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亚单位对秀丽隐杆线虫左旋咪唑敏感型烟碱型乙酰胆碱受体功能的贡献。

Contribution of subunits to Caenorhabditis elegans levamisole-sensitive nicotinic receptor function.

机构信息

Instituto de Investigaciones Bioquímicas de Bahia Blanca, Universidad Nacional del Sur/Consejo Nacional de Investigaciones Científicas y Técnicas, Bahia Blanca, Argentina.

出版信息

Mol Pharmacol. 2012 Sep;82(3):550-60. doi: 10.1124/mol.112.079962. Epub 2012 Jun 25.

DOI:10.1124/mol.112.079962
PMID:22734069
Abstract

Caenorhabditis elegans muscle contains seven different nicotinic receptor (AChR) subunits, five of which have been shown to be components of adult levamisole-sensitive AChRs (L-AChRs). To elucidate the reason for such subunit diversity, we explore their functional roles in larva 1 (L1) muscle cells. Single-channel and macroscopic current recordings reveal that the α-type LEV-8 subunit is a component of native L1 L-AChRs but behaves as a nonessential subunit. It plays a key role in maintaining a low rate and extent of desensitization of L-AChRs. In the absence of the α-type ACR-8 subunit, L-AChR channel properties are not modified, thus indicating that ACR-8 is not a component of L1 L-AChRs. Together with our previous findings, this study reveals that L1 muscle cells express a main L-AChR type composed of five different subunits: UNC-38, UNC-63, UNC-29, LEV-1, and LEV-8. Analysis of a double lev-8; acr-8-null mutant, which shows an uncoordinated and levamisole-resistant phenotype, reveals that ACR-8 can replace LEV-8 in its absence, thus attributing a functional role to this subunit. Docking into homology modeled L-AChRs proposes that ACh forms the typical cation-π interaction, suggests why levamisole is less efficacious than ACh, and shows that ACR-8 can form activatable binding-sites, thus opening doors for elucidating subunit arrangement and anthelmintic selectivity.

摘要

秀丽隐杆线虫肌肉含有七种不同的烟碱型乙酰胆碱受体 (AChR) 亚基,其中五种已被证明是成人左旋咪唑敏感型 AChR (L-AChR) 的组成部分。为了阐明这种亚基多样性的原因,我们探索了它们在幼虫 1 (L1) 肌肉细胞中的功能作用。单通道和宏观电流记录表明,α型 LEV-8 亚基是天然 L1 L-AChR 的组成部分,但表现为非必需亚基。它在维持 L-AChR 的低脱敏率和程度方面起着关键作用。在缺乏 α 型 ACR-8 亚基的情况下,L-AChR 通道特性不会改变,因此表明 ACR-8 不是 L1 L-AChR 的组成部分。结合我们之前的发现,这项研究表明,L1 肌肉细胞表达一种由五种不同亚基组成的主要 L-AChR 类型:UNC-38、UNC-63、UNC-29、LEV-1 和 LEV-8。对双 lev-8; acr-8 缺失突变体的分析表明,在缺乏 LEV-8 的情况下,ACR-8 可以替代 LEV-8,从而赋予该亚基功能作用。对接到同源建模的 L-AChR 表明 ACh 形成典型的阳离子-π 相互作用,解释了为什么左旋咪唑不如 ACh 有效,并表明 ACR-8 可以形成可激活的结合位点,从而为阐明亚基排列和驱虫选择性开辟了道路。

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