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CSTX-1是一种来自狩猎蜘蛛巴西游走蛛毒液的毒素,它是哺乳动物神经元中L型钙通道的选择性阻滞剂。

CSTX-1, a toxin from the venom of the hunting spider Cupiennius salei, is a selective blocker of L-type calcium channels in mammalian neurons.

作者信息

Kubista Helmut, Mafra Roberta A, Chong Youmie, Nicholson Graham M, Beirão Paulo S L, Cruz Jader S, Boehm Stefan, Nentwig Wolfgang, Kuhn-Nentwig Lucia

机构信息

Center for Biomolecular Medicine and Pharmacology, Institute of Pharmacology, Medical University of Vienna, Waehringerstrasse 13a, A-1090 Vienna, Austria.

出版信息

Neuropharmacology. 2007 Jun;52(8):1650-62. doi: 10.1016/j.neuropharm.2007.03.012. Epub 2007 Apr 4.

Abstract

The inhibitor cystine-knot motif identified in the structure of CSTX-1 from Cupiennius salei venom suggests that this toxin may act as a blocker of ion channels. Whole-cell patch-clamp experiments performed on cockroach neurons revealed that CSTX-1 produced a slow voltage-independent block of both mid/low- (M-LVA) and high-voltage-activated (HVA) insect Ca(v) channels. Since C. salei venom affects both insect as well as rodent species, we investigated whether Ca(v) channel currents of rat neurons are also inhibited by CSTX-1. CSTX-1 blocked rat neuronal L-type, but no other types of HVA Ca(v) channels, and failed to modulate LVA Ca(v) channel currents. Using neuroendocrine GH3 and GH4 cells, CSTX-1 produced a rapid voltage-independent block of L-type Ca(v) channel currents. The concentration-response curve was biphasic in GH4 neurons and the subnanomolar IC(50) values were at least 1000-fold lower than in GH3 cells. L-type Ca(v) channel currents of skeletal muscle myoballs and other voltage-gated ion currents of rat neurons, such as I(Na(v)) or I(K(v)) were not affected by CSTX-1. The high potency and selectivity of CSTX-1 for a subset of L-type channels in mammalian neurons may enable the toxin to be used as a molecular tool for the investigation of this family of Ca(v) channels.

摘要

在来自智利游走蛛毒液的CSTX-1结构中鉴定出的抑制剂胱氨酸结基序表明,这种毒素可能作为离子通道的阻滞剂发挥作用。对蟑螂神经元进行的全细胞膜片钳实验表明,CSTX-1对中/低电压激活(M-LVA)和高电压激活(HVA)昆虫Ca(v)通道均产生缓慢的电压非依赖性阻滞。由于智利游走蛛毒液会影响昆虫和啮齿动物物种,我们研究了大鼠神经元的Ca(v)通道电流是否也会被CSTX-1抑制。CSTX-1阻断大鼠神经元的L型,但不阻断其他类型的HVA Ca(v)通道,并且未能调节LVA Ca(v)通道电流。使用神经内分泌GH3和GH4细胞,CSTX-1对L型Ca(v)通道电流产生快速的电压非依赖性阻滞。浓度-反应曲线在GH4神经元中呈双相,亚纳摩尔IC(50)值比GH3细胞中至少低1000倍。骨骼肌肌球的L型Ca(v)通道电流和大鼠神经元的其他电压门控离子电流,如I(Na(v))或I(K(v))不受CSTX-1影响。CSTX-1对哺乳动物神经元中一部分L型通道的高效力和选择性可能使该毒素能够用作研究此Ca(v)通道家族的分子工具。

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