Avian TRIM13 attenuates antiviral innate immunity by targeting MAVS for autophagic degradation.

Peng Zhou, Qingxiang Zhang, Yueshan Yang, Dong Chen, Anan Jongkaewwattana, Hui Jin, Hongbo Zhou, Rui Luo
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Abstract

MAVS (mitochondrial antiviral signaling protein) is a crucial adaptor in antiviral innate immunity that must be tightly regulated to maintain immune homeostasis. In this study, we identified the duck Anas platyrhynchos domesticus TRIM13 (ApdTRIM13) as a novel negative regulator of duck MAVS (ApdMAVS) that mediates the antiviral innate immune response. Upon infection with RNA viruses, ApdTRIM13 expression increased, and it specifically binds to ApdMAVS through its TM domain, facilitating the degradation of ApdMAVS in a manner independent of E3 ligase activity. Furthermore, ApdTRIM13 recruits the autophagic cargo receptor duck SQSTM1 (ApdSQSTM1), which facilitates its interaction with ApdMAVS independent of ubiquitin signaling, and subsequently delivers ApdMAVS to phagophores for degradation. Depletion of ApdSQSTM1 reduces ApdTRIM13-mediated autophagic degradation of ApdMAVS, thereby enhancing the antiviral immune response. Collectively, our findings reveal a novel mechanism by which ApdTRIM13 regulates type I interferon production by targeting ApdMAVS for selective autophagic degradation mediated by ApdSQSTM1, providing insights into the crosstalk between selective autophagy and innate immune responses in avian species.

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禽类TRIM13通过靶向MAVS进行自噬降解来削弱抗病毒先天免疫力。
MAVS(线粒体抗病毒信号蛋白)是抗病毒先天免疫中的一个关键适配因子,必须对其进行严格调控才能维持免疫平衡。在这项研究中,我们发现鸭TRIM13(ApdTRIM13)是鸭MAVS(ApdMAVS)的一种新型负调控因子,可介导抗病毒先天性免疫反应。感染 RNA 病毒后,ApdTRIM13 的表达量增加,它通过其 TM 结构域特异性地与 ApdMAVS 结合,以一种独立于 E3 连接酶活性的方式促进 ApdMAVS 的降解。此外,ApdTRIM13还能招募自噬货物受体鸭SQSTM1(ApdSQSTM1),从而促进其与ApdMAVS的相互作用,而不依赖于泛素信号转导,并随后将ApdMAVS送到吞噬细胞中降解。消耗 ApdSQSTM1 会减少 ApdTRIM13 介导的 ApdMAVS 自噬降解,从而增强抗病毒免疫反应。总之,我们的研究结果揭示了一种新的机制,即 ApdTRIM13 通过将 ApdMAVS 靶向于 ApdSQSTM1 介导的选择性自噬降解来调节 I 型干扰素的产生,为了解禽类物种中选择性自噬与先天性免疫应答之间的相互关系提供了深入的见解。
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Deciphering melanophagy: role of the PTK2-ITCH-MLANA-OPTN cascade on melanophagy in melanocytes. HSP90 N-terminal inhibition promotes mitochondria-derived vesicles related metastasis by reducing TFEB transcription via decreased HSP90AA1-HCFC1 interaction in liver cancer. Efficient PHB2 (prohibitin 2) exposure during mitophagy depends on VDAC1 (voltage dependent anion channel 1). PINK1-deficiency facilitates mitochondrial iron accumulation and colon tumorigenesis. Avian TRIM13 attenuates antiviral innate immunity by targeting MAVS for autophagic degradation.
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