Kirsch G E, Alam M, Hartmann H A
Department of Anesthesiology, Baylor College of Medicine, Houston, Texas 77030.
Biophys J. 1994 Dec;67(6):2305-15. doi: 10.1016/S0006-3495(94)80716-7.
We have probed a cysteine residue that confers resistance to tetrodotoxin (TTX) block in heart Na channels, with membrane-impermeant, cysteine-specific, methanethiosulfonate (MTS) analogs. Covalent addition of a positively charged group to the cysteinyl sulfhydryl reduced pore conductance by 87%. The effect was selectively prevented by treatment with TTX, but not saxitoxin (STX). Addition of a negatively charged group selectively inhibited STX block without affecting TTX block. These results agree with models that place an exposed cysteinyl sulfhydryl in the TTX site adjacent to the mouth of the pore, but do not support the contention that STX and TTX are interchangeable. The surprising differences between the two toxins are consistent with the hypothesis that the toxin-receptor complex can assume different conformations when STX or TTX bound.
我们使用膜不通透性、半胱氨酸特异性的甲硫基磺酸盐(MTS)类似物,探究了心脏钠通道中赋予对河豚毒素(TTX)阻断具有抗性的一个半胱氨酸残基。向半胱氨酸巯基共价添加一个带正电荷的基团,可使孔道电导降低87%。用TTX处理可选择性地阻止这种效应,但用石房蛤毒素(STX)处理则不能。添加一个带负电荷的基团可选择性地抑制STX阻断,而不影响TTX阻断。这些结果与将一个暴露的半胱氨酸巯基置于靠近孔口的TTX位点的模型一致,但不支持STX和TTX可互换的观点。这两种毒素之间令人惊讶的差异与以下假设一致,即当结合STX或TTX时,毒素-受体复合物可呈现不同的构象。
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