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肠出血性埃希氏菌黏附素螺旋体长度与酶促方向性相关,并受到水杨醛酰肼的干扰。

Enterohaemorrhagic AdhE spirosome length correlates with enzymatic directionality and is perturbed by salicylidene acylhydrazides.

作者信息

Serrano Ester, Zhao Tianxiao, Mark David R, Soroor Mostafa, Floria Iris, Terrill Nicholas J, Kapur Nikil, Tyler Arwen I I, Horrocks Mathew H, Roe Andrew J, Byron Olwyn

机构信息

School of Infection and Immunity, University of Glasgow, Glasgow G12 8TA, UK.

EaStCHEM School of Chemistry, University of Edinburgh, Edinburgh EH9 3FJ, UK.

出版信息

Open Biol. 2025 Jun;15(6):250041. doi: 10.1098/rsob.250041. Epub 2025 Jun 18.

Abstract

Enterohaemorrhagic causes sporadic, and sometimes large-scale, food poisoning outbreaks, for which antibiotic treatment in humans is contraindicated. As an alternative form of therapy, previous studies developed the family of salicylidene acylhydrazide (SA) anti-virulence compounds. One target of the SA compounds is AdhE, an enzyme that converts acetyl-CoA to ethanol and vice versa. AdhE oligomerizes, forming helicoidal filaments, heterogeneous in length, called spirosomes. We show it is possible to only partially fractionate AdhE spirosomes because they oligomerize in the absence of stimuli, and that spirosome formation is necessary to regulate the direction of AdhE enzymatic reactions. We also show that the SA compound ME0054 binds and perturbs AdhE spirosomes, enhancing the conversion of ethanol to acetyl-CoA. This mechanistic understanding of how ME0054 impacts AdhE function will help in the development of SA compounds as novel anti-virulence inhibitors.

摘要

肠出血性大肠杆菌会引发散发性、有时是大规模的食物中毒疫情,人类使用抗生素治疗这类疫情是禁忌的。作为一种替代治疗形式,先前的研究开发了水杨醛酰肼(SA)抗毒力化合物家族。SA化合物的一个靶点是AdhE,一种将乙酰辅酶A转化为乙醇以及反之亦然的酶。AdhE会寡聚化,形成长度各异的螺旋状细丝,称为螺体。我们表明,仅对AdhE螺体进行部分分级分离是可能的,因为它们在没有刺激的情况下就会寡聚化,而且螺体形成对于调节AdhE酶促反应的方向是必要的。我们还表明,SA化合物ME0054会结合并扰乱AdhE螺体,增强乙醇向乙酰辅酶A的转化。这种对ME0054如何影响AdhE功能的机制性理解将有助于开发SA化合物作为新型抗毒力抑制剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2a69/12173503/8038d227a41a/rsob.250041.fg001.jpg

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