α-芋螺毒素Arenatus IB[V11L,V16D](已修正)是大鼠和人天然α7烟碱型乙酰胆碱受体的强效选择性拮抗剂。
Alpha-conotoxin Arenatus IB[V11L,V16D] [corrected] is a potent and selective antagonist at rat and human native alpha7 nicotinic acetylcholine receptors.
作者信息
Innocent Neal, Livingstone Phil D, Hone Arik, Kimura Atsuko, Young Tracey, Whiteaker Paul, McIntosh J Michael, Wonnacott Susan
机构信息
Department of Biology and Biochemistry, University of Bath, Bath BA27AY, UK.
出版信息
J Pharmacol Exp Ther. 2008 Nov;327(2):529-37. doi: 10.1124/jpet.108.142943. Epub 2008 Jul 29.
A recently developed alpha-conotoxin, alpha-conotoxin Arenatus IB-[V11L,V16D] (alpha-CtxArIB[V11L,V16D]) [corrected], is a potent and selective competitive antagonist at rat recombinant alpha7 nicotinic acetylcholine receptors (nAChRs), making it an attractive probe for this receptor subtype. alpha7 nAChRs are potential therapeutic targets that are widely expressed in both neuronal and non-neuronal tissues, where they are implicated in a variety of functions. In this study, we evaluate this toxin at rat and human native nAChRs. Functional alpha7 nAChR responses were evoked by choline plus the allosteric potentiator PNU-120596 [1-(5-chloro-2,4-dimethoxy-phenyl)-3-(5-methyl-isoxazol-3-yl)-urea] in rat PC12 cells and human SH-SY5Y cells loaded with calcium indicators. alpha-CtxArIB[V11L,V16D] specifically inhibited alpha7 nAChR-mediated increases in Ca2+ in PC12 cells. Responses to other stimuli, 5-I-A-85380 [5-iodo-3-(2(S)-azetidinylmethoxy)pyridine dihydrochloride], nicotine, or KCl, that did not activate alpha7 nAChRs were unaffected. Human alpha7 nAChRs were also sensitive to alpha-CtxArIB[V11L, V16D]; acetylcholine-evoked currents in Xenopus laevis oocytes expressing human alpha7 nAChRs were inhibited by alpha-CtxArIB[V11L,V16D] (IC(50), 3.4 nM) in a slowly reversible manner, with full recovery taking 15 min. This is consistent with the time course of recovery from blockade of rat alpha7 nAChRs in PC12 cells. alpha-CtxArIB[V11L,V16D] inhibited human native alpha7 nAChRs in SHSY5Y cells, activated by either choline or AR-R17779 [(2)-spiro[1-azabicyclo[2.2.2]octane-3,59-oxazolidin]-29-one] plus PNU-120596. Rat brain alpha7 nAChRs contribute to dopamine release from striatal minces; alpha-CtxArIB[V11L,V16D] (300 nM) selectively inhibited choline-evoked dopamine release without affecting responses evoked by nicotine that activates heteromeric nAChRs. This study establishes that alpha-CtxArIB[V11L,V16D] selectively inhibits human and rat native alpha7 nAChRs with comparable potency, making this a potentially useful antagonist for investigating alpha7 nAChR functions.
一种最近研发的α-芋螺毒素,α-芋螺毒素Arenatus IB-[V11L,V16D](α-CtxArIB[V11L,V16D])[已修正],是大鼠重组α7烟碱型乙酰胆碱受体(nAChRs)的一种强效且选择性的竞争性拮抗剂,使其成为该受体亚型颇具吸引力的研究探针。α7 nAChRs是潜在的治疗靶点,在神经元和非神经元组织中均广泛表达,参与多种功能。在本研究中,我们在大鼠和人类天然nAChRs上评估了这种毒素。在加载了钙指示剂的大鼠PC12细胞和人类SH-SY5Y细胞中,胆碱加变构增强剂PNU-120596 [1-(5-氯-2,4-二甲氧基苯基)-3-(5-甲基异恶唑-3-基)-脲]可诱发功能性α7 nAChR反应。α-CtxArIB[V11L,V16D]特异性抑制PC12细胞中α7 nAChR介导的Ca2+增加。对其他未激活α7 nAChRs的刺激,如5-I-A-85380 [5-碘-3-(2(S)-氮杂环丁烷甲氧基)吡啶二盐酸盐]、尼古丁或KCl的反应未受影响。人类α7 nAChRs对α-CtxArIB[V11L, V16D]也敏感;表达人类α7 nAChRs的非洲爪蟾卵母细胞中,乙酰胆碱诱发的电流被α-CtxArIB[V11L,V16D](IC(50),3.4 nM)以缓慢可逆的方式抑制,完全恢复需15分钟。这与PC12细胞中大鼠α7 nAChRs阻断后的恢复时间进程一致。α-CtxArIB[V11L,V16D]抑制了SHSY5Y细胞中由胆碱或AR-R17779 [(2)-螺[1-氮杂双环[2.2.2]辛烷-3,59-恶唑烷]-29-酮]加PNU-120596激活的人类天然α7 nAChRs。大鼠脑α7 nAChRs参与纹状体匀浆中多巴胺的释放;α-CtxArIB[V11L,V16D](300 nM)选择性抑制胆碱诱发的多巴胺释放,而不影响由激活异聚体nAChRs的尼古丁诱发的反应。本研究证实α-CtxArIB[V11L,V16D]以相当的效力选择性抑制人类和大鼠天然α7 nAChRs,使其成为研究α7 nAChR功能的潜在有用拮抗剂。
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