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原癌基因jun家族的不同成员在对β型转化生长因子的反应中表现出不同的表达模式。

Different members of the jun proto-oncogene family exhibit distinct patterns of expression in response to type beta transforming growth factor.

作者信息

Li L, Hu J S, Olson E N

机构信息

Department of Biochemistry and Molecular Biology, University of Texas M. D. Anderson Cancer Center, Houston 77030.

出版信息

J Biol Chem. 1990 Jan 25;265(3):1556-62.

PMID:2104845
Abstract

Type beta transforming growth factor (TGF-beta) is a multifunctional regulator of cell growth and differentiation. In the BC3H1 muscle cell line, TGF-beta blocks the onset of differentiation when added to undifferentiated myoblasts and causes dedifferentiation when added to fully differentiated myocytes. The goal of the present study was to determine whether TGF-beta-dependent repression of muscle-specific genes was preceded by modulation in expression of members of the jun proto-oncogene family, which function as growth factor-inducible transcription factors. junB mRNA was expressed at a basal level in differentiated BC3H1 myocytes. Within 15 min following exposure of myocytes to TGF-beta, junB mRNA began to accumulate; a peak of expression 20-fold above basal levels was observed after 2 h with a gradual decline thereafter. Nuclear run-on transcription assays showed that induction of junB by TGF-beta occurred at the level of transcription through a mechanism independent of protein synthesis. junB was also induced by 20% fetal bovine serum, platelet-derived growth factor, and insulin, but the maximal level of expression in response to these growth factors was lower and less sustained than in the presence of TGF-beta. In contrast to the dramatic effects of TGF-beta on junB expression, c-jun showed only a 2.5-fold increase in expression in response to TGF-beta. In an effort to identify additional members of the jun family which might be regulated by TGF-beta, a cDNA library was prepared from the poly(A)+ mRNA of TGF-beta-stimulated BC3H1 myocytes and was screened under conditions of reduced stringency with a v-jun DNA probe. From this screen, a new jun-related gene product was identified which shared a high degree of homology with regions of c-jun and junB which have been implicated in transcriptional activation, dimerization, and DNA binding. The transcript for this jun-related gene was expressed constitutively in BC3H1 cells and was not regulated by TGF-beta. Three members of the jun family thus exhibit distinct responses to TGF-beta in BC3H1 cells. The rapid transcriptional induction of junB is among the earliest and most dramatic responses to TGF-beta yet described and suggests that junB may mediate certain of the diverse biological effects of this growth factor.

摘要

β型转化生长因子(TGF-β)是细胞生长和分化的多功能调节因子。在BC3H1肌肉细胞系中,将TGF-β添加到未分化的成肌细胞中时会阻断分化的起始,而添加到完全分化的肌细胞中时会导致去分化。本研究的目的是确定在TGF-β依赖性抑制肌肉特异性基因之前,原癌基因jun家族成员的表达是否发生了调节,该家族成员作为生长因子诱导型转录因子发挥作用。junB mRNA在分化的BC3H1肌细胞中以基础水平表达。在肌细胞暴露于TGF-β后的15分钟内,junB mRNA开始积累;2小时后观察到表达峰值比基础水平高20倍,此后逐渐下降。核转录分析表明,TGF-β对junB的诱导发生在转录水平,其机制独立于蛋白质合成。junB也可被20%胎牛血清、血小板衍生生长因子和胰岛素诱导,但对这些生长因子的最大表达水平低于TGF-β存在时,且维持时间较短。与TGF-β对junB表达的显著影响相反,c-jun对TGF-β的反应仅表现为表达增加2.5倍。为了鉴定可能受TGF-β调节的jun家族其他成员,从TGF-β刺激的BC3H1肌细胞的聚腺苷酸加尾mRNA制备了cDNA文库,并用v-jun DNA探针在低严谨度条件下进行筛选。从该筛选中,鉴定出一种新的jun相关基因产物,它与c-jun和junB中与转录激活、二聚化和DNA结合相关的区域具有高度同源性。该jun相关基因的转录本在BC3H1细胞中组成性表达,不受TGF-β调节。因此,jun家族的三个成员在BC3H1细胞中对TGF-β表现出不同的反应。junB的快速转录诱导是对TGF-β最早且最显著的反应之一,这表明junB可能介导了这种生长因子的某些多样的生物学效应。

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