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Characterization of Kbot21 Reveals Novel Side Chain Interactions of Scorpion Toxins Inhibiting Voltage-Gated Potassium Channels

机译:Kbot21的表征揭示了蝎毒素抑制电压门控钾通道的新型侧链相互作用。

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摘要

Scorpion toxins are important pharmacological tools for probing the physiological roles of ion channels which are involved in many physiological processes and as such have significant therapeutic potential. The discovery of new scorpion toxins with different specificities and affinities is needed to further characterize the physiology of ion channels. In this regard, a new short polypeptide called Kbot21 has been purified to homogeneity from the venom of Buthus occitanus tunetanus scorpion. Kbot21 is structurally related to BmBKTx1 from the venom of the Asian scorpion Buthus martensii Karsch. These two toxins differ by only two residues at position 13 (R /V) and 24 (D/N).Despite their very similar sequences, Kbot21 and BmBKTx1 differ in their electrophysiological activities. Kbot21 targets KV channel subtypes whereas BmBKTx1 is active on both big conductance (BK) and small conductance (SK) Ca2+-activated K+ channel subtypes, but has no effects on Kv channel subtypes. The docking model of Kbot21 with the Kv1.2 channel shows that the D24 and R13 side-chain of Kbot21 are critical for its interaction with KV channels.
机译:蝎毒素是探测离子通道的生理作用的重要药理工具,离子通道涉及许多生理过程,因此具有重大的治疗潜力。需要发现具有不同特异性和亲和力的新蝎毒素以进一步表征离子通道的生理特性。在这方面,一种新的称为Kbot21的短多肽已经从Buthus occitanus tunetanus蝎子的毒液中纯化至同质。 Kbot21在结构上与亚洲蝎子Buthus martensii Karsch的毒液中的BmBKTx1有关。这两种毒素在第13位(R / V)和第24位(D / N)仅相差两个残基。尽管它们的序列非常相似,但Kbot21和BmBKTx1的电生理活性不同。 Kbot21靶向KV通道亚型,而BmBKTx1对大电导(BK)和小电导(SK)Ca 2 + 激活的K + 通道亚型均有效,但没有作用在Kv频道子类型上Kbot21与Kv1.2通道的对接模型表明,Kbot21的D24和R13侧链对于其与KV通道的交互至关重要。

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