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来自蝎毒的一种兴奋性昆虫毒素和一种抑制性昆虫毒素均影响钠电导,并拥有一个共同的结合位点。

An excitatory and a depressant insect toxin from scorpion venom both affect sodium conductance and possess a common binding site.

作者信息

Zlotkin E, Kadouri D, Gordon D, Pelhate M, Martin M F, Rochat H

出版信息

Arch Biochem Biophys. 1985 Aug 1;240(2):877-87. doi: 10.1016/0003-9861(85)90098-0.

Abstract

Two insect selective toxins were purified by gel-permeation and ion-exchange chromatographies from the venom of the scorpion, Leiurus quinquestriatus quinquestriatus, and their chemical and pharmacological properties were studied. The first toxin (LqqIT1) induces a fast excitatory contraction paralysis of fly larvae and is about 40 times more toxic than the crude venom. It is a polypeptide composed of 71 amino acids, including 8 half-cystines and devoid of methionine and tryptophan, with an estimated molecular weight of 8189 and a pI value of 8.5. The second toxin (LqqIT2) induces a slow depressant, flaccid paralysis of fly larvae. It is composed of 72 amino acids, including 8 half-cystines, is devoid of proline methionine and histidine, and has an estimated molecular weight of 7990 and a pI value of 8.3. The contrasting symptomatology of these toxins is interpreted in terms of their effects on an isolated axonal preparation of the cockroach in current and voltage clamp conditions. LqqIT1 (0.5-4 microM) induced repetitive firing of the axon which was attributable to two changes in the sodium conductance, a small increase in the peak conductance and a slowing of its turning off. LqqIT2 (1-8 microM) caused a blockage of the evoked action potentials, attributable to both a strong depolarization of the axonal membrane and a progressive suppression of the sodium current. Neither toxin affected potassium conductance. The two toxins differ mainly in their opposite effects on the activatable sodium permeability. In binding assays to a preparation of insect synaptosomal membrane vesicles, the two toxins were shown to competitively displace the radioiodinated excitatory insect toxin derived from the venom of the scorpion, Androctonus australis [( 125I]AaIT), which strongly resembles, in its chemistry and action, the LqqIT1 toxin. The present two toxins have demonstrated a strong affinity closely resembling the AaIT, with KD values of 0.4, 1.9, and 1.0 nM for LqqIT1, LqqIT2, and AaIT, respectively. These data suggest the possibility that the excitatory and depressant insect toxins share a common binding site associated with sodium channels in insect neuronal membranes.

摘要

从蝎子黄肥尾蝎(Leiurus quinquestriatus quinquestriatus)的毒液中通过凝胶渗透色谱法和离子交换色谱法纯化出两种昆虫选择性毒素,并对其化学和药理特性进行了研究。第一种毒素(LqqIT1)可诱导果蝇幼虫快速兴奋性收缩麻痹,其毒性比粗毒液高约40倍。它是一种由71个氨基酸组成的多肽,包括8个半胱氨酸,不含甲硫氨酸和色氨酸,估计分子量为8189,pI值为8.5。第二种毒素(LqqIT2)可诱导果蝇幼虫缓慢的抑制性、弛缓性麻痹。它由72个氨基酸组成,包括8个半胱氨酸,不含脯氨酸、甲硫氨酸和组氨酸,估计分子量为7990,pI值为8.3。根据这些毒素在电流钳和电压钳条件下对蟑螂离体轴突标本的作用,对它们截然不同的症状学进行了解释。LqqIT1(0.5 - 4 microM)可诱导轴突重复放电,这归因于钠电导的两种变化,即峰值电导的小幅增加及其关闭的减慢。LqqIT2(1 - 8 microM)导致诱发动作电位的阻断,这归因于轴突膜的强烈去极化和钠电流的逐渐抑制。两种毒素均不影响钾电导。这两种毒素的主要区别在于它们对可激活钠通透性的相反作用。在与昆虫突触体膜囊泡制剂的结合试验中,这两种毒素被证明可竞争性取代源自蝎子澳链尾蝎(Androctonus australis)毒液的放射性碘化兴奋性昆虫毒素[(125I]AaIT),其化学和作用与LqqIT1毒素非常相似。目前的这两种毒素已显示出与AaIT非常相似的强亲和力,LqqIT1、LqqIT2和AaIT的KD值分别为0.4、1.9和1.0 nM。这些数据表明,兴奋性和抑制性昆虫毒素可能共享一个与昆虫神经元膜中的钠通道相关的共同结合位点。

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