与电鳐烟碱型乙酰胆碱受体上的γ-酪氨酸-111和突变型δ-酪氨酸-113近距离相互作用的α-芋螺毒素残基。

Alpha-conotoxin residues that interact at close range with gamma-tyrosine-111 and mutant delta-tyrosine-113 on the Torpedo nicotinic acetylcholine receptor.

作者信息

Vélez-Carrasco Wanda, Valdés Sonia, Agresar Lyann, Lettich Alyssa, Guerra Astrid Y, Hann Richard M

机构信息

Department of Biochemistry and Center for Molecular and Behavioral Neuroscience, Universidad Central del Caribe, Bayamón, Puerto Rico 00960.

出版信息

Biochemistry. 2004 Oct 5;43(39):12700-8. doi: 10.1021/bi030248b.

DOI:10.1021/bi030248b

PMID:15449960

Abstract

The alpha-conotoxins MI and GI display stronger affinities for the alphagamma agonist site on the Torpedo californica electrocyte nicotinic acetylcholine receptor (ACHR) than for the alphadelta agonist site, while alpha-conotoxin SI binds with the same affinity to both sites. Prior studies reported that the arginine at position 9 on GI and the tyrosine at position 111 on the receptor gamma subunit were responsible for the stronger alphagamma affinities of GI and MI, respectively. This study was undertaken to determine if the alpha-conotoxin midchain cationic residues interact with Torpedo gammaY111. The findings show that lysine 10 on MI is responsible for the alphagamma selectivity of MI and confirm the previously reported importance of R9 on GI and on the SI analogue, SIP9R. The results also show that gammaY111 contributes substantially to the selective alphagamma high affinity of all three peptides. Double-mutant cycle analyses reveal that, in the alphagamma site, K10 on MI and R9 on SIP9R interact with the aromatic ring of gammaY111 to stabilize the high-affinity complex, while in contrast, R9 on GI does not. The substitution of Y for R at position 113 on the delta subunit converts the alphadelta site into a high-affinity site for MI, GI, and SIP9R through the interacting of deltaY113 with K10 on MI and with R9 on both GI and SIP9R. The overall data show that the residues in the two sites with which MI interacts, other than at gamma111/delta113, are either the same or similar enough to exert equivalent effects on MI, indicating that MI binds in the same orientation at the alphagamma and alphadelta sites. Similar findings show that SIP9R probably also binds in the same orientation at the wild-type alphagamma and alphadelta sites. The finding that R9 on GI interacts closely with deltaR113Y but not with gammaY111 means that GI binds in different orientations at the alphagamma and alphadelta sites. This report also discusses the molecular basis of the difference in the MI high-affinity sites on Torpedo and embryonic mouse muscle ACHRs.

摘要

α-芋螺毒素MI和GI对加州电鳐电细胞烟碱型乙酰胆碱受体（ACHR）上的αγ激动剂位点的亲和力比对αδ激动剂位点的亲和力更强，而α-芋螺毒素SI对这两个位点的结合亲和力相同。先前的研究报道，GI上第9位的精氨酸和受体γ亚基上第111位的酪氨酸分别是GI和MI具有更强的αγ亲和力的原因。本研究旨在确定α-芋螺毒素中链阳离子残基是否与电鳐γY111相互作用。研究结果表明，MI上的赖氨酸10是MI具有αγ选择性的原因，并证实了先前报道的GI上R9以及SI类似物SIP9R上R9的重要性。结果还表明，γY111对所有三种肽的选择性αγ高亲和力有很大贡献。双突变循环分析表明，在αγ位点，MI上的K10和SIP9R上的R9与γY111的芳香环相互作用以稳定高亲和力复合物，而相比之下，GI上的R9则不然。δ亚基上第113位的酪氨酸取代精氨酸，通过δY113与MI上的K10以及GI和SIP9R上的R9相互作用，将αδ位点转变为MI、GI和SIP9R的高亲和力位点。总体数据表明，MI相互作用的两个位点中除γ111/δ113之外的残基要么相同，要么相似到足以对MI产生等效作用，这表明MI在αγ和αδ位点以相同方向结合。类似的研究结果表明，SIP9R可能也以相同方向结合在野生型αγ和αδ位点。GI上的R9与δR113Y紧密相互作用但不与γY111相互作用这一发现意味着GI在αγ和αδ位点以不同方向结合。本报告还讨论了电鳐和胚胎小鼠肌肉ACHR上MI高亲和力位点差异的分子基础。