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利用分子动力学构象系综对α-甘露糖苷贮积症中错义突变的新见解。

A new view of missense mutations in α-mannosidosis using molecular dynamics conformational ensembles.

作者信息

Mandl Špela, Di Geronimo Bruno, Alonso-Gil Santiago, Grininger Christoph, George Gibu, Ferstl Ulrika, Herzog Sereina Annik, Žagrović Bojan, Nusshold Christoph, Pavkov-Keller Tea, Sánchez-Murcia Pedro A

机构信息

Laboratory of Computer-Aided Molecular Design, Division of Medicinal Chemistry, Otto-Loewi Research Center, Medical University of Graz, Graz, Austria.

Max Perutz Labs, Vienna Biocenter Campus (VBC), Vienna, Austria.

出版信息

Protein Sci. 2025 Apr;34(4):e70080. doi: 10.1002/pro.70080.

Abstract

The mutation of remote positions on enzyme scaffolds and how these residue changes can affect enzyme catalysis is still far from being fully understood. One paradigmatic example is the group of lysosomal storage disorders, where the enzyme activity of a lysosomal enzyme is abolished or severely reduced. In this work, we analyze molecular dynamics simulation conformational ensembles to unveil the molecular features controlling the deleterious effects of the 43 reported missense mutations in the human lysosomal α-mannosidase. Using residue descriptors for protein dynamics, their coupling with the active site, and their impact on protein stability, we have assigned the contribution of each of the missense mutations into protein stability, protein dynamics, and their connectivity with the active site. We demonstrate here that the use of conformational ensembles is a powerful approach not only to better understand missense mutations at the molecular level but also to revisit the missense mutations reported in lysosomal storage disorders in order to aid the treatment of these diseases.

摘要

酶支架上远端位置的突变以及这些残基变化如何影响酶催化作用,目前仍远未得到充分理解。一个典型的例子是溶酶体贮积症群体,其中溶酶体酶的酶活性被消除或严重降低。在这项工作中,我们分析分子动力学模拟构象集合,以揭示控制人类溶酶体α-甘露糖苷酶中43个已报道错义突变的有害影响的分子特征。利用蛋白质动力学的残基描述符、它们与活性位点的耦合以及它们对蛋白质稳定性的影响,我们确定了每个错义突变对蛋白质稳定性、蛋白质动力学及其与活性位点连通性的贡献。我们在此证明,使用构象集合不仅是一种强大的方法,可在分子水平上更好地理解错义突变,而且还可重新审视溶酶体贮积症中报道的错义突变,以辅助这些疾病的治疗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/288e/11931667/65588d27dd73/PRO-34-e70080-g006.jpg

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