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首页> 外文期刊>PLoS Pathogens >Phospholipid synthesis fueled by lipid droplets drives the structural development of poliovirus replication organelles
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Phospholipid synthesis fueled by lipid droplets drives the structural development of poliovirus replication organelles

机译:脂滴驱动的磷脂合成驱动脊髓灰质炎病毒复制细胞器的结构发展

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Rapid development of complex membranous replication structures is a hallmark of picornavirus infections. However, neither the mechanisms underlying such dramatic reorganization of the cellular membrane architecture, nor the specific role of these membranes in the viral life cycle are sufficiently understood. Here we demonstrate that the cellular enzyme CCTα, responsible for the rate-limiting step in phosphatidylcholine synthesis, translocates from the nuclei to the cytoplasm upon infection and associates with the replication membranes, resulting in the rerouting of lipid synthesis from predominantly neutral lipids to phospholipids. The bulk supply of long chain fatty acids necessary to support the activated phospholipid synthesis in infected cells is provided by the hydrolysis of neutral lipids stored in lipid droplets. Such activation of phospholipid synthesis drives the massive membrane remodeling in infected cells. We also show that complex membranous scaffold of replication organelles is not essential for viral RNA replication but is required for protection of virus propagation from the cellular anti-viral response, especially during multi-cycle replication conditions. Inhibition of infection-specific phospholipid synthesis provides a new paradigm for controlling infection not by suppressing viral replication but by making it more visible to the immune system.
机译:复杂的膜复制结构的快速发展是小核糖核酸病毒感染的标志。然而,既没有充分了解这种细胞膜结构戏剧性重组的机制,也没有充分了解这些膜在病毒生命周期中的特定作用。在这里,我们证明了负责磷脂酰胆碱合成中限速步骤的细胞酶CCTα在感染后从细胞核转移到细胞质并与复制膜结合,从而导致脂质合成从主要的中性脂质重新路由到磷脂。支持被感染细胞中活化的磷脂合成的长链脂肪酸的大量供应是由脂质滴中储存的中性脂质的水解提供的。磷脂合成的这种活化驱动受感染细胞中的大规模膜重塑。我们还显示,复制细胞器的复杂膜状支架对于病毒RNA复制不是必不可少的,但是对于保护病毒免受细胞抗病毒应答的传播是必需的,尤其是在多周期复制条件下。抑制感染特异性磷脂合成为控制感染提供了新的范式,而不是通过抑制病毒复制,而是通过使免疫系统更易察觉。

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