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胚胎成纤维细胞中的TAF4失活会激活TGFβ信号传导和自分泌生长。

TAF4 inactivation in embryonic fibroblasts activates TGF beta signalling and autocrine growth.

作者信息

Mengus Gabrielle, Fadloun Anas, Kobi Dominique, Thibault Christelle, Perletti Lucia, Michel Isabelle, Davidson Irwin

机构信息

Institut de Génétique et de Biologie Moléculaire et Cellulaire, CNRS/INSERM/ULP, Illkirch, France.

出版信息

EMBO J. 2005 Aug 3;24(15):2753-67. doi: 10.1038/sj.emboj.7600748. Epub 2005 Jul 14.

Abstract

We have inactivated transcription factor TFIID subunit TBP-associated factor 4 (TAF4) in mouse embryonic fibroblasts. Mutant taf4(-/-) cells are viable and contain intact TFIID comprising the related TAF4b showing that TAF4 is not an essential protein. TAF4 inactivation deregulates more than 1000 genes indicating that TFIID complexes containing TAF4 and TAF4b have distinct target gene specificities. However, taf4(-/-) cell lines have altered morphology and exhibit serum-independent autocrine growth correlated with the induced expression of several secreted mitotic factors and activators of the transforming growth factor beta signalling pathway. In addition to TAF4 inactivation, many of these genes can also be induced by overexpression of TAF4b. A competitive equilibrium between TAF4 and TAF4b therefore regulates expression of genes controlling cell proliferation. We have further identified a set of genes that are regulated both by TAF4 and upon adaptation to serum starvation and which may be important downstream mediators of serum-independent growth. Our study also shows that TAF4 is an essential cofactor for activation by the retinoic acid receptor and CREB, but not for Sp1 and the vitamin D3 receptor.

摘要

我们已在小鼠胚胎成纤维细胞中使转录因子TFIID亚基TBP相关因子4(TAF4)失活。突变的taf4(-/-)细胞能够存活,并且含有完整的TFIID,其中包含相关的TAF4b,这表明TAF4不是必需蛋白。TAF4失活会使1000多个基因失调,这表明含有TAF4和TAF4b的TFIID复合物具有不同的靶基因特异性。然而,taf4(-/-)细胞系形态发生改变,并表现出与几种分泌的有丝分裂因子和转化生长因子β信号通路激活剂的诱导表达相关的血清非依赖性自分泌生长。除了TAF4失活外,许多这些基因也可由TAF4b的过表达诱导。因此,TAF4和TAF4b之间的竞争性平衡调节控制细胞增殖的基因表达。我们进一步鉴定了一组基因,它们既受TAF4调节,又在适应血清饥饿时受到调节,并且可能是血清非依赖性生长的重要下游介质。我们的研究还表明,TAF4是视黄酸受体和CREB激活所必需的辅助因子,但不是Sp1和维生素D3受体激活所必需的。

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