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细胞色素b5连接域的长度和序列在刺激细胞色素P450 2B4催化中的作用。

The role of the length and sequence of the linker domain of cytochrome b5 in stimulating cytochrome P450 2B4 catalysis.

作者信息

Clarke Thomas A, Im Sang-Choul, Bidwai Anil, Waskell Lucy

机构信息

Centre of Metalloprotein Spectroscopy and Biology, School of Biological Sciences, University of East Anglia, Norwich NR4 7TJ, United Kingdom.

出版信息

J Biol Chem. 2004 Aug 27;279(35):36809-18. doi: 10.1074/jbc.M406055200. Epub 2004 Jun 12.

Abstract

Cytochrome b(5) (cyt b(5)) is a 15-kDa amphipathic protein with a cytosolic amino-terminal catalytic heme domain, which is anchored to the microsomal membrane by a hydrophobic transmembrane alpha-helix at its carboxyl terminus. These two domains are connected by an approximately 15-amino acid linker domain, Ser(90)-Asp(104), which has been modified by site-directed mutagenesis to investigate whether the length or sequence of the linker influences the ability of cyt b(5) to bind ferric cytochrome P450 2B4 and donate an electron to oxyferrous (cyt P450 2B4), thereby stimulating catalysis. Because shortening the linker by 8 or more amino acids markedly inhibited the ability of cyt b(5) to bind cyt P450 2B4 and stimulate catalysis by this isozyme, it is postulated 7 amino acids are sufficient to allow a productive interaction. All mutant cyts b(5) except the protein lacking the entire 15-amino acid linker inserted normally into the microsomal membrane. Alternatively, lengthening the linker by 16 amino acids, reversing the sequence of the amino acids in the linker, and mutating conserved linker residues did not significantly alter the ability of cyt b(5) to interact with cyt P450 2B4. A model for the membrane-bound cyt b(5)-cyt P450 complex is presented.

摘要

细胞色素b(5)(细胞色素b(5))是一种15 kDa的两亲性蛋白质,其氨基末端催化血红素结构域位于胞质中,通过羧基末端的疏水跨膜α螺旋锚定在微粒体膜上。这两个结构域由一个约15个氨基酸的连接结构域(Ser(90)-Asp(104))相连,该连接结构域已通过定点诱变进行修饰,以研究连接结构域的长度或序列是否会影响细胞色素b(5)结合铁细胞色素P450 2B4并向亚铁(细胞色素P450 2B4)提供电子从而刺激催化作用的能力。由于将连接结构域缩短8个或更多氨基酸会显著抑制细胞色素b(5)结合细胞色素P450 2B4并刺激该同工酶催化作用的能力,因此推测7个氨基酸足以实现有效的相互作用。除了缺少整个15个氨基酸连接结构域的蛋白质外,所有突变型细胞色素b(5)都能正常插入微粒体膜。另外,将连接结构域延长16个氨基酸、颠倒连接结构域中氨基酸的序列以及突变连接结构域中的保守残基,均未显著改变细胞色素b(5)与细胞色素P450 2B4相互作用的能力。本文提出了一个膜结合的细胞色素b(5)-细胞色素P450复合物模型。

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