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Molecular Insights into the Klotho-Dependent, Endocrine Mode of Action of Fibroblast Growth Factor 19 Subfamily Members▿

机译:分子洞察力对成纤维细胞生长因子19亚家族成员的Klotho依赖性内分泌作用的作用

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摘要

Unique among fibroblast growth factors (FGFs), FGF19, -21, and -23 act in an endocrine fashion to regulate energy, bile acid, glucose, lipid, phosphate, and vitamin D homeostasis. These FGFs require the presence of Klotho/βKlotho in their target tissues. Here, we present the crystal structures of FGF19 alone and FGF23 in complex with sucrose octasulfate, a disaccharide chemically related to heparin. The conformation of the heparin-binding region between β strands 10 and 12 in FGF19 and FGF23 diverges completely from the common conformation adopted by paracrine-acting FGFs. A cleft between this region and the β1-β2 loop, the other heparin-binding region, precludes direct interaction between heparin/heparan sulfate and backbone atoms of FGF19/23. This reduces the heparin-binding affinity of these ligands and confers endocrine function. Klotho/βKlotho have evolved as a compensatory mechanism for the poor ability of heparin/heparan sulfate to promote binding of FGF19, -21, and -23 to their cognate receptors.
机译:在成纤维细胞生长因子(FGFs)中,FGF19,-21和-23以内分泌方式发挥独特作用,以调节能量,胆汁酸,葡萄糖,脂质,磷酸盐和维生素D稳态。这些FGF需要在其靶组织中存在Klotho /βKlotho。在这里,我们介绍了单独的FGF19和FGF23与蔗糖八硫酸盐(一种与肝素化学相关的二糖)的晶体结构。 FGF19和FGF23中β链10和12之间的肝素结合区构象完全不同于旁分泌作用FGF所采用的常见构象。在该区域与另一个与肝素结合的区域β1-β2环之间的裂口阻止了肝素/硫酸乙酰肝素与FGF19 / 23的骨架原子之间的直接相互作用。这降低了这些配体的肝素结合亲和力并赋予了内分泌功能。 Klotho /βKlotho已发展成为一种补偿机制,可降低肝素/硫酸乙酰肝素促进FGF19,-21和-23与它们的同源受体结合的能力。

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