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本文引用的文献

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Regulation of insulin gene transcription.胰岛素基因转录的调控
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The role of the insulin control element and RIPE3b1 activators in glucose-stimulated transcription of the insulin gene.胰岛素控制元件和RIPE3b1激活剂在胰岛素基因葡萄糖刺激转录中的作用。
Mol Endocrinol. 1995 Nov;9(11):1468-76. doi: 10.1210/mend.9.11.8584024.
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The pancreatic islet factor STF-1 binds cooperatively with Pbx to a regulatory element in the somatostatin promoter: importance of the FPWMK motif and of the homeodomain.胰岛因子STF-1与Pbx协同结合于生长抑素启动子中的一个调控元件:FPWMK基序和同源结构域的重要性。
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Glucose modulates the binding of an islet-specific factor to a conserved sequence within the rat I and the human insulin promoters.葡萄糖调节一种胰岛特异性因子与大鼠I型和人胰岛素启动子内保守序列的结合。
Proc Natl Acad Sci U S A. 1993 May 1;90(9):3865-9. doi: 10.1073/pnas.90.9.3865.
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The insulin gene contains multiple transcriptional elements that respond to glucose.胰岛素基因包含多个对葡萄糖作出反应的转录元件。
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Glucose modulates the binding activity of the beta-cell transcription factor IUF1 in a phosphorylation-dependent manner.葡萄糖以磷酸化依赖的方式调节β细胞转录因子IUF1的结合活性。
Biochem J. 1994 Oct 15;303 ( Pt 2)(Pt 2):625-31. doi: 10.1042/bj3030625.
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Pit-1 determines cell types during development of the anterior pituitary gland. A model for transcriptional regulation of cell phenotypes in mammalian organogenesis.Pit-1在前脑垂体发育过程中决定细胞类型。哺乳动物器官发生中细胞表型转录调控的模型。
J Biol Chem. 1994 Nov 25;269(47):29335-8.
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Transcriptional regulation of the human insulin gene is dependent on the homeodomain protein STF1/IPF1 acting through the CT boxes.人类胰岛素基因的转录调控依赖于通过CT盒起作用的同源结构域蛋白STF1/IPF1。
Proc Natl Acad Sci U S A. 1994 Oct 25;91(22):10465-9. doi: 10.1073/pnas.91.22.10465.
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Insulin-promoter-factor 1 is required for pancreas development in mice.胰岛素启动因子1是小鼠胰腺发育所必需的。
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在正常和转化的胰岛细胞中差异激活胰岛素基因的β细胞葡萄糖敏感因子的纯化。

Purification of the beta-cell glucose-sensitive factor that transactivates the insulin gene differentially in normal and transformed islet cells.

作者信息

Marshak S, Totary H, Cerasi E, Melloul D

机构信息

Department of Endocrinology and Metabolism, Hebrew University Hadassah Medical Center, Jerusalem, Israel.

出版信息

Proc Natl Acad Sci U S A. 1996 Dec 24;93(26):15057-62. doi: 10.1073/pnas.93.26.15057.

DOI:10.1073/pnas.93.26.15057
PMID:8986763
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC26355/
Abstract

The beta cell-specific glucose-sensitive factor (GSF), which binds the A3 motif of the rat I and human insulin promoters, is modulated by extracellular glucose. A single mutation in the GSF binding site of the human insulin promoter abolishes the stimulation by high glucose only in normal islets, supporting the suggested physiological role of GSF in the glucose-regulated expression of the insulin gene. GSF binding activity was observed in all insulin-producing cells. We have therefore purified this activity from the rat insulinoma RIN and found that a single polypeptide of 45 kDa was responsible for DNA binding. Its amino acid sequence, determined by microsequencing, provided direct evidence that GSF corresponds to insulin promoter factor 1 (IPF-1; also known as PDX-1) and that, in addition to its essential roles in development and differentiation of pancreatic islets and in beta cell-specific gene expression, it functions as mediator of the glucose effect on insulin gene transcription in differentiated beta cells. The human cDNA coding for GSF/IPF-1 has been cloned, its cell and tissue distribution is described. Its expression in the glucagon-producing cell line alpha TC1 transactivates the wild-type human insulin promoter more efficiently than the mutated construct. It is demonstrated that high levels of ectopic GSF/IPF-1 inhibit the expression of the human insulin gene in normal islets, but not in transformed beta TC1 cells. These results suggest the existence of a control mechanism, such as requirement for a coactivator of GSF/IPF-1, which may be present in limiting amounts in normal as opposed to transformed beta cells.

摘要

β细胞特异性葡萄糖敏感因子(GSF)可与大鼠Ⅰ型和人胰岛素启动子的A3基序结合,并受细胞外葡萄糖的调节。人胰岛素启动子GSF结合位点的单个突变仅在正常胰岛中消除了高葡萄糖的刺激作用,这支持了GSF在胰岛素基因葡萄糖调节表达中所暗示的生理作用。在所有胰岛素产生细胞中均观察到GSF结合活性。因此,我们从大鼠胰岛素瘤RIN中纯化了这种活性,发现一种45 kDa的单一多肽负责DNA结合。通过微量测序确定的其氨基酸序列提供了直接证据,表明GSF对应于胰岛素启动子因子1(IPF-1;也称为PDX-1),并且除了在胰岛发育和分化以及β细胞特异性基因表达中发挥重要作用外,它还作为葡萄糖对分化的β细胞中胰岛素基因转录作用的介质。编码GSF/IPF-1的人cDNA已被克隆,并描述了其细胞和组织分布。它在产生胰高血糖素的细胞系αTC1中的表达比突变构建体更有效地激活野生型人胰岛素启动子。结果表明,高水平的异位GSF/IPF-1抑制正常胰岛中人胰岛素基因的表达,但不抑制转化的βTC1细胞中的表达。这些结果提示存在一种控制机制,例如对GSF/IPF-1共激活因子的需求,在正常β细胞与转化的β细胞中,这种共激活因子的含量可能有限。