洞察 MIC2 和 M2AP 的分子相互作用:TSR6 的作用和跨物种保护

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-10-22 DOI:10.1002/prot.26758
Xu Xia, Chenqiang Du, Yang Wang, Gaojie Song
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引用次数: 0

摘要

小体蛋白2(MIC2)及其相关蛋白M2AP对弓形虫的滑翔运动和宿主细胞侵袭至关重要。在之前的研究中,我们发现 M2AP 与 MIC2 的第六个 TSR 结构域特异性结合,这种相互作用主要由位于 TSR6 中心的热点残基 H620 介导。为了深入研究 H620 的功能意义并探索 Y602 的动态行为,我们对弓形虫 TSR6-M2AP 复合物(包括野生型和突变型)进行了分子动力学(MD)模拟。我们的发现强调了 H620 在 TSR6 中的关键作用,尤其是它与 M2AP 的 K72 之间的氢键相互作用。H620A 突变破坏了附近的疏水网络,而对其他亲水相互作用的影响却很小。此外,我们的数据揭示了不同物种中 M2AP 与 TSR6 之间高度保守的结合姿势,这与之前的跨种研究一致,从而为未来感染控制策略的开发提供了启示。
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Insights Into the Molecular Interactions of MIC2 and M2AP: Role of TSR6 and Conservation Across Species.

Microneme protein 2 (MIC2) and its associated protein M2AP are pivotal for the gliding motility and host cell invasion by Toxoplasma gondii. In our prior work, we showed that M2AP binds specifically to the sixth TSR domain of MIC2, with this interaction mediated dominantly by the hotspot residue H620 situated at the center of TSR6. To delve deeper into the functional significance of H620 and explore the dynamic behavior of Y602, we conducted molecular dynamic (MD) simulations of the Toxoplasma TSR6-M2AP complex, encompassing both wild-type and mutant forms. Our findings underscore the critical role of H620 within TSR6, particularly its hydrogen bond interaction with K72 of M2AP. The H620A mutation disrupts the nearby hydrophobic network while minimally affecting other hydrophilic interactions. Furthermore, our data reveal a highly conserved binding pose between M2AP and TSR6 across different species, consistent with previous trans-genera studies, thereby offering insights for future strategies in infection control development.

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CiteScore
7.20
自引率
4.30%
发文量
567
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