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分化和代谢所需转录因子网络的调控。

Regulation of a transcription factor network required for differentiation and metabolism.

作者信息

Duncan S A, Navas M A, Dufort D, Rossant J, Stoffel M

机构信息

Laboratories of Molecular Cell Biology and Metabolic Diseases, Rockefeller University, New York, NY 10021, USA.

出版信息

Science. 1998 Jul 31;281(5377):692-5. doi: 10.1126/science.281.5377.692.

Abstract

Hepatocyte nuclear factors (HNFs) are a heterogeneous class of evolutionarily conserved transcription factors that are required for cellular differentiation and metabolism. Mutations in HNF-1alphaand HNF-4alpha genes impair insulin secretion and cause type 2 diabetes. Regulation of HNF-4/HNF-1 expression by HNF-3alpha and HNF-3beta was studied in embryoid bodies in which one or both HNF-3alpha or HNF-3beta alleles were inactivated. HNF-3beta positively regulated the expression of HNF-4alpha/HNF-1alpha and their downstream targets, implicating a role in diabetes. HNF-3beta was also necessary for expression of HNF-3alpha. In contrast, HNF-3alpha acts as a negative regulator of HNF-4alpha/HNF-1alpha demonstrating that HNF-3alpha and HNF-3beta have antagonistic transcriptional regulatory functions in vivo. HNF-3alpha does not appear to act as a classic biochemical repressor but rather exerts its negative effect by competing for HNF-3 binding sites with the more efficient activator HNF-3beta. In addition, the HNF-3alpha/HNF-3beta ratio is modulated by the presence of insulin, providing evidence that the HNF network may have important roles in mediating the action of insulin.

摘要

肝细胞核因子(HNFs)是一类异质性的、进化上保守的转录因子,对于细胞分化和代谢是必需的。HNF-1α和HNF-4α基因的突变会损害胰岛素分泌并导致2型糖尿病。在胚状体中研究了HNF-3α和HNF-3β对HNF-4/HNF-1表达的调控,其中一个或两个HNF-3α或HNF-3β等位基因被灭活。HNF-3β正向调节HNF-4α/HNF-1α及其下游靶点的表达,提示其在糖尿病中发挥作用。HNF-3β对于HNF-3α的表达也是必需的。相反,HNF-3α作为HNF-4α/HNF-1α的负调节因子,表明HNF-3α和HNF-3β在体内具有拮抗的转录调节功能。HNF-3α似乎并不作为经典的生化阻遏物起作用,而是通过与更有效的激活剂HNF-3β竞争HNF-3结合位点来发挥其负面作用。此外,胰岛素的存在可调节HNF-3α/HNF-3β的比例,这为HNF网络在介导胰岛素作用中可能发挥重要作用提供了证据。

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