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热休克蛋白 90 的 K64 乙酰化抑制家蚕核多角体病毒的复制。

K64 acetylation of heat shock protein 90 suppresses nucleopolyhedrovirus replication in Bombyx mori.

机构信息

Department of Biopharmaceuticals, College of Life Sciences and Medicine, Zhejiang Sci-Tech University, Hangzhou, Zhejiang, China.

Zhejiang Provincial Key Laboratory of Silkworm Bioreactor and Biomedicine, Hangzhou, Zhejiang, China.

出版信息

Arch Insect Biochem Physiol. 2024 Jan;115(1):e22079. doi: 10.1002/arch.22079.

Abstract

HSP90 is a highly conserved chaperone that facilitates the proliferation of many viruses, including silkworm (bombyx mori) nucleopolyhedrovirus (BmNPV), but the underlying regulatory mechanism was unclear. We found that suppression of HSP90 by 17-AAG, a HSP90-specific inhibitor, significantly reduced the expression of BmNPV capsid protein gp64 and viral genome replication, whereas overexpression of B. mori HSP90(BmHSP90) promoted BmNPV replication. Furthermore, in a recent study of the lysine acetylome of B. mori infected with BmNPV, we focused on the reduced viral proliferation due to changes of BmHSP90 lysine acetylation. Site-directed introduction of acetylated (K/Q) or deacetylated (K/R) mimic mutations into BmHSP90 revealed that lysine 64 (K64) acetylation activated the JAK/STAT pathway and reduced BmHSP90 ATPase activity, leading to diminished chaperone activity and ultimately inhibiting BmNPV proliferation. In this study, a single lysine 64 acetylation change of BmHSP90 was elucidated as a model of posttranslational modifications occurring in the wake of host-virus interactions, providing novel insights into potential antiviral strategies.

摘要

热休克蛋白 90(HSP90)是一种高度保守的伴侣蛋白,可促进多种病毒的增殖,包括家蚕(Bombyx mori)核型多角体病毒(BmNPV),但其潜在的调控机制尚不清楚。我们发现,HSP90 特异性抑制剂 17-AAG 的抑制作用可显著降低 BmNPV 衣壳蛋白 gp64 的表达和病毒基因组的复制,而 B. mori HSP90(BmHSP90)的过表达则促进了 BmNPV 的复制。此外,在最近一项对感染 BmNPV 的家蚕赖氨酸乙酰化组的研究中,我们关注了由于 BmHSP90 赖氨酸乙酰化变化导致的病毒增殖减少。将乙酰化(K/Q)或去乙酰化(K/R)模拟突变定点引入 BmHSP90 后发现,赖氨酸 64(K64)乙酰化激活了 JAK/STAT 通路,降低了 BmHSP90 的 ATP 酶活性,导致伴侣活性降低,最终抑制了 BmNPV 的增殖。本研究以 BmHSP90 的单个赖氨酸 64 乙酰化变化为模型,阐明了宿主-病毒相互作用后发生的翻译后修饰,为潜在的抗病毒策略提供了新的见解。

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