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人TFIIB在体外和体内转录起始位点选择中的作用。

The role of human TFIIB in transcription start site selection in vitro and in vivo.

作者信息

Hawkes N A, Roberts S G

机构信息

Division of Gene Expression, Department of Biochemistry, Wellcome Trust Building, University of Dundee, Dundee DD1 5EH, United Kingdom.

出版信息

J Biol Chem. 1999 May 14;274(20):14337-43. doi: 10.1074/jbc.274.20.14337.

Abstract

The general transcription factor TFIIB plays a crucial role in selecting the transcription initiation site in yeast. We have analyzed the human homologs of TFIIB mutants that have previously been shown to affect transcription start site selection in the yeast Saccharomyces cerevisiae. Despite the distinct mechanisms of transcription start site selection observed in S. cerevisiae and humans, the role of TFIIB in this process is similar. However, unlike their yeast counterparts, the human mutants do not show a severe defect in supporting either basal transcription or transcription stimulated by an acidic activator in vitro. Transient transfection analysis revealed that, in addition to a role in transcription start site selection, human TFIIB residue Arg-66 performs a critical function in vivo that is bypassed in vitro. Furthermore, although correct transcription start site selection is dependent upon an arginine residue at position 66 in human TFIIB, innate function in vivo is determined by the charge of the residue alone. Our observations raise questions as to the evolutionary conservation of TFIIB and uncover an additional function for TFIIB that is required in vivo but can be bypassed in vitro.

摘要

通用转录因子TFIIB在酵母中选择转录起始位点的过程中起着关键作用。我们分析了TFIIB突变体的人类同源物,这些突变体先前已被证明会影响酿酒酵母中的转录起始位点选择。尽管在酿酒酵母和人类中观察到转录起始位点选择的机制不同,但TFIIB在此过程中的作用是相似的。然而,与它们的酵母对应物不同,人类突变体在体外支持基础转录或酸性激活剂刺激的转录方面没有表现出严重缺陷。瞬时转染分析表明,除了在转录起始位点选择中的作用外,人类TFIIB残基Arg-66在体内执行一项关键功能,而在体外该功能可被绕过。此外,虽然正确的转录起始位点选择依赖于人类TFIIB中第66位的精氨酸残基,但体内的固有功能仅由该残基的电荷决定。我们的观察结果引发了关于TFIIB进化保守性的问题,并揭示了TFIIB在体内需要但在体外可被绕过的一项额外功能。

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