Characterization of adjacent charged residues near the agonist binding site of the nematode UNC-49 GABA receptor

IF 1.4 4区 医学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY Molecular and biochemical parasitology Pub Date : 2022-11-01 DOI:10.1016/j.molbiopara.2022.111521
Everett Cochrane, Joshua Foster, Mohammad Hassan Khatami, Hendrick W. de Haan, Sean G. Forrester
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引用次数: 1

Abstract

The UNC-49 receptor is a Cys-loop GABA receptor that is unique to the nematode phylum. The receptor differs from mammalian GABA receptors both in amino acid sequence and pharmacology which highlights its potential as a novel anthelmintic target. Sequence differences within and near the various ligand-binding loops of the nematode receptor suggest that there could be structural differences compared to mammalian receptors that result in different pharmacological and functional features. Here we investigated three residues in the UNC-49 receptor from the parasitic nematode Haemonchus contortus: K181, E183, and T230. Analysis of these residues was conducted via site-directed mutagenesis, electrophysiology, MD simulations, and mutant cycling analysis. In the UNC-49 receptor, E183 lies in close proximity to K181 where together they appear to play a role in GABA sensitivity and pharmacology, possibly interacting via an ionic bond. While the introduction of single alanine residues at each position separately had a negative impact on GABA EC50, the double alanine mutant (K181A/E183A) exhibited wildtype-level GABA EC50 and some differences in pharmacology. Overall, this study has revealed a potentially novel role for these two residues in nematode UNC-49 GABA receptors that could aid in understanding their function.

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线虫UNC-49 GABA受体激动剂结合位点附近带电残基的表征
UNC-49受体是一种Cys-loop GABA受体,是线虫门特有的。该受体与哺乳动物GABA受体在氨基酸序列和药理学上都不同,这突出了它作为一种新的驱虫药靶点的潜力。线虫受体的各种配体结合环内部和附近的序列差异表明,与哺乳动物受体相比,线虫受体可能存在结构差异,从而导致不同的药理学和功能特征。本文研究了弯曲血蜱(Haemonchus contortus)寄生线虫UNC-49受体的三个残基:K181、E183和T230。这些残基的分析是通过位点定向诱变、电生理学、MD模拟和突变循环分析进行的。在UNC-49受体中,E183靠近K181,它们似乎在GABA敏感性和药理学中发挥作用,可能通过离子键相互作用。在每个位置分别引入单个丙氨酸残基对GABA EC50有负面影响,而双丙氨酸突变体(K181A/E183A)表现出野生型水平的GABA EC50,并且在药理学上存在一定差异。总的来说,这项研究揭示了这两个残基在线虫UNC-49 GABA受体中的潜在新作用,可以帮助理解它们的功能。
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来源期刊
CiteScore
2.90
自引率
0.00%
发文量
51
审稿时长
63 days
期刊介绍: The journal provides a medium for rapid publication of investigations of the molecular biology and biochemistry of parasitic protozoa and helminths and their interactions with both the definitive and intermediate host. The main subject areas covered are: • the structure, biosynthesis, degradation, properties and function of DNA, RNA, proteins, lipids, carbohydrates and small molecular-weight substances • intermediary metabolism and bioenergetics • drug target characterization and the mode of action of antiparasitic drugs • molecular and biochemical aspects of membrane structure and function • host-parasite relationships that focus on the parasite, particularly as related to specific parasite molecules. • analysis of genes and genome structure, function and expression • analysis of variation in parasite populations relevant to genetic exchange, pathogenesis, drug and vaccine target characterization, and drug resistance. • parasite protein trafficking, organelle biogenesis, and cellular structure especially with reference to the roles of specific molecules • parasite programmed cell death, development, and cell division at the molecular level.
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