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脂肪酶A热稳定突变体的复杂网络分析

Complex network analysis of thermostable mutants of Lipase A.

作者信息

Kandhari Nitika, Sinha Somdatta

机构信息

Centre for Protein Science Design and Engineering, Department of Biological Sciences, Indian Institute of Science Education and Research, Mohali, Punjab 140306 India.

出版信息

Appl Netw Sci. 2017;2(1):18. doi: 10.1007/s41109-017-0039-y. Epub 2017 Jun 26.

Abstract

Three-dimensional structures of proteins that regulate their functions can be modelled using complex network based approaches for understanding the structure-function relationship. The six mutants of the protein Lipase A from , harbouring 2 to 12 mutations, retain their function at higher temperatures with negligible variation in their overall three-dimensional crystallographic structures. This enhanced thermostability of the mutants questions the structure-function paradigm. In this paper, a coarse-grained complex network approach is used to elucidate the structural basis of enhanced thermostability in the mutant proteins, by uncovering small but significant local changes distributed throughout the structure, rendering stability to the mutants at higher temperatures. Community structure analysis of the six mutant protein networks uncovers the specific reorganisations among the nodes/residues that occur, in absence of overall structural variations, which induce enhanced rigidity underlying the increased thermostability. This study offers a novel and significant application of complex network analysis that proposes to be useful in the understanding and designing of thermostable proteins.

摘要

可以使用基于复杂网络的方法对调节蛋白质功能的三维结构进行建模,以理解其结构-功能关系。来自[具体来源未给出]的脂肪酶A蛋白的六个突变体,含有2至12个突变,在较高温度下仍保留其功能,其整体三维晶体结构的变化可忽略不计。这些突变体增强的热稳定性对结构-功能范式提出了质疑。在本文中,通过揭示分布在整个结构中的微小但显著的局部变化,从而使突变体在较高温度下具有稳定性,采用粗粒度复杂网络方法来阐明突变蛋白中热稳定性增强的结构基础。对六个突变蛋白网络的群落结构分析揭示了在没有整体结构变化的情况下节点/残基之间发生的特定重组,这些重组导致了热稳定性增加背后的刚性增强。这项研究提供了复杂网络分析的一种新颖且重要的应用,该应用有望在热稳定蛋白质的理解和设计中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a00f/6214246/b5d2d17a822f/41109_2017_39_Fig1_HTML.jpg

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