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Inactive dimeric structure of the protease domain of stomatin operon partner protein

机译:蛋白酶活性的二聚的结构域stomatin操纵子的伴侣蛋白质

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摘要

The N-terminal region of the stomatin operon partner protein (STOPP) PH1510 (1510-N) from the hyperthermophilic archaeon Pyrococcus horikoshii is a serine protease with a catalytic Ser-Lys dyad (Ser97 and Lysl38) and specifically cleaves the C-terminal hydrophobic region of the p-stomatin PH1511. In a form of human hemolytic anemia known as hereditary stomatocytosis, stomatin is deficient in the erythrocyte membrane owing to mis-trafficking. Stomatin is thought to act as an oligomeric scaffolding protein to support cell membranes. The cleavage of stomatin by STOPP might be involved in a regulatory system. Several crystal structures of 1510-N have previously been determined: the wild type, the K138A mutant and its complex with a substrate peptide. Here, the crystal structure of the S97A mutant of 1510-N (1510-N S97A) was determined at 2.25 A resolution. The structure contained two 1510-N S97A molecules in the asymmetric unit. On the superposition of one monomer of the 1510-N S97A and wild-type dimers, the S97A C atom of the other monomer of 1510-N S97A deviated by 23 A from that of the wild type. This result indicates that 1510-N can greatly change the form of its dimer. Because of crystallographic symmetry in space group P6_5, a sixfold helical structure is constructed using the 1510-N dimer as a basic unit. This helical structure may be common to STOPP structures.
机译:氨基stomatin操纵子的区域伴侣蛋白(阻止)PH1510 (1510 - n)hyperthermophilic archaeon海床horikoshii是一种丝氨酸蛋白酶催化Ser-Lys双(Ser97和Lysl38)特别是劈开c端疏水区域p-stomatin PH1511。贫血称为遗传stomatocytosis,红细胞膜stomatin不足由于mis-trafficking。作为一个低聚物的支架蛋白细胞膜的支持。通过阻止可能参与监管系统。此前决定:野生型的K138A突变体及其复杂的基质肽。突变体1510 - n (1510 - n S97A)决定2.25一项决议。1510 - n S97A分子不对称单位。一个单体的叠加1510 - nS97A和野生型二聚体,S97A C原子的其他单体通过23 1510 - n S97A相同从野生型的。1510 - n可以极大地改变它的形式二聚体。螺旋结构空间群P6_5, 6倍构造使用1510 - n二聚体作为基础单位。阻止结构。

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