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DNA-Packing Portal and Capsid-Associated Tegument Complexes in the Tumor Herpesvirus KSHV

机译:肿瘤疱疹病毒KSHV中的DNA包装门户和衣壳相关的外皮复合体

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摘要

Assembly of Kaposi’s sarcoma-associated herpesvirus (KSHV) begins at a bacteriophage-like portal complex that nucleates formation of an icosahedral capsid with capsid-associated tegument complexes (CATCs) and facilitates translocation of an ∼150-kb dsDNA genome, followed by acquisition of a pleomorphic tegument and envelope. Because of deviation from icosahedral symmetry, KSHV portal and tegument structures have largely been obscured in previous studies. Using symmetry-relaxed cryo-EM, we determined the structure of the KSHV portal and its interactions with surrounding capsid proteins, CATCs, and the terminal end of KSHV’s dsDNA genome. Our atomic models of the portal and capsid/CATC, together with visualization of CATCs’ variable occupancy and alternate orientation of CATC-interacting vertex triplexes, suggest a mechanism whereby the portal orchestrates procapsid formation and asymmetric long-range determination of CATC attachment during DNA packaging prior to pleomorphic tegumentation/envelopment. Structure-based mutageneses confirm that a triplex deep binding groove for CATCs is a hotspot that holds promise for antiviral development.
机译:卡波济氏肉瘤相关疱疹病毒(KSHV)的组装始于噬菌体样的门户复合物,该复合物使二十面体衣壳与衣壳相关的外皮复合物(CATC)成核,并促进约150 kb dsDNA基因组的易位,随后获得多形的外皮和信封。由于偏离二十面体对称性,在先前的研究中很大程度上掩盖了KSHV门和被膜结构。我们使用对称松弛的cryo-EM,确定了KSHV门户的结构及其与周围衣壳蛋白,CATC和KSHV dsDNA基因组末端的相互作用。我们的门户和衣壳/ CATC原子模型,以及CATC可变占有率的可视化以及与CATC相互作用的顶点三元体的交替取向,提出了一种机制,通过该机制,门户在DNA包装过程中编排衣壳形成和CATC附着的不对称远程确定进行多形的外皮/包膜之前。基于结构的突变体证实,CATC的三链体深结合槽是一个热点,为抗病毒的发展提供了希望。

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