The Saga of Endocrine FGFs

FGF19 is involved in the organogenesis of energy-intensive organs such as the ear, eye, heart, and brain [71,72]. FGF19 is also expressed in human embryonic stem cells and the expression levels correlate with the pluripotent state [73]. In contrast, during adulthood, FGF19 would disappear globally from the central nervous system and is predominantly expressed in the ileum, and acts in the human liver through its receptor FGFR4 and co-receptor KLB [73]. The binding of FGF19 to FGFR4 leads to phosphorylation of extracellular signal-regulated protein kinase 1 (ERK1), extracellular signal-regulated protein kinase 2 (ERK2), and Stat-3, and this affects the proteins involved in the regulation of gluconeogenesis, lipogenesis, bile acid biosynthesis, and cell proliferation [74,75,76] (Figure 2A). Bile acids are important for intestinal lipid absorption and their synthesis represents a major pathway for cholesterol catabolism [77]. In physiological states, circulating levels of FGF19 represses bile acids synthesis, which are signaling molecules that activate specific bile salt receptors (FXR) during enterohepatic circulation from the ileum to the liver [78]. FXR is a bile acid nuclear receptor encoded by Nuclear Receptor Subfamily 1 Group H Member 4 (NR1H4) gene [11,23]. Specifically, bile acid activates FXR and subsequently upregulates the synthesis of FGF19 [79]. In turn, FGF19 creates a negative feedback loop and negatively regulates the bile acid biosynthesis by suppressing the expression of Cholesterol 7a-hydroxylase (CYP7A1), a rate-limiting enzyme in the production of bile acid [80]. A study showed that in FXR-deficient mice, FGF19 cannot be expressed, resulting in an elevated expression of CYP7A1. This indicates that the bile acid synthesis is abolished [81]. However, recent studies suggest that there may be an FGF19-independent suppression of bile acid synthesis through the activation of hepatic FXR [82] creating new opportunities for further investigation on the role(s) of FGF19 in bile acid regulation. FGF19 is also expressed in human epithelial cells of the gallbladder. Bile acid is stored in the gallbladder until it is needed by the body [83]. FGF19 is expressed due to the bile acid-mediated induction of FXR. The expression of FGF19 subsequently induces gallbladder relaxation and filling [80]. Additionally, another postprandial hormone involved in the gallbladder emptying process, CCK, is also affected by FGF19 [84]. Specifically, CCK aids in the emptying process of the gallbladder, which stores and concentrates bile acid during fasting, and releases bile acid during digestion [83,84]. FGF19 administration suppresses the action of CCK directly which leads to the induction of gallbladder filling in CCK-treated mice [24,80].

Studies in mice with whole-body FGFR4 deficiency have impaired glucose tolerance and reduced insulin sensitivity [85]. Treatment with FGF19 regained the normal glucose tolerance. These findings provided a piece of evidence for a new physiological role of FGF19 in glucose homeostasis [5,80]. FGF19 contributes to the regulation of hepatic glucose homeostasis through its effect on gluconeogenesis in an insulin-independent manner [14]. More specifically, FGF19 represses the expression of a gluconeogenic gene through cAMP-response element-binding/protein-peroxisome proliferator-activated receptor-γ co-activator 1α (CREB/PGC1α) pathway that is not dependent upon insulin signaling [14]. This allows FGF19 to activate ERK 1 and 2 signaling in adipocytes and increase glucose uptake [81,86]. Furthermore, FGF19 can promote glycogen synthesis to further regulate glucose homeostasis [80]. Glycogen synthesis is negatively regulated by glycogen synthase kinase 3α (GSK3) α and β, i.e., these enzymes phosphorylate and inactivate glycogen synthase to suppress glycogen synthesis [80]. However, FGF19 induces the inactivation of GSK3α and GSK3β thereby, increasing glycogen synthesis [80]. With evidence that FGF19 is a key regulator of metabolism, further interests in the field of FGF19 reported a new function for the protein in skeletal muscle. Previous works showed that mTOR and its downstream target, ribosomal protein S6 kinase (S6K), are the key regulators of muscle cell growth [87,88]. Furthermore, it has been reported that mice treated with recombinant FGF19 consecutively for 7 days had a higher skeletal muscle mass and strength than the control mice [89]. Additionally, treatment with recombinant FGF19 increased the myotube area in human muscle cells during differentiation from myoblast to myotube, as well as in fully differentiated myotube [89]. Recently, Guo et al. (2021) demonstrated the role of FGF19 in regulating skeletal muscle of mice by enlarging muscle fiber size as well as detailed a mechanism for such function [90]. Specifically, FGF19 increases the muscle fiber size by stimulating the phosphorylation of the ERK 1 and 2 and S6K1 pathways [90]. Furthermore, they also showed that FGF19 was able to protect the skeletal muscle against obesity-induced muscle atrophy through the AMP-activated protein kinase (AMPK)-Sirtuin-1 (SIRT1)-PGC1α pathway, which may be a potential target for obesity treatment [90].

In addition, recent findings indicate that FGF19 might have an interesting relationship with mitochondrial function(s) through the mediation of the palmitate oxidation process [91]. The excess levels of palmitate had been shown to inhibit glucose uptake, increase insulin resistance, and upregulate β-oxidation in mitochondria leading to mitochondrial overload accompanied by increased levels of reactive oxygen species (ROS) production [92,93]. FGF19 was recently found to promote the expression of mitochondrial biogenesis and antioxidant response regulators (PGC1α, TFAM, HO-1, etc.) in skeletal muscle [91]. The regulatory effects of FGF19 are postulated to involve the AMP-activated protein kinase (AMPK)/PGC1α pathway to help amend the palmitate-induced mitochondrial dysfunction in skeletal muscle [91]. Similarly, a recent study reported that treatment of FGF19 prevented mitochondrial overload and apoptosis while maintaining normal insulin signaling in mouse myoblasts (C2C12) cells with palmitate-induced dysfunction [93]. Consequently, the effects of palmitate led to activation of the mitochondria-mediated apoptosis process, inhibition of insulin signaling pathway, and myotube atrophy [92,93]. However, administration of FGF19 facilitated inhibition of the β-oxidation of palmitate, consequently alleviating mitochondrial overload and prevention of mitochondria-mediated apoptosis [93].

Another new area of research for FGF19 is its ability to induce protein synthesis by increasing the phosphorylation of eukaryotic initiation factor 4B (eIF4B) and eukaryotic initiation factor 4E (eIF4E). Both these initiation factors are part of the eIF4F complex that induces the binding of mRNA to the ribosome [80]. Furthermore, FGF19 increases the phosphorylation of the ribosomal protein subunit 6 (rpS6) and enhances protein synthesis [7]. These new areas give a better grasp of the diverse role of FGF19 in the system and may provide clues for future therapeutical developments.

FGF19 is a metabolic regulator and is associated with many diseases. Studies have demonstrated that an elevated level of serum FGF19 is observed in CKD patients and is associated with lipid and carbohydrate metabolism [94]. Moreover, the study also indicated that hemodialysis and kidney transplantation result in the reduced levels of FGF19 [94]. However, the causative factor for the increase in serum FGF19 concentration in CKD patients is still unknown. Additionally, FGF19 is believed to play a role in alcoholic hepatitis. In a recent study, it was shown that the serum levels of FGF19 were significantly increased, and the hepatic expressions of the FGF19 gene were also induced in alcoholic hepatitis patients [95]. FGF19 is also associated with type 2 diabetes mellitus (T2DM). T2DM patients often suffer from atherosclerosis, thus, understanding the underlying mechanisms involved in metabolism is crucial in understanding atherosclerosis, which may ultimately improve the development of T2DM [96,97]. Subclinical atherosclerosis is an early indicator of the onset of atherosclerosis, which could be examined by increased intima-media thickness (IMT) of arteries [98]. A recent study found that serum levels of FGF19 were positively correlated with carotid IMT in men that showed that the level of FGF19 could be a predictor of subclinical atherosclerosis in men with [97]. Additionally, reports showed that the administration of NGM282, an analog of FGF19, has proven to be a protective factor for atherosclerosis [99]. Thus, FGF19-based therapeutic agents have the potential to be further developed to improve T2DM prognosis. Diabetic cardiomyopathy is another major cause of mortality in diabetic patients in which high cardiac oxygen consumption and mitochondrial dysfunction often result in ventricular dysfunction and cardiomyocyte death [100,101]. Recent works reported that FGF19 enhanced mitochondrial function through an increase in the expression of mitochondrial biogenesis regulators, i.e., PGC1α, via the AMPK/ NF-E2-related factor 2 (Nrf2)/HO-1 pathway, thus, relieving the oxidative stress on the heart and improved diabetic cardiomyopathy [91]. Despite the positive initial findings, the roles of FGF19 in regulating mitochondrial biogenesis and antioxidant responses are still under-studied and worthy of more investigation.

Interestingly, mitochondrial dysfunction has been shown to arise in many cases of non-alcoholic fatty liver diseases (NAFLD) and promotes liver damage, induces inflammation and fibrosis, and produces a hostile microenvironment that promotes anti-apoptotic programs and mutations of hepatocytes, leading to NAFLD-driven malignant hepatocytes and HCC [102]. With FGF19 having a new and detailed relationship with mitochondria and its functions as previously discussed, one can assume that FGF19 may also be intricately linked to cancers [27,91]. Indeed, as mentioned previously in the historical perspective of FGF19, the protein was found to be heavily involved with HCC and shown to be useful for the diagnosis and prognosis of the condition [27]. One study also proposed FGF19 as a potent marker and potential driver of lung squamous cell carcinoma (LSQ) [103]. Later, studies by the same group demonstrated for the first time that overexpression of FGF19 enhanced tumor cell proliferation and metastasis in an in vivo model of LSQ [104]. The results also showed that inhibiting the mechanistic target of rapamycin (mTOR) in the in vivo LSQ models overexpressing FGF19, was an effective way to inhibit the tumor. Thus, growing evidence indicates that the FGF19-FGFR4 pathway plays a vital role in the initiation and progression of distinct types of cancers [27,105,106]. However, the exact mechanism by which FGF19 influences the development of cancer remains unknown and requires additional studies. Such studies will likely trigger new interests in targeting FGF19-FGFR4 pathways with new or existing drugs and pave the way for new treatment options in various cancers.

Experimental evidence suggests that FGF21 is a potent metabolic regulator of glucose uptake through stimulation of glucose transporter (GLUT) 1-mediated glucose uptake in 3T3L1 adipocytes [40] (Figure 2B). In addition to the role of FGF21 in the liver, this protein also acts in an endocrine manner in adipose tissues to stimulate lipolysis through PGC1α, the major regulator of mitochondrial functions and biogenesis [11,49]. Adipose tissue is classified into two parts: white adipose tissue (WAT), which has a role in energy and lipids storage, and brown adipose tissue (BAT), which functions in generating heat during the adaptive response to cold exposure [107]. In WAT, FGF21 is a potent inducer of uncoupling protein 1 (UCP1) which is mediated through PGC1α activity, and finally triggers thermogenic genes such as type II iodothyronine deiodinase (DIO2), PGC1α, and PPARα [108,109]. Cold exposure enhances circulating FGF21 levels in humans, which corresponds to increased energy expenditure and lipolysis [110]. Mitochondrial dysfunction has been implicated in several neurodegenerative disorders like Parkinson’s disease, and Alzheimer’s disease [111]. Since PGC1α has been suggested as a therapeutic target to increase mitochondrial efficacy, studies demonstrate that FGF21 can enhance mitochondrial function by increasing mitochondrial antioxidants in human dopaminergic neurons, via NAD(+)- dependent deacetylase Sirtuin-1 (SIRT1) [112]. The proposed mechanism for such enhancement is through an increase in the phosphorylation of AMPK+, which increases cellular NAD+ levels leading to activation of SIRT1 and deacetylation of PGC1α, which in turn, increases oxygen consumption and citrate synthase activity in adipocytes [113].

FGF21 is an important regulator of macronutrient intake. It has been observed that fructose or alcohol consumption robustly increases plasma FGF21 [114,115]. Similarly, a high protein restriction or high carbohydrate diet increases FGF21 levels [116]. In addition, one study indicated that FGF21 is a liver-induced endocrine FGF that enters the circulation to act on the brain to suppress simple sugar intake and sweet-taste preference without altering the protein intake [117]. However, the mechanism underlying these effects has not been reported clearly. FGF21 signaling to glutamatergic neurons in the ventromedial hypothalamus (VMH) is required to regulate sugar intake [86]. Hill et al. (2017) recently demonstrated that FGF21 is essential for coordinating the metabolic response to protein restriction in lean mice [118]. Later, the same group reported that FGF21 signaling in the brain is only required to drive the metabolic response to protein restriction [119].

The previous reports indicated that FGFs are the active factors promoting hair follicle growth and development [120]. However, the relationship between FGF21 expression and hair follicle growth and development has not been reported well. A recent study demonstrated that FGF21 affects hair follicle growth and development which may be associated with PI3k/Akt and mitogen-activated protein kinase (MAPK)/ERK signaling pathways [121].

It has been observed that the level of FGF21 fluctuates with different metabolic disorders. Indeed, elevated levels of FGF21 have been observed in patients with obesity and T2DM relative to lean subjects [122]. Additionally, Zhen et al. (2016) reported enzymes that facilitate enzymatic cleavage on FGF21 [123]. The first enzyme is dipeptidyl peptidase IV, which cleaves FGF21 at the N-terminus after the proline-2 and -proline-4 [123]. The second is fibroblast activation protein (FAP), which catalyzes the cleavage of FGF21 at the C-terminus end after proline 171, rendering FGF21 inactive [123]. Thus, inhibition of FAP is thought to be a potential approach to increase endogenous FGF21 activity for the treatment of obesity and T2DM [123]. Likewise, it has been well studied that the level of FGF21 is high in NAFLD patients [124]. Additionally, a recent study demonstrated that an FGF21-to-adiponectin ratio (FAR) is elevated in NAFLD children [125]. Therefore, FGF21 and adiponectin ratio could be a potentially useful biomarker of NAFLD in children [125].

FGF21 is a serum biomarker for several primary mitochondrial disorders (PMD) with high sensitivity and accuracy [126,127,128,129]. A recent meta-analysis of the literature which included five randomized controlled trials encompassing 718 FGF21 assessments demonstrated the utility of FGF21 as a promising biomarker for mitochondrial disease diagnosis [130]. The proposed mechanism of action regulating levels of FGF21 was by activating the mTOR-PGC1α pathway in PMD patients [131]. Another recent PMD study demonstrated that the mitochondrial integrated stress response is regulated by the autocrine and endocrine effects of FGF21 to induce step-wise changes in glucose and lipid metabolism, weight loss, and brain defects, emphasizing the importance of FGF21 as a key mediator of metabolic remodeling and progression of mitochondrial integrated stress response in PMDs [132].

The role of FGF21 in carcinogenesis is not well understood. Previous works reported an elevated serum level of FGF21 in aggressive thyroid cancer yet cannot precisely determine the origin of this upregulation of FGF21 [133]. Similarly, increased serum levels of FGF21 are also observed in breast cancers [134], renal cancer [135], and endometrial cancer [136]. These reports all indicate that FGF21 may be a suitable biomarker for diagnosis and prognosis for several types of cancers [133,134,135,136]. On the other hand, other studies have indicated that administration of recombinant FGF21 does not stimulate tumor growth in obese and diabetic patients [46,133,137], providing inconsistencies with other findings [136]. Such limited understanding of the role of FGF21 and detailed mechanism in cancer development may provide new avenues for future research.

FGF23 is a regulator of phosphate homeostasis and is synthesized by osteoblast, osteocyte, and bone marrow [138,139] (Figure 2C). It functions as a regulator of PTH metabolism through MAPK (ERK 1 and 2 and Akt) pathway [140]. The other key role of FGF23 is to suppresses the synthesis of 1α, 25-dihydroxy vitamin D3 (1,25(OH)2D3) in the kidney [62], whereas PTH and 1,25(OH)2D3 regulate the production of FGF23 [141]. A recent study reported insulin and IGF1 as negative regulators of FGF23 production. The suppression of FGF23 production by insulin and IGF1 was mediated through phosphoinositide 3-kinase (PI3K)/protein kinase B (PKB)/Akt/ forkhead box protein O1 (FOXO1) signaling [67]. FGF23 also has physiologically relevant functions in bone mineralization through FGFR3, in a klotho-independent pathway [142]. Tissue non-specific alkaline phosphatase (TNAP) plays a key role in the regulation of bone mineralization by cleaving the mineralization inhibitor, pyrophosphate, which is secreted by osteoblasts [143]. However, FGF23 is reported to be a powerful suppressor of transcription of TNAP mRNA in bone cells, which decreases the degradation of pyrophosphate and lowers the production of inorganic phosphate, leading to impaired bone mineralization [142].

A recent study identified that erythropoietin (EPO) could be a potential link between anemia, iron status, and FGF23 production [144]. An association between EPO and FGF23 was examined in healthy humans. It was found that EPO induced an increase in the levels of the C-terminus fragment of FGF23 (cFGF3) but not intact FGF23 (iFGF23) [144]. However, in mice, it has been observed that EPO first elevates C-term FGF23 and then iFGF23 [145]. It has been demonstrated that FGF23 controls the production of Fetuin A (ASGH), a serum protein with anti-calcification activity in osteocytes [146]. In addition, another study also identified the involvement of FGF23 in the regulation of Fetuin A in the liver with a biphasic effect [147].

Although the expression of FGF23 was identified in skeletal muscle tissue, its relationship with the skeletal muscle and mitochondrial functions merits further investigation [148,149]. However, a recent study demonstrated that physical exercise induces high expression of FGF23 resulting in an increased exercise endurance [148]. In addition, exogenous treatment of FGF23 contributed to reduced exercise-induced ROS and H₂O₂ production, increased PPARδ and citrate synthase activity, thus, enhancing mitochondrial function in skeletal muscle [148]. However, the new relationship between FGF23, mitochondrial functions, and skeletal muscle is not well understood and warrants more research to understand the molecular mechanisms of FGF23 regulation.

It is a well-known fact that diseases characterized by excessive blood concentrations of intact FGF23 lead to renal phosphate wasting and low-circulating 1,25(OH)2D3 levels in patients with functional kidney [150]. In humans, the expression of FGF23 is modified in several diseases. Elevated levels of FGF23 were reported mainly in genetic X-linked hypophosphatemia (XLH) and non-genetic tumor-induced osteomalacia (TIO), a rare condition of hypophosphatemia caused due to increased levels of FGF23 and associated with low levels of 1,25-(OH)2D [151]. Elevated levels of FGF23 have been quantified in a majority of XLH patients and hypophosphatemia mice, an orthologous animal model of XLH [152]. Furthermore, elevated levels of FGF23 are also associated with CKD-mineral bone disorder [153]. CKD is an extremely complex disease with complications like renal failure and bone mineral disorder. It has been observed that elevated levels of FGF23 were correlated with bone mineral density in the lumbar spine site in CKD patients [154]. Thus, FGF23 can be used to predict bone loss at the lumbar spine site in the end stages of CKD [154]. On the other hand, a low level of FGF23 is reported in hyperphosphatemic tumoral calcinosis [155].

Mutation in FGF23 is associated with ADHR through a gain of function mutation(s) in the FGF23 gene [56]. This mutation affects residue at positions 176 and 179, often called the RXXR site, by the subtilisin-like pro-protein convertases (SPC), which prevents proteolytic cleavage of FGF23 [56]. Later, a novel missense mutation was identified in autosomal recessive hyperphosphatemic familial tumoral calcinosis patients and the level of FGF23 was found to be lower [156].

FGF23 has been identified as a mediator of left-ventricular hypertrophy [157,158]. Angiotensin II (ATII) is also a strong trigger for the development of cardiac hypertrophy [159]. Interestingly, one study demonstrated that FGF23 enhanced the intracellular expression of ATII from cardiomyocytes in an autocrine manner [159]. The study suggested that the ATII’s FGF23-induced enhanced synthesis may work through the secretory pathway that involved angiotensin-converting enzyme, but the exact mechanism of this relationship is still unknown [159]. However, the increased expression of both ATII and FGF2-FGFR4 signaling induced the development of cardiac hypertrophy through IP3-nuclear Ca²⁺-dependent signaling [159]. Both in vivo and in vitro studies indicated that FGF23 promotes cardiac hypertrophy and fibrosis through the activation of the local renin–angiotensin–aldosterone system in the heart [160].

FGF1 and FGF2 are prototype members of the fibroblast growth factor family. Initially, FGF2 was found to be a 146 amino acid long protein isolated from the pituitary gland [2]. Like all the paracrine FGFs, FGF2 binds strongly to glycosaminoglycans such as heparin sulfate, which in turn helps ease the purification of FGF2 using heparin-Sepharose affinity chromatography [174]. Just like other members of the FGF family, FGF2 shares the common “β-trefoil fold” [175] (Figure 4D). Out of 146 amino acids, 26 residues are conserved in all members of the FGF family. Of these 26, 7 are glycine/proline (G/P) and 13 are hydrophobic amino acids. The conserved G/P forms the turns between the β-strands, thereby playing a major role in the structural scaffold. FGF2 has 4 cysteine residues (Cys 33, 77, 95, and 100). Of these four cysteines, Cys33 and 100 are conserved amongst the FGF family members [2].

As discussed in the previous section, FGF2 is a heparin-binding protein. The binding of FGF2 to heparin induces dimerization of FGF, which in turn, is a prerequisite for FGFR activation and signaling [177]. FGF2 has two different receptor binding sites namely, primary and secondary. These binding sites were identified based on site-directed mutagenesis studies. The primary binding site is conserved in the FGF family and provides a significant binding interaction with FGFR. This primary binding site comprises of Y24, E96, N101, Y103, L140, and M142 [165,166]. Alternatively, the secondary receptor binding site consists of K110, Y111, and W114 [178,179,180,181].

A conservative structural similarity exists between FGF19 and other FGF family members. Like other FGFs, FGF19 forms a β-trefoil like structure (Figure 4A). β strands 1, 4, 5, 8, 9, and 12 are involved in the formation of β-trefoil with a well-formed β barrel at the base of the trefoil. Extended β-sheets of strands 1 and 9 form β-hairpin-like structures [13]. One of the special features that separate FGF19 from other FGFs is the presence of two disulfide bonds. These two disulfide bonds are situated to stabilize β hairpins formed by the β sheets of strand-1 and -9. The first disulfide bond is located between -C58 of β-strand 2 and C70 of β-strand 3, and the second is situated between C102 of β-strand 6 and C120 of a loop between strands-7 and -8. C120, in the case of FGF19, is conserved across the FGF family [4]. The first disulfide bond in FGF19 aids in holding the extended loop formed by strands-1 and -2. The second disulfide bond stabilizes the protein backbone. Correlation of the extended loop between strands-7 and -8 by only one residue and inclusion of disulfide link leads to correct folding of FGF19, thereby enhancing the stability of the protein [13].

One structural difference between FGF19 and other FGFs is the presence of an extended N-terminus [13]. The presence of this extended loop is also observed in FGF7 and FGF10 for providing a key interaction with the “b” splice form of FGFR2 [182], but there is no evidence to suggest a functional role for extended β1 in FGF19. FGF19 also shows an extended loop of eight amino acids linking strands β1 and β2 [4]. This conformation is stabilized by the heparin with its sulfate ions forming hydrogen bonds with the amide groups of FGF19 (H53, L55, and S56). Additionally, the extended loop interaction with the sulfate group of heparin, makes it functionally relevant as this is spatially closer to the heparin-binding domain of FGF19 [13].

Another most important structural feature revolves around strand β11 of FGF19 [13] (Figure 4A). Unlike other FGFs, this strand is missing a loop observed in the heparin-binding FGFs [179,183] (Figure 4A). It has been demonstrated that β11 is present in most of the FGF subfamily members and is responsible for heparin-binding [182,183] (Figure 4D). Therefore, the disordered loop in β11 of FGF19 explains the reduced heparin-binding affinity. This conformational change (disorientation) brings great significance to the discussion related to the requirement of heparin-binding for FGF downstream signaling [184]. In particular, the disorientation allows FGF19 to have a low affinity towards heparin thus, permitting the protein to diffuse into the blood and act as a hormone, while evading its paracrine/autocrine functions [7,15,184]. Interestingly, according to Wu et al. (2007), FGF19 shows increased FGFR4 activation with increasing heparin concentration [185]. However, heparin-binding experimental data suggest FGF19 requires lower concentrations of NaCl (less than 400 mM) to release from heparin-bound column compared to the FGF1 subfamily members (1.5 M). FGF1 and FGF2 form strong interactions with heparin through the backbone and sulfate groups around the disoriented portion of FGF19. This renders FGF19 sterically unconducive to bind to heparin in the same manner as FGF1 and FGF2 [13].

Like other FGFs, FGF21 is a 181 amino-acid protein that functions in an endocrine fashion and requires KLB, a single transmembrane glycoprotein to bind to FGFR [53]. FGF21 has a 13-residue N-terminus and a 40-residue C-terminus with a β-trefoil core domain (FGF21 core) [44,53] (Figure 4B). However, unlike other members of the endocrine FGF subfamily (FGF19 and 23), there is only limited information regarding the structure of FGF21. Most recently, the core structure of FGF21 was elucidated by nuclear magnetic resonance spectroscopy (Figure 4B), and the crystal structure of the C-terminus domain—KLB binary structure was determined at high resolution [53,186].

The core sequence of FGF21 was thought to have a typical 120 amino acid β-trefoil core structure like many FGFs [43]. However, it has been recently indicated that the core region of FGF21 only has 11 β-strands (1–10, 12) and misses the canonical β-11 strand. β10 is linked to β12 through a proline-rich 18-residue disordered random coil [53]. Such replacement leads to divergence in topology and structures of FGF21 compared to typical FGFs and even other endocrine FGFs, FGF19 and 23. The β10-β12 region of FGF21 is shorter than that of FGF19 and FGF23, with little to no sequence identity shared amongst the three proteins [187]. Additionally, the overall sequence identity increases to 40–45% if this region is omitted during multiple sequence alignment of all endocrine FGFs, indicating it to be the key region accounting for the low sequence identity amongst the members of endocrine FGFs [187]. Another region of endocrine FGFs called the HBS region (β1-β2 loop), also shares little sequence identity and structure amongst its members [167]. If the HBS region was omitted, the alignment identity of the members will increase to 40% [167]. Furthermore, additional data reveals that the β2-β3 hairpin structures and neighboring segments also display high flexibility, which decreases the stability of the protein [53].

The N-terminus and C-terminus of FGF21 play different roles when the protein is bound to FGFR and KLB [43]. Specifically, the C-terminus has been shown to constitute the binding site for KLB and the N-terminus domain plays a crucial role in receptor activation [43,44]. Serial truncations of the C-terminus domain of FGF21 weakened the ability of the protein to interact and bind to KLB [43,44]. In contrast, when the N-terminus was subjected to the same serial truncations, it did not affect the ability of FGF21 to bind to KLB [43,44]. Instead, this truncation affected the efficacy of FGFR activation by FGF21 [43,44]. It is reported that residues 198–200 of FGF21 C-terminus (FGF21CT) are flexible and can be potentially accessible for proteolysis to abolish the binding of FGF21 to the extracellular binding sites in human KLB (sKLB) [186]. Furthermore, FAP (introduced in Section 2.4) is believed to be responsible for cleaving FGF21 at proline 171 and inactivating the protein, thus providing the mechanism for termination of FGF21 signaling [123,188]. Interestingly, it is also believed that FGF21 signaling occurs solely through FGFR and not through the co-receptor, KLB, because KLB only has a few amino acid residues in its intracellular domain [43]. Therefore, the N-terminus of FGF21 is seen as a point of interest to investigate the efficacy of FGFR activation of FGF21 [43].

FGF23 is a 32 kDa protein produced in the bone by osteoblasts and osteocytes under physiological conditions. Its co-receptor, KLA, is mainly synthesized in the distal kidney tubules, parathyroid gland, and choroid plexus [189,190]. These tissues are, therefore, the targets for FGF23 [191,192]. KLA binds to the C-terminus of FGF23 and FGFR to accelerate the ligand-receptor affinity [187]. The protein is produced in the bone and is involved mainly in the mineral metabolism of phosphate and vitamin D [193]. FGF23 decreases the reabsorption of phosphate from urine and the synthesis of 1,25(OH)2D3, vitamin D [193]. The low affinity of FGF23 to heparin allows it to enter the circulation and function as an endocrine secretion [194].

Like other endocrine FGFs, FGF23 has an atypical β-trefoil fold and does not have a β11 strand [187] (Figure 4C). β10 and β12 conformation of FGF23 is different from the β10 and β12 conformation of the paracrine FGFs [187]. Specifically, FGF23 lacks the β11 strand in its core structure, a consistent characteristic shared amongst FGF19, 21, and 23 [187]. Such divergence explains the non-canonical β-trefoil core structure of FGF23 [187]. Additionally, FGF23 and its endocrine FGF cousins also have a shorter β9-10 loop, compared to paracrine FGFs, and may influence the conformation of the β10-12 loop [187]. Despite the seemingly uniting structure features amongst endocrine FGFs, there exist distinct differences between them, especially in the β1-2 region and HBS region, as described previously [187].

Another difference amongst the endocrine subfamily members is the C-terminus sequence. The C-terminus of FGF23 differs from those of FGF19 and FGF21 in possessing 89 amino acids that form two parts, called R1 and R2 [69]. Both parts bind to KLA with high affinity, while FGF19 and FGF21 bind to KLB through the same binding site [69]. In mammals, the R2 is flanked by two cysteine residues Cys206 and Cys244. The disulfide bridging of two cysteine does not influence the susceptibility of FGF23 proteolytic digestion. Also, R2 in its oxidized form can form an active ternary complex with KLA and FGFR1c [69]. Interestingly, the 73-residue C-terminus of FGF23 is suggested to be innately flexible that causes difficulties in the crystallization process of FGF23 [187].

Many important structural and physiological significances of FGF23 involve its C-terminus. For example, circulating levels of physiologically active FGF23 are regulated by a highly conserved proteolytic cleavage site at the C-terminus to produce two forms of FGF23 in the bloodstream [56,195,196,197]. The first form is the full-length form called wild-type FGF23 that contains Tyr25-Ile252 and is physiologically active. The second form is the truncated form consisting of residues only from Tyr25-Arg179 called core FGF23 that does not have the 73 amino acids of the C-terminus, thus cannot assert its activities through the C-terminus [56,195,196,197]. This conserved cleavage site within FGF23 is a furin proconvertase recognition site and it ranges from Arg176 to Arg179, often called the RXXR (RHTR¹⁷⁹) site [56,197,198]. This cleavage is processed by SPC and cleaves between arginine 179 and serine 180, which leads to the inactivation of FGF23 [199]. As mentioned previously, this cleavage site is often mutated in ADHR patients [56,197,198]. The mutations usually replace arginine residues with glutamine at either position 176 or 179 [56,197]. Another mutation was also found at position 179, where arginine is replaced by tryptophan [56,197]. The mutations result in an FGF23 mutant with resistance to proteolysis and an increased half-life, leading to elevated levels of 1,25(OH)2D3, and decreased levels of serum phosphorous [56,197]. Both phenotypes are characteristics of ADHR condition [56,197]. Thus, the cleaving process is essential in the normal regulation of phosphate homeostasis [200].

FGF23 undergoes multiple post-translational modifications that influence the stability and susceptibility of FGF23 against proteolysis. For example, to protect FGF23 from C-terminus cleavage, the protein is O-glycosylated by GalNAc-transferase at the C-terminus RXXR cleavage site [199,200]. Specifically, within the RXXR cleavage site, there is a threonine residue at position 178 that is shown to be an O-glycosylated position for FGF23 [200]. Additionally, FGF23 undergoes modification through disulfide bond formation (C95–C113) and O-glycosylation by uridine diphosphate-N-acetyl-α-D-galactosamine: polypeptide N-acetyl galactosaminyltransferase 3 at multiple sites to produce the mature 32 kDa protein [201]. Another modification of FGF23 is its phosphorylation at the region of the cleavage site [202]. The serine residue at position 180 plays a dual role: (1) a phosphorylation site for FGF23 and (2) a cleavage site for SPC [56,202]. This phosphorylation process is conducted by a kinase family called: family with sequence similarity 20, member C (Fam20C), which phosphorylates proteins at Ser-X-Glu motifs [202]. Fam20C phosphorylation is believed to prevent the glycosylation at the cleavage site as well as expose the site for the subsequent proteolysis process [202]. Combining with the other modification processes, FGF23 shows to have a dynamic and complex regulatory system that warrants further investigations.

Paracrine FGFs interact and activate FGFRs through a high-affinity interaction with heparan sulfate proteoglycan (HSPG) [53,217] (Figure 4D). Such appearance of HSPG with high affinity to FGFs helps induce notable and prolonged FGFR dimerization [218]. On the other hand, the endocrine subfamily members have a weak binding affinity to HSPG [43,44,46,53]. This low affinity to HSPG is believed to be caused by aberrant conformation with the entailed steric hindrance of the β10–12 regions (Figure 4A–C) as indicated previously [53]. However, it is established that FGF21 requires KLB to interact with its cognate receptor [187,206,219] to the aforementioned list of FGF21-binding receptors: FGFR1c, 2c, 3c, and 4 [217,220].

The interactions between FGF21 and KLB through FGF21 C-terminus is well-documented [217]. The structure of FGF21CT and sKLB complex revealed that FGF21CT binds to the interface between two domains D1 and D2 of the sKLB [186] (Figure 6B). On these two domains of sKLB, there are two binding sites for FGF21CT, called sites 1 and 2, that are 30 Å apart [186]. Site 1 is on the domain D1 and binds to FGF21CT in the segment, P186-V197, through hydrophobic interactions with several β-turns [186]. Site 2 is on domain D2 and binds to FGF21CT in the segment of S200-S209, which contains a high amount of hydroxyl side chain [186]. Interestingly, this second binding site mimics the binding interactions between glycoside hydrolase 1 enzyme and its substrate. Furthermore, the S204-P205-S206 sugar-mimicking motif at the end of FGF21CT interacts strongly with the “catalytic” E693 of sKLB and resembles the substrate interactions in GH1 [186]. Combining these aspects, the data suggest that FGF21 may be mimicking a glycosidic substrate [186].

The S-P-S sequence motif is also present at the C-terminus of FGF19, specifically S211-P212-S213, which helps in binding to KLB (Figure 4A and Figure 6A) [186]. FGF19 and 21 present similar mechanistic interactions while interacting with KLB (Figure 6A,B), which is different from FGF23 that is angled towards KLA (Figure 6C) [186]. This is because FGF23 does not contain a similar sequence motif, making it unable to bind to KLB but binds to KLA through different mechanistic pathways [186]. Another important motif called the D-P-F/L sequence, D198-P199-F200 specifically, is also involved in the interaction with klotho through hydrogen bonding to maintain the complex conformation of FGF19 and KLB [186]. This D-P-F/L motif is also conserved in FGF21 and 23, specifically D192-P193-L194 in FGF21 and D188-P189-L190 in FGF23, contributing to the same function of binding to their respective klotho proteins [69,186] (Figure 4C and Figure 6C).

The N-terminus is not required for KLB binding, but it does contribute towards the binding and activation of FGF21 to FGFR [43,44]. FGFR1c is shown to be a preferred receptor for binding to FGF21 [217]. Removal of 5 amino acids from the N-terminal end of FGF21 appears to reduce responses in signaling and functional activity [44]. As mentioned previously, FGFRs contain 3 immunoglobin (Ig)-like domains (D1-D3) and a linker between D1 and D2 domains [217]. Interestingly, the autoinhibitory D1/linker region of FGFR1c, which comprises of D1 domain and D1-D2 linker, can suppress the FGF21/FGFR1c interaction and FGFR1c//KLB interaction, rendering FGF21 unable to stimulate signaling with FGFR1c alone without KLB [217].

FGF21 is suggested to interact with D2-D3 extracellular regions of FGFR1c directly through its N-terminus [217](Figure 6B). Furthermore, the β1-β2 loop in FGF21 is important for the FGFR interaction and activation as it is the direct contact to the D2 domain of FGFR1c [53]. However, this β1-β2 loop can be disturbed by the destruction of another loop, the β2-β3 loop, thus affecting the binding of FGF21 to the D2 domain of FGFR1c [53]. The β2-β3 region of FGF21 is also quite important due to its role in providing stability to the triangular array architecture of FGF21. This region is also flexible, thus making FGF21 unfavorable for the interaction with FGFR, allowing FGF21 to escape to the local extracellular matrix [53]. Although the direct interaction of FGF21 and FGFR1c without KLB is weak and transient, it is thought to be similar to paracrine FGFs-FGFRs in a 2:2 ratio complex, with multiple points of interactions [169,217].

FGF23 binds and activates FGF receptor tyrosine kinases (FGFRs) like FGFR1c, FGFR3c, and FGFR4 to produce downstream signaling and subsequently, regulates phosphate and vitamin D levels [187,191,192,221]. There is a preference for FGF23 to bind to the c isoform of FGFR1–3 and FGFR4. This preference was known to be originated during the interaction studies between FGF23 and FGFR1c receptors. These studies showed that the signaling of FGF23 was negatively affected when the specific serine residue in the FGFR1 c isoform was replaced by a tyrosine residue to convert it to the b isoform of the receptor [214]. FGF23 was found to bind to FGFR1c between the D2 and D3 domains. However, FGF23 makes weaker contacts with D3 and D2-D3 linkers when compared with the paracrine FGFs [214].

Another important difference between the interaction of FGF23 with its receptor and paracrine FGFs with their receptors is the presence of co-receptor KLA [222]. Studies have shown that KLA enhanced the binding affinity of FGF23 to FGFR by a factor of 20, further emphasizing the role of KLA in the successful binding and activation of FGF23 to FGFR [222]. The R1 and R2 sections of the C-terminus of FGF23 play an important role in binding FGF23 to its co-receptor KLA [69,214]. This is because both R1 and R2 have D-P-L/F motifs and specific Asp188-Pro-Leu-Asn-Val-Leu193 residues in the C-terminus of FGF23 form a compact, rigid cage-like conformation when bound to its co-receptor KLA [69,214]. These 2 parts with similar D-P-L/F motifs indicate that one molecule of FGF23 might have two binding sites for KLA [69]. Variants of FGF23, containing either R1 or R2 repeat, show similar binding affinities to KLA when compared to the native FGF23 [69,186], thereby permitting the use of either FGF23 variants as antagonists in studies related to the functions of FGF23 in vitro and in vivo [69,186]. Interestingly, this D-P-L/F motif is conserved amongst endocrine FGFs to serve as interaction points for klotho proteins [69,186]. Although all vertebrate FGF23 proteins have long C termini, only the mammalian FGF23 proteins have a second repeat (R2) that is homologous to the klotho binding regions of FGF19, 21, and 23 [69].

The crystal structure of the ternary complex of FGF23, FGFR1c ectodomain (comprises of domains D2, D3, and D2-D3 linker) and KLA, shows that KLA contains two domains, called KL1 and 2, which are connected by a short proline-rich stiff linker (Pro-507 to Pro-514) (Figure 6C). KL1 is on top of KL2, held by a few interdomain contacts between KL1 (the N-terminus preceding the β1 strand and the α7 helix) and KL2 (the β5α5, β6α6 loops, and the α7 helix) [214]. These interdomain interactions create a deep cleft between the 2 KL domains and merge with the β-barrel structure in KL2 to form a large pocket [214]. This large pocket is the binding site for the C-terminus tail of FGF23 past the protein’s RXXR proteolytic cleavage site [214] (Figure 7). At the same time, the long β1α1 loop of KL2 clamps on FGFR1c’s D3 domain and assists in connecting FGFR1c to KLA [214]. Due to this interaction, this part of KL2 is called the receptor binding arm (RBA) [214]. Both soluble and transmembrane KLAs have the same function as the co-receptors for FGF23 signaling [214]. However, the soluble form of KLA that does not have the binding arm (RBA), fails to form a binary complex with FGFR1c ectodomain in solution and hence could not support FGF23 signaling [214,223].