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酵母线粒体型焦磷酸酶的晶体结构为研究其人类同源物的病理性突变提供了模型。

The crystal structure of yeast mitochondrial type pyrophosphatase provides a model to study pathological mutations in its human ortholog.

机构信息

Lomonosov Moscow State University, Chemistry Department, 119991, Moscow, Russia.

A.N. Bach Institute of Biochemistry, Federal Research Centre of Biotechnology of the Russian Academy of Sciences, 119071, Moscow, Russia; Landau Phystech School of Physics and Research, Moscow Institute of Physics and Technology, Institutsky Lane, 9, Dolgoprudny, 141700, Moscow, Russia.

出版信息

Biochem Biophys Res Commun. 2024 Dec 17;738:150563. doi: 10.1016/j.bbrc.2024.150563. Epub 2024 Aug 17.

DOI:10.1016/j.bbrc.2024.150563
PMID:39178581
Abstract

Mutations in human ppa2 gene encoding mitochondrial inorganic pyrophosphatase (PPA2) result in the mitochondria malfunction in heart and brain and lead to early death. In comparison with its cytosolic counterpart, PPA2 of any species is a poorly characterized enzyme with a previously unknown 3D structure. We report here the crystal structure of PPA2 from yeast Ogataea parapolymorpha (OpPPA2), as well as its biochemical characterization. OpPPA2 is a dimer, demonstrating the fold typical for other eukaryotic Family I pyrophosphatases, including the human cytosolic enzyme. Cofactor Mg ions found in OpPPA2 structure have similar coordination to most known Family I pyrophosphatases. Most of the residues associated with the pathological mutations in human PPA2 are conserved in OpPPA2, and their structural context suggests possible explanations for the effects of the mutations on the human enzyme. In this work, the mutant variant of OpPPA2, Met52Val, corresponding to the natural pathogenic variant Met94Val of human PPA2, is characterized. The obtained structural and biochemical data provide a step to understanding the structural basis of PPA2-associated pathologies.

摘要

人类 ppa2 基因编码的线粒体无机焦磷酸酶(PPA2)突变导致心脏和大脑中的线粒体功能障碍,并导致早逝。与细胞质同工酶相比,任何物种的 PPA2 都是一种特征研究不足的酶,其三维结构以前未知。我们在此报告来自酵母 Ogataea parapolymorpha(OpPPA2)的 PPA2 的晶体结构及其生化特性。OpPPA2 是二聚体,表现出与其他真核细胞 I 族焦磷酸酶典型的折叠,包括人类细胞质酶。在 OpPPA2 结构中发现的辅助因子 Mg 离子与大多数已知的 I 族焦磷酸酶具有相似的配位。与人类 PPA2 中与病理突变相关的大多数残基在 OpPPA2 中保守,其结构背景表明突变对人类酶的影响的可能解释。在这项工作中,表征了与天然致病性人类 PPA2 的 Met94Val 对应的 OpPPA2 的突变变体 Met52Val。获得的结构和生化数据为理解 PPA2 相关病理学的结构基础提供了一个步骤。

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