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参与稳定期代谢的四种大肠杆菌酶的X射线溶液散射研究。

X-Ray Solution Scattering Study of Four Escherichia coli Enzymes Involved in Stationary-Phase Metabolism.

作者信息

Dadinova Liubov A, Shtykova Eleonora V, Konarev Petr V, Rodina Elena V, Snalina Natalia E, Vorobyeva Natalia N, Kurilova Svetlana A, Nazarova Tatyana I, Jeffries Cy M, Svergun Dmitri I

机构信息

A.V. Shubnikov Institute of Crystallography of Federal Scientific Research Centre "Crystallography and Photonics" of Russian Academy of Sciences, Moscow, Russia.

M.V. Lomonosov Moscow State University, Physics Department, Moscow, Russia.

出版信息

PLoS One. 2016 May 26;11(5):e0156105. doi: 10.1371/journal.pone.0156105. eCollection 2016.

Abstract

The structural analyses of four metabolic enzymes that maintain and regulate the stationary growth phase of Escherichia coli have been performed primarily drawing on the results obtained from solution small angle X-ray scattering (SAXS) and other structural techniques. The proteins are (i) class I fructose-1,6-bisphosphate aldolase (FbaB); (ii) inorganic pyrophosphatase (PPase); (iii) 5-keto-4-deoxyuronate isomerase (KduI); and (iv) glutamate decarboxylase (GadA). The enzyme FbaB, that until now had an unknown structure, is predicted to fold into a TIM-barrel motif that form globular protomers which SAXS experiments show associate into decameric assemblies. In agreement with previously reported crystal structures, PPase forms hexamers in solution that are similar to the previously reported X-ray crystal structure. Both KduI and GadA that are responsible for carbohydrate (pectin) metabolism and acid stress responses, respectively, form polydisperse mixtures consisting of different oligomeric states. Overall the SAXS experiments yield additional insights into shape and organization of these metabolic enzymes and further demonstrate the utility of hybrid methods, i.e., solution SAXS combined with X-ray crystallography, bioinformatics and predictive 3D-structural modeling, as tools to enrich structural studies. The results highlight the structural complexity that the protein components of metabolic networks may adopt which cannot be fully captured using individual structural biology techniques.

摘要

主要借助溶液小角X射线散射(SAXS)及其他结构技术所获结果,对维持和调节大肠杆菌稳定生长期的四种代谢酶进行了结构分析。这些蛋白质分别是:(i)I类果糖-1,6-二磷酸醛缩酶(FbaB);(ii)无机焦磷酸酶(PPase);(iii)5-酮-4-脱氧尿苷酸异构酶(KduI);以及(iv)谷氨酸脱羧酶(GadA)。此前结构未知的FbaB酶预计会折叠成TIM桶基序,形成球状原体,SAXS实验表明这些原体可组装成十聚体。与先前报道的晶体结构一致,PPase在溶液中形成六聚体,与先前报道的X射线晶体结构相似。分别负责碳水化合物(果胶)代谢和酸应激反应的KduI和GadA均形成由不同寡聚状态组成的多分散混合物。总体而言,SAXS实验为这些代谢酶的形状和组织提供了更多见解,并进一步证明了混合方法的实用性,即溶液SAXS与X射线晶体学、生物信息学和预测性三维结构建模相结合,作为丰富结构研究的工具。结果突出了代谢网络蛋白质成分可能具有的结构复杂性,而使用单一结构生物学技术无法完全捕捉到这些复杂性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b9a0/4881948/6db64b96f692/pone.0156105.g001.jpg

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