source during the early stages of life. Subsequent binding affinity studies identified Lf on the surface of B-cells, T-cells and monocytes, as well as on platelets and intestinal cells17,43. Lf can facilitate the adaptation of an infant intestine because Lf hydrolysis is minimal at the prevailing postprandial pH in infants; therefore, Lf may have greater biological potential in infants than in adults. Lf bi-directionally stimulates the proliferation and differentiation of small intestinal epithelial cells, which are concentration-dependent and affect the mass, length and epithelial digestive enzyme expression of the small intestines44.
The constant interaction between the intestinal epithelium and the gut microbiota is a challenge for the preterm gut. Mature intestines have many physical barriers that are designed to limit bacterial access to the gut lumen and prevent attachment and translocation across the intestinal epithelium. In contrast, external factors render the preterm intestine more susceptible to microbial interaction and translocation. Preterm infants face many challenges when transitioning from the in utero to extrauterine environment. Failure in the maturation of the preterm gut to accommodate bacteria and food leads to significant morbidity, such as neonatal necrotizing enterocolitis45.
Among the Antigen Presenting Cells (APCs), macrophages (Mf), dendritic cells (DCs) and B-cells are of critical importance for the maintenance of tissue homeostasis and the innate response; and this response occurs via the major histocompatibility complex II (MHC II), as well as by linking the innate and adaptive immune responses. Mfs are highly phagocytic cells that play a central role in the control of infections, either by the direct intracellular killing of microorganisms or the secretion of cytokines to inhibit the replication of microorganisms. Mfs are also involved in type II inflammation and tissue repair processes46,47,48. DCs are a heterogeneous population of cells that are highly specialized for antigen recognition; and they play a key role in the immune system because they control the induction of immunity and tolerance. B-cells utilize specific surface receptors to capture foreign antigens and present their associated epitopes to T-cells49,50.
Macrophages (Mfs) are Antigen Presenting Cells (APCs), and their role in the innate immune response involves inducing the phagocytosis of foreign particles and subsequently releasing pro-inflammatory mediators. Mfs also enable cross-talk between the innate and adaptive immune systems to stimulate antigen-specific T cells. Active binding studies revealed that Lf receptors are located on the surface of Mf in bovine and human models51,52. Lf also contributes to the suppression of pro-inflammatory cytokines and type I interferon (IFN α/β) induction53,54, and it affects the ability of Mfs to present antigens for antigen-specific CD4+ T-cells in the adaptive immune system. Lf can increase the phagocytic activity of Mfs that are infected or have not yet been activated55,56. IL-12, one of the major cytokines that are produced by Mfs, is a key modulator of IFNα. The main role of IL-12 at the site of infection is to recruit Mf57,58, and it acts as a co-stimulator to maximize the secretion of IFNα from differentiated Th1 cells and memory T-cells59. Up-regulation of adhesion molecules on the surface of the endothelium plays a key role in the recruitment and infiltration of leukocytes at inflammation sites. Lf strongly inhibits TNF-a-stimulated expression of ICAM-1 by competing with NF-jB in endothelial cells, which suggests that Lf reduces inflammatory events and the development of inflammatory diseases such as atherosclerosis60.
Dendritic cells (DCs) are a group of functionally related phagocytic cells that can manipulate T-cell differentiation61 and redirect memory T-cell functions62,63. DCs play an important role in triggering T-cell responses that lead to the secretion of Th1 cytokines64,65. It has also been shown that β-defensin 2, another key innate immunity molecule, acts directly on DCs to induce their functional maturation and enable them to elicit a Th1 response66,67.
The ability of Lf to promote antigen-specific delayed-type hypersensitivity (DTH) responses and to activate bacillus Calmette-Guerin (Mycobacterium strain) (BCG)-specific T cells suggests that Lf plays a role in the initiation of T-cell activation through the modulation of dendritic cell function68. Dendritic cells possess Lf receptors because bovine and human Lf binds to the surface of peripheral blood-derived dendritic cells69. The ability of dendritic cells to migrate upon antigen stimulation or capture is essential in the promotion of antigen-specific immune responses70. Lf acts as an alarmin to promote the recruitment and activation of APCs and antigen-specific immune responses. It has also been reported as a novel maturation factor for human dendritic cells10,71. Lf is a strong mediator of dendritic cell function. This observation, together with the above-described impact on Mfs, suggests that Lf exerts its effect on cells involved in the commitment of pathogens (antigens) and can direct the development of adaptive immunity (Figure 2).
A key immunomodulatory function (eg, APC activation, maturation, migration and antigen presentation) that may be mediated by Lf is the bridging of innate and adaptive cell functions for the T- and B- cell responses.
Considerable attention is focused on Lf because of its potential role in the maturation and function of immune system cells72. Significantly, Lf leads to an increase in the expression of the complement 3 receptor (C3R) and acquisition of surface IgD. Also of importance is the interaction between Lf and the Lf receptor on T- and B-lymphocytes73. Structural changes in the N-terminal basic region and the basic characteristics of the entire molecule contribute to its interaction with B lymphocytes74. Oral administration of Lf increases the secretion of IgA and IgG in murine mucosa with intestinal secretion75,76. These data suggest that Lf acts on B-cells, which are well-known antigen presenters, to allow for their subsequent interaction with T cells, which favors elevation of the antibody response (Figure 2).
The effect of Lf on T-cell populations can be further delineated in terms of the cellular subset that is specifically targeted. The adaptive immune response is dominated by T-cell activity, which includes various functions. T-helper cell type 1 (Th1) and type 2 (Th2) stimulate and activate Mf, resulting in intracellular killing events that eliminate intracellular pathogens77. Lf can downregulate allergic rhinitis, which reduces inflammatory responses, because it upregulates the expression of Th2, Th17 and regulatory T cells. Lf can promote Th1 responses while inhibiting Th2 responses, and it causes T-cell receptor cross-linking, which leads to the inhibition of T-cell activation, reduces the release of inflammatory factors such as IL-5 and IL-17, and further alleviates the degree of inflammation78. Lf accelerates T-cell maturation by inducing the expression of CD4 surface markers through the activation of a transduction pathway79. The expression of Lf receptors has been reported in all T-cell subsets. Bovine and human Lf is capable of binding to surface receptors on the human T-cell line (Jurkat)73,80. These associated changes to the surface of molecules that regulate T-cell function suggest that Lf is capable of modulating T cell and NK cell activity due to T-cell proliferation. Indeed, Lf can potentiate the restoration of the humoral immune response of the host, suggesting a possible mechanism for cell reconstitution through proliferative pathways63. Lf induces Th1 polarization in diseases in which the ability to control infection or tumor relies on a strong immune response; however, Lf may also reduce Th1 cytokines to prevent excessive inflammatory responses81.
The antimicrobial effects of Lf have been demonstrated in vivo for the parenteral administration of Lf in several experimental animal models, most notably in mice82. Additionally, studies have shown that bovine Lf reinforces the immune system and antioxidant status in healthy human volunteers83. Furthermore, several in vitro studies have indicated that the structure of Lf plays a vital role in antimicrobial activity (eg, the interaction with viruses and bacterial toxins) because the glycosylation sites of the Lf protein expose its outer surface and allow it to maintain contact with microorganisms54. Some of the mechanisms through which Lf triggers an immune response against pathogens are summarized in Table 1.
Mechanism of action of Lf | Target | Reference |
---|---|---|
Enhancing of phagocytosis | Gram-Positive bacteria S mutans S epidermidis S aureus Gram-Negative bacteria: P aeruginosa B cepacia B cenocepacia Porphyromonas gingivalis Virus: VSV (Vesicular Stomatitis Virus) Fungi: Candida spp. A Fumigatus Parasites: E histolytica B caballi T cruzi | 6,84,121,122,54,84 |
Biofilms inhibition | Gram-Negative bacteria: Porphyromonas gingivalis Prevetella intermedi P aeruginosa B cepacia B cenocepacia E coli M bovis Gram-Positive bacteria: S epidermidis | 84,87,92,123 |
Positive domain union with negative charges on microorganisms | Gram-Negative bacteria: E coli Parasites: T gondii E stiedai | 6,124 |
Modification of the interactions of microbes, with the host cells, or with the extracellular matrix | Gram-Positive bacteria: B subtilis K pneumoniae S mutans Virus: Rotavirus Enterovirus | 84,87 |
Inhibits LPS-mediated activation | Gram-Negative bacteria | 6,85,125 |
Induction of apoptosis | Fungi: Candida albicans | 90 |
It is well known that Lf interacts directly with bacterial LPS, thereby preventing interaction between the endotoxin-containing LPS binding protein (LBP) and CD1484,85. In addition, this Lf-LPS interaction triggers a signaling cascade that results in the release of pro-inflammatory mediators, such as cytokines and chemokines, as well as small molecules, such as lipid mediators and reactive oxygen species48. In addition to LPS, other pro-inflammatory microbial molecules (eg, unmethylated CpG-containing oligonucleotides) can be neutralized by Lf. The ability to bind unmethylated CpG-containing oligonucleotides allows Lf to have anti-inflammatory effects on B-cells, which supports the possibility that Lf may interact with TLR-917,86. This mechanism is attributed to the N-terminal domain of Lf and its ability to bind large amounts of iron84,87, thereby preventing the host cell from inhibiting the production of pro-inflammatory cytokines (eg, TNF-α, IL-1β, IL-6 and IL-8)6,54. The contribution of Lf to pro-inflammatory cytokine release enhances phagocytosis and cell adhesion and provides protection against pathogens and their metabolites17,87. However, when Lf is orally administered in Staphylococcus aureus-infected models, an increase in the host response can be observed as an increase in TNF-αlevels and decrease in IL-5 and IL-10 levels17.
Although Lf only exerts its antiviral activity against enveloped viruses, it is currently believed that it has antiviral activity against a broad spectrum of RNA and DNA viruses. Its main contribution to this antiviral defense is the ability to bind to cell membrane glycosaminoglycans39,87. In the presence of some viruses (eg, vesicular stomatitis virus), Lf can increase the phagocytic activity of Mfs17. On the other hand, Lf has strong interactions with the protein gp120 of the Human Immunodeficiency Virus, wherein Lf binds to the DC-SING receptor of dendritic cells to block their interactions and subsequently inhibit the transmission of the virus6,88.
Candida albicans is one of the most common causes of vaginal infections89. The adherence of this fungus to the vaginal epithelium can be prevented by the action of Lf because of its ability to sequester iron87. In addition, Lf has the ability to induce apoptosis in yeast, which was first reported by Madeo et al in 199790. In 2000, Wakabayashi et al reported that Lf inhibits the in vivo growth of Trichophyton mentagrophytes and Trichophyton rubrum, two of the principal etiological agents of dermatophytosis91. This growth inhibition occurs because Lf enhances the inflammatory response involved in the cell-mediated immunity that is required to cure this mycosis92.
The mechanisms involved in the antiparasitic activity of Lf are complex93. Lf exhibits activity against Entamoeba histolytica, Trichomonas faetus, Trypanosoma cruzi, Trypanozoma brucei, Plasmodium falciparum, Toxoplasma gondii and Eimeria stiedai. It is not clear whether the antimicrobial properties of Lf are related to its direct action against microbes or to the activation of the immune system, but several lines of evidence now indicate that both forms of action are involved. This hypothesis is supported by reports that Lf can modulate and direct changes in the balance of T-cell immunity. In studies involving Toxoplasma gondii infection, oral administration of Lf promotes Th2 cell responses in the intestinal mucosa, which is characterized by decreased levels of IFN-γ and elevated levels of IL-106,17.
As we discussed in a previous paper87, the different benefits of Lf have led us to be interested in using molecular strategies to develop recombinant Lf from different species to increase its availability. Because of its broad antimicrobial capacity, Lf could be used as a nutraceutical protein or adjuvant drug. Although colostrum contains high Lf levels, industrial companies will require the production or purification of Lf without affecting the alimentary industry uses of milk. Currently, highly purified bovine lactoferrin (bLf) and human lactoferrin (hLf) can be produced93. In addition, lactoferrin from other species (eg, mouse, rat, chimpanzee, boar, sheep, goat, buffalo, camel and dog) was sequenced and found to vary by 2112 to 2530 bp94,95. It has been possible to produce recombinant Lf specific to human, bovine, equine, porcine, caprine, yak and Kunming by using various expression systems (eg, bacteria, fungi, yeast, cell lines, insects, mammals and plants). While Lf is produced in quantities ranging from 0.756 mg/L to 10.6 g/L, human Lf remains the most expressed among all of the different expression systems87,96,97,98,99,100,101,102,103.
Lf has multiple activities, it can bind a significant number of compounds and substances, such as lipopolysaccharides, heparin, glycosaminoglycans, DNA and metal ions (eg, Fe, Al, Mn, Co, Cu, Zn)39,104; is involved in iron homeostasis; has a wide range of antimicrobial activity against bacteria, virus, fungi and parasites; and has anti-inflammatory, immunomodulatory, anticarcinogenic and enzymatic activities105. Antibiotic-resistant microorganisms are extremely dangerous to humans, and extensive scientific research has resulted in the development of new antibiotics with different effects in an effort to solve the issue. The scientific community has targeted Lf as a promising candidate to help break the vicious cycle of antibiotic resistances5,106. Oral Lf supplementation in human newborns can prevent infection or decrease the severity of an existing infection107,108,109. A human study found that nutritional supplementation with colostrum was equally efficient in preventing episodes of the flu compared to a vaccine29,110. In clinical trials, the administration of bovine Lf suppressed carcinogenesis in the colon and other organs, and human studies have recently shown that Lf inhibits the growth of adenomatous polyps and can reduce the risk of colon carcinogenesis111. The ability of Lf affecting metabolism by reducing triacylglycerol and cholesterol levels have been reported112, and a study in Japan has revealed that the use of oral Lf can reduce visceral fat in humans113. Lf-derived peptides with antihypertensive effects have shown similar effects as specific drugs114. In addition to its application to human health, Lf has industrial application. One study has shown that Lf can be used to extend the shelf-life of various meat patties and other meat products, and fresh ground pork with added Lf had lower total plate counts115. Lf can also be used as an alternative animal feed additive that can reduce or eliminate the impact of antibiotic consumption on animal husbandry and strengthen the natural immune systems of livestock. Along these lines, a study found that early weaned piglets receiving rice bran expressing porcine recombinant-Lf as a feed additive had improved antimicrobial characteristics and IgG concentration116,117,118. Additionally, Lf could be used to control diseases caused by fungal pathogens in crops119,120. In cell culture applications, a concern regarding potential contamination when using protein and peptides from animals exists; therefore, the expression of recombinant Lf in rice has been studied to enhance the growth of intestinal cells, hybridoma cells, human embryonic kidney cells and osteoblasts. This study concluded that Lf is effective in promoting mammalian cell growth and increasing cell productivity121.
Human Lf is safe and is considered by the FDA as a GRAS product with no contraindications in either pediatric or adult patients82,106. Some pharmaceutical industries (eg, Venture LLC, Biopharming, Ventria Bioscience, AusBioMed, Max Biocare, Morinaga Milk Industry Co LTD) are currently commercializing human and bovine Lf in different products including a nutraceutical powder, a vitamin supplement for children, infant formula, beverages and a cell growth promoter. The bio-pharmacy company Agennix has a product, talactoferrin, which is currently undergoing clinical trials for consideration as a GRAS product. This product is proposed for use in the treatment of diverse carcinomas, severe sepsis and diabetic foot ulcers. Infant formulas supplemented with Lf are among the products in which industry is particularly interested.
Lf is a versatile molecule that was molded by natural selection to be a first-line defense in mammals. Its ability to exert multiple regulatory effects due to its cationic nature allows it to bind a large number of surface molecules or metal ions during the development of microorganisms and induce host immune-modulatory activation, which influences the adaptive and innate immunities. The development of Lf expression systems for food and pharmaceutical applications are required, due to its plethora of abilities as a multifunctional, nutraceutical protein.
This work was supported in part by an internal grant from Facultad de Ciencias Químicas, Universidad Autónoma de Chihuahua, Mexico and Proteo/Muuu-Technologies de México.