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蝎α-样毒素对哺乳动物和昆虫均有毒性,它与哺乳动物和昆虫电压门控钠通道上的受体位点3存在不同的相互作用。

Scorpion alpha-like toxins, toxic to both mammals and insects, differentially interact with receptor site 3 on voltage-gated sodium channels in mammals and insects.

作者信息

Cestèle S, Stankiewicz M, Mansuelle P, De Waard M, Dargent B, Gilles N, Pelhate M, Rochat H, Martin-Eauclaire M F, Gordon D

机构信息

Laboratire de Biochimie, Ingénierie des Protéines, CNRS UMR 6560, France.

出版信息

Eur J Neurosci. 1999 Mar;11(3):975-85. doi: 10.1046/j.1460-9568.1999.00505.x.

Abstract

alpha-Like toxins, a unique group designated among the scorpion alpha-toxin class that inhibit sodium channel inactivation, are highly toxic to mice but do not compete for alpha-toxin binding to receptor site 3 on rat brain sodium channels. We analysed the sequence of a new alpha-like toxin, which was also highly active on insects, and studied its action and binding on both mammalian and insect sodium channels. Action of the alpha-like toxin on isolated cockroach axon is similar to that of an alpha-toxin, and the radioactive toxin binds with a high affinity to insect sodium channels. Other sodium channel neurotoxins interact competitively or allosterically with the insect alpha-like toxin receptor site, similarly to alpha-toxins, suggesting that the alpha-like toxin receptor site is closely related to receptor site 3. Conversely, on rat brain sodium channels, specific binding of 125I-alpha-like toxin could not be detected, although at high concentration it inhibits sodium current inactivation on rat brain sodium channels. The difficulty in measuring binding to rat brain channels may be attributed to low-affinity binding due to the acidic properties of the alpha-like toxins that also impair the interaction with receptor site 3. The results suggest that alpha-like toxins bind to a distinct receptor site on sodium channels that is differentially related to receptor site 3 on mammalian and insect sodium channels.

摘要

α-样毒素是蝎α-毒素类中独特的一组,可抑制钠通道失活,对小鼠剧毒,但不与α-毒素竞争结合大鼠脑钠通道上的受体位点3。我们分析了一种新的α-样毒素的序列,该毒素对昆虫也具有高活性,并研究了其对哺乳动物和昆虫钠通道的作用及结合情况。α-样毒素对分离的蟑螂轴突的作用与α-毒素相似,放射性毒素以高亲和力与昆虫钠通道结合。其他钠通道神经毒素与昆虫α-样毒素受体位点竞争性或别构性相互作用,类似于α-毒素,这表明α-样毒素受体位点与受体位点3密切相关。相反,在大鼠脑钠通道上,虽然高浓度时它可抑制大鼠脑钠通道的钠电流失活,但未检测到125I-α-样毒素的特异性结合。难以测量与大鼠脑通道的结合可能归因于α-样毒素的酸性性质导致的低亲和力结合,这也损害了与受体位点3的相互作用。结果表明,α-样毒素与钠通道上一个独特的受体位点结合,该位点与哺乳动物和昆虫钠通道上的受体位点3有不同的关系。

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