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蝎α毒素 LqhαIT 特异性地与电压门控钠离子通道孔域的聚糖相互作用。

Scorpion α-toxin LqhαIT specifically interacts with a glycan at the pore domain of voltage-gated sodium channels.

机构信息

Discovery Sciences, Novartis Biomedical Research, 250 Massachusetts Avenue, Cambridge, MA 02139, USA.

Global Discovery Chemistry, Novartis Biomedical Research, 181 Massachusetts Avenue, Cambridge, MA 02139, USA.

出版信息

Structure. 2024 Oct 3;32(10):1611-1620.e4. doi: 10.1016/j.str.2024.07.021. Epub 2024 Aug 23.

Abstract

Voltage-gated sodium (Nav) channels sense membrane potential and drive cellular electrical activity. The deathstalker scorpion α-toxin LqhαIT exerts a strong action potential prolonging effect on Nav channels. To elucidate the mechanism of action of LqhαIT, we determined a 3.9 Å cryoelectron microscopy (cryo-EM) structure of LqhαIT in complex with the Nav channel from Periplaneta americana (NavPas). We found that LqhαIT binds to voltage sensor domain 4 and traps it in an "S4 down" conformation. The functionally essential C-terminal epitope of LqhαIT forms an extensive interface with the glycan scaffold linked to Asn330 of NavPas that augments a small protein-protein interface between NavPas and LqhαIT. A combination of molecular dynamics simulations, structural comparisons, and prior mutagenesis experiments demonstrates the functional importance of this toxin-glycan interaction. These findings establish a structural basis for the specificity achieved by scorpion α-toxins and reveal the conserved glycan as an essential component of the toxin-binding epitope.

摘要

电压门控钠离子(Nav)通道感知膜电位并驱动细胞电活动。死亡杀手蝎 α-毒素 LqhαIT 对 Nav 通道具有很强的动作电位延长作用。为了阐明 LqhαIT 的作用机制,我们确定了 LqhαIT 与美洲大蠊(NavPas)Nav 通道复合物的 3.9Å 冷冻电镜(cryo-EM)结构。我们发现 LqhαIT 结合到电压传感器域 4 并将其捕获在“S4 向下”构象中。LqhαIT 的功能必需的 C 末端表位与与 NavPas 的 Asn330 相连的聚糖支架形成广泛的界面,增强了 NavPas 和 LqhαIT 之间的小蛋白-蛋白界面。分子动力学模拟、结构比较和先前的突变实验的组合证明了这种毒素-聚糖相互作用的功能重要性。这些发现为蝎 α-毒素所达到的特异性建立了结构基础,并揭示了保守聚糖作为毒素结合表位的重要组成部分。

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