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BRLF1 抑制 EBV 裂解周期早期 RNA Pol III 介导的 RIG-I 炎性小体激活。

BRLF1 suppresses RNA Pol III-mediated RIG-I inflammasome activation in the early EBV lytic lifecycle.

机构信息

Institute of Human Virology, Zhongshan School of Medicine, Sun Yat-Sen University, Guangzhou, Guangdong, China.

Key Laboratory of Tropical Disease Control (Sun Yat-Sen University), Ministry of Education, Guangzhou, Guangdong, China.

出版信息

EMBO Rep. 2021 Jan 7;22(1):e50714. doi: 10.15252/embr.202050714. Epub 2020 Nov 23.

DOI:10.15252/embr.202050714
PMID:33225563
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7788446/
Abstract

Latent infection with herpesviruses constitutively activates inflammasomes, while lytic replication suppresses their activation through distinct mechanisms. However, how Epstein-Barr virus (EBV) lytic replication inhibits the activation of inflammasomes remains unknown. Here, we reveal that the EBV immediate-early protein BRLF1 inhibits inflammasome activation, and BRLF1 deficiency significantly increases the activation of inflammasomes and pyroptosis during early lytic lifecycle. BRLF1 interacts with RNA polymerase III subunits to suppress immunostimulatory small RNA transcription, RIG-I inflammasome activation, and antiviral responses. Consequently, BRLF1-deficient EBV primary infection induces robust T-cell and NK cell activation and killing through IL-1β and IL-18. A BRLF1-derived peptide that inhibits inflammasome activation is sufficient to suppress T-cell and NK cell responses during BRLF1-deficient EBV primary infection in lymphocytes. These results reveal a novel mechanism involved in the evasion of inflammasome activation and antiviral responses during EBV early lytic infection and provide a promising approach for the manipulation of inflammasomes against infection of oncogenic herpesviruses.

摘要

潜伏感染的疱疹病毒持续激活炎症小体,而裂解复制则通过不同的机制抑制其激活。然而,EBV 裂解复制如何抑制炎症小体的激活尚不清楚。在这里,我们揭示了 EBV 早期即刻蛋白 BRLF1 抑制炎症小体的激活,并且 BRLF1 缺陷显著增加了早期裂解周期中炎症小体和细胞焦亡的激活。BRLF1 与 RNA 聚合酶 III 亚基相互作用,抑制免疫刺激小 RNA 的转录、RIG-I 炎症小体的激活和抗病毒反应。因此,BRLF1 缺陷型 EBV 原发性感染通过 IL-1β 和 IL-18 诱导强烈的 T 细胞和 NK 细胞激活和杀伤。抑制炎症小体激活的 BRLF1 衍生肽足以抑制 BRLF1 缺陷型 EBV 原发性感染在淋巴细胞中引起的 T 细胞和 NK 细胞反应。这些结果揭示了 EBV 早期裂解感染期间逃避炎症小体激活和抗病毒反应的一种新机制,并为操纵炎症小体对抗致癌疱疹病毒感染提供了一种有前途的方法。

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