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肝 FGF21 表达在出生时通过 PPARalpha 被诱导,以响应奶的摄入,并有助于新生儿棕色脂肪的产热激活。

Hepatic FGF21 expression is induced at birth via PPARalpha in response to milk intake and contributes to thermogenic activation of neonatal brown fat.

机构信息

Departament de Bioquímica i Biologia Molecular, Institut de Biomedicina de la Universitat de Barcelona and CIBER Fisiopatologia de la Obesidad y Nutrición, Barcelona, Catalonia, Spain.

出版信息

Cell Metab. 2010 Mar 3;11(3):206-12. doi: 10.1016/j.cmet.2010.02.001.

DOI:10.1016/j.cmet.2010.02.001
PMID:20197053
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2847690/
Abstract

Plasma FGF21 levels and hepatic FGF21 gene expression increase dramatically after birth in mice. This induction is initiated by suckling, requires lipid intake, is impaired in PPARalpha null neonates, and is mimicked by treatment with the PPARalpha activator, Wy14,643. Neonates exhibit reduced FGF21 expression in response to fasting, in contrast to the upregulation occurring in adults. Changes in FGF21 expression due to suckling or nutritional manipulations were associated with circulating free fatty acid and ketone body levels. We mimicked the FGF21 postnatal rise by injecting FGF21 into fasting neonates, and found that this enhanced the expression of genes involved in thermogenesis within brown fat, and increased body temperature. Brown adipocytes treated with FGF21 exhibited increased expression of thermogenic genes, higher total and uncoupled respiration, and enhanced glucose oxidation. We propose that the induction of FGF21 production by the liver mediates direct activation of brown fat thermogenesis during the fetal-to-neonatal transition.

摘要

出生后,小鼠血浆 FGF21 水平和肝脏 FGF21 基因表达显著增加。这种诱导始于哺乳,需要脂肪摄入,在 PPARα 缺失的新生鼠中受损,并可被 PPARα 激活剂 Wy14,643 模拟。与成人发生的上调相反,禁食会导致新生鼠的 FGF21 表达减少。由于哺乳或营养处理引起的 FGF21 表达变化与循环游离脂肪酸和酮体水平有关。我们通过向禁食的新生鼠注射 FGF21 来模拟 FGF21 出生后的增加,发现这增强了棕色脂肪中与产热相关的基因的表达,并升高了体温。用 FGF21 处理的棕色脂肪细胞表现出产热基因表达增加、总呼吸和非耦联呼吸增加以及葡萄糖氧化增强。我们提出,肝脏中 FGF21 产生的诱导介导了胎儿到新生儿过渡期间棕色脂肪产热的直接激活。

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