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转化生长因子-β可增加正常大鼠肾成纤维细胞中编码表皮生长因子受体和纤连蛋白的基因转录。

Transforming growth factor-beta increases transcription of the genes encoding the epidermal growth factor receptor and fibronectin in normal rat kidney fibroblasts.

作者信息

Thompson K L, Assoian R, Rosner M R

机构信息

Department of Applied Biological Sciences, Massachusetts Institute of Technology, Cambridge 02139.

出版信息

J Biol Chem. 1988 Dec 25;263(36):19519-24.

PMID:3198640
Abstract

Transforming growth factor-beta (TGF-beta) is a potent modulator of cell growth in many systems. In normal rat kidney (NRK) fibroblasts, TGF-beta synergizes with epidermal growth factor (EGF) to stimulate growth in soft agar, a characteristic of the transformed phenotype. Many biochemical effects of TGF-beta occur at the cell surface. Increased binding of EGF and synthesis of extracellular matrix components such as fibronectin and collagen are primary responses of NRK cells to TGF-beta. Although specific membrane receptors for TGF-beta have been identified, the mechanism of action of this factor is not well understood. Here we demonstrate that TGF-beta enhances the expression of the EGF receptor in NRK cells through an increase in the level of EGF receptor gene transcripts. Analysis of nuclear run-off transcription levels and mRNA half-lives indicate that the elevation in EGF-receptor mRNA results from an increase in the rate of transcription. Dose-response and kinetic studies suggest that the EGF receptor response to TGF-beta is biphasic, possibly resulting from the action of multiple TGF-beta receptors. TGF-beta also elevates the levels of fibronectin and tubulin transcripts in NRK cells; however, the mechanism differs for each gene. The increase in fibronectin mRNA in response to TGF-beta results from an increased rate of gene transcription. Tubulin mRNA levels, in contrast, appear to be post-transcriptionally regulated. These results implicate TGF-beta as a transcriptional activator of the genes for both the EGF receptor and fibronectin and suggest the two genes may be regulated through a common pathway in this cell type.

摘要

转化生长因子-β(TGF-β)在许多系统中是细胞生长的有效调节剂。在正常大鼠肾(NRK)成纤维细胞中,TGF-β与表皮生长因子(EGF)协同作用,以刺激软琼脂中的生长,这是转化表型的一个特征。TGF-β的许多生化作用发生在细胞表面。EGF结合增加以及细胞外基质成分如纤连蛋白和胶原蛋白的合成是NRK细胞对TGF-β的主要反应。尽管已经鉴定出TGF-β的特异性膜受体,但该因子的作用机制尚未完全了解。在这里,我们证明TGF-β通过增加EGF受体基因转录本的水平来增强NRK细胞中EGF受体的表达。对核转录水平和mRNA半衰期的分析表明,EGF受体mRNA的升高是由于转录速率增加所致。剂量反应和动力学研究表明,EGF受体对TGF-β的反应是双相的,这可能是多种TGF-β受体作用的结果。TGF-β还可提高NRK细胞中纤连蛋白和微管蛋白转录本的水平;然而,每个基因的机制不同。TGF-β诱导的纤连蛋白mRNA增加是由于基因转录速率增加所致。相比之下,微管蛋白mRNA水平似乎受到转录后调控。这些结果表明TGF-β是EGF受体和纤连蛋白基因的转录激活因子,并提示这两个基因可能在这种细胞类型中通过共同途径进行调控。

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