来自大肠杆菌、枯草芽孢杆菌、噬菌体SP01和噬菌体T4的σ因子是同源蛋白。
Sigma factors from E. coli, B. subtilis, phage SP01, and phage T4 are homologous proteins.
作者信息
Gribskov M, Burgess R R
出版信息
Nucleic Acids Res. 1986 Aug 26;14(16):6745-63. doi: 10.1093/nar/14.16.6745.
Abstract
We show, using dot matrix comparisons and statistical analysis of sequence alignments, that seven sequenced sigma factors, E. coli sigma-70 and sigma-32, B. subtilis sigma-43 and sigma-29, phage SP01 gene products 28 and 34, and phage T4 gene product 55, comprise a homologous family of proteins. Sigma-70, sigma-32, and sigma-43 each have two copies of a sequence similar to the helix-turn-helix DNA binding motif seen in CRP, and lambda repressor and cro proteins. B. subtilis sigma-29, SP01 gp28, and SP01 gp34 have at least one copy similar to this sequence. We propose that a second sequence, conserved in all seven proteins is the core RNA polymerase binding site. A third region, present only in sigma-70 and sigma-43, may also be involved in interaction with core. Available mutational evidence supports our model for sigma factor structure.
摘要
我们通过点阵比较和序列比对的统计分析表明,七个已测序的σ因子,即大肠杆菌的σ-70和σ-32、枯草芽孢杆菌的σ-43和σ-29、噬菌体SP01的基因产物28和34以及噬菌体T4的基因产物55,构成了一个蛋白质同源家族。σ-70、σ-32和σ-43各自有两个与在CRP、λ阻遏蛋白和cro蛋白中所见的螺旋-转角-螺旋DNA结合基序相似的序列拷贝。枯草芽孢杆菌的σ-29、SP01 gp28和SP01 gp34至少有一个与该序列相似的拷贝。我们提出,在所有七种蛋白质中保守的第二个序列是核心RNA聚合酶结合位点。仅存在于σ-70和σ-43中的第三个区域也可能参与与核心的相互作用。现有的突变证据支持我们关于σ因子结构的模型。
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