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The breadth of FGF21's metabolic actions are governed by FGFR1 in adipose tissue

机译:FGF21代谢作用的广度受脂肪组织中FGFR1的控制

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FGF21 is a multifunctional metabolic regulator. The co-factor @bKlotho (KLB) allows FGF21 to signal via FGF receptors. Given the widespread nature of FGFR expression and KLB presence in several organs, it remains unclear which tissue/FGFR isoform determine FGF21 action. Here we show that deletion of FGFR1 in fat (FR1KO) leads to a complete ablation of FGF21 stimulated transcriptional activity in this tissue. Furthermore, FR1KO mice showed no FGF21-mediated lowering of plasma glucose, insulin and triglycerides, altered serum levels of adipokines, no increase in energy expenditure, but preserved reductions in serum/liver FFAs as compared to wild type mice. Of importance, the anti-glycaemic actions of FGF19 were fully evident in FR1KO mice implying that FGF19 functions in a FGFR1/adipose independent manner. Taken together, our findings reveal the existence of an adipose FGFR1 driven axis of cross-tissue communication which defines several aspects of FGF21 biology and delineates mechanistic distinctions between FGF21 and FGF19.
机译:FGF21是多功能代谢调节剂。辅因子@bKlotho(KLB)允许FGF21通过FGF受体发出信号。鉴于FGFR表达的普遍性质和KLB在多个器官中的存在,尚不清楚哪个组织/ FGFR同工型决定FGF21的作用。在这里,我们表明脂肪中的FGFR1缺失(FR1KO)导致该组织中FGF21刺激的转录活性完全消融。此外,与野生型小鼠相比,FR1KO小鼠未表现出FGF21介导的血浆葡萄糖,胰岛素和甘油三酸酯降低,脂联素的血清水平改变,能量消耗没有增加,但保留了血清/肝脏FFA的降低。重要的是,在FR1KO小鼠中FGF19的抗血糖作用是完全明显的,这表明FGF19以FGFR1 /脂肪独立的方式起作用。综上所述,我们的发现揭示了由脂肪FGFR1驱动的跨组织通讯轴的存在,该轴定义了FGF21生物学的几个方面,并描绘了FGF21和FGF19之间的机械区别。

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