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An Annular Lipid Belt Is Essential for Allosteric Coupling and Viral Inhibition of the Antigen Translocation Complex TAP (Transporter Associated with Antigen Processing)

机译:环形脂质带对于抗原转运复合物TAP(与抗原加工相关的转运蛋白)的变构偶联和病毒抑制是必不可少的

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摘要

The transporter associated with antigen processing (TAP) constitutes a focal element in the adaptive immune response against infected or malignantly transformed cells. TAP shuttles proteasomal degradation products into the lumen of the endoplasmic reticulum for loading of major histocompatibility complex (MHC) class I molecules. Here, the heterodimeric TAP complex was purified and reconstituted in nanodiscs in defined stoichiometry. We demonstrate that a single heterodimeric core-TAP complex is active in peptide binding, which is tightly coupled to ATP hydrolysis. Notably, with increasing peptide length, the ATP turnover was gradually decreased, revealing that ATP hydrolysis is coupled to the movement of peptide through the ATP-binding cassette transporter. In addition, all-atom molecular dynamics simulations show that the observed 22 lipids are sufficient to form an annular belt surrounding the TAP complex. This lipid belt is essential for high affinity inhibition by the herpesvirus immune evasin ICP47. In conclusion, nanodiscs are a powerful approach to study the important role of lipids as well as the function, interaction, and modulation of the antigen translocation machinery.
机译:与抗原加工(TAP)相关的转运蛋白构成针对感染或恶性转化细胞的适应性免疫应答中的焦点元素。 TAP将蛋白酶体降解产物穿梭到内质网腔中,以装载主要的组织相容性复合体(MHC)I类分子。在这里,异二聚体TAP复合物被纯化,并以确定的化学计量在纳米圆盘中重构。我们证明了一个单一的异二聚体核心-TAP复合物是活跃的肽结合,这与ATP水解紧密耦合。值得注意的是,随着肽长度的增加,ATP周转率逐渐降低,这表明ATP水解与通过ATP结合盒转运蛋白的肽运动有关。此外,所有原子的分子动力学模拟表明,观察到的22种脂质足以形成围绕TAP复合物的环形带。该脂质带对于疱疹病毒免疫evasin ICP47抑制高亲和力至关重要。总之,纳米光盘是研究脂质的重要作用以及抗原转运机制的功能,相互作用和调节的有效方法。

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