Depression compromises antiviral innate immunity via the AVP-AHI1-Tyk2 axis

抑郁症通过 AVP-AHI1-Tyk2 轴损害抗病毒先天免疫力。

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作者:Hong-Guang Zhang #,Bin Wang #,Yong Yang,Xuan Liu,Junjie Wang,Ning Xin,Shifeng Li,Ying Miao,Qiuyu Wu,Tingting Guo,Yukang Yuan,Yibo Zuo,Xiangjie Chen,Tengfei Ren,Chunsheng Dong,Jun Wang,Hang Ruan,Miao Sun,Xingshun Xu ,Hui Zheng

Abstract

Depression is a serious public-health issue. Recent reports have suggested higher susceptibility to viral infections in depressive patients. However, how depression affects antiviral innate immune signaling remains unknown. Here, we revealed a reduction in expression of Abelson helper integration site 1 (AHI1) in the peripheral blood mononuclear cells (PBMCs) and macrophages from the patients with major depressive disorder (MDD), which leads to attenuated antiviral immune response. We found that depression-related arginine vasopressin (AVP) induces reduction of AHI1 in macrophages. Further studies demonstrated that AHI1 is a critical stabilizer of basal type-I-interferon (IFN-I) signaling. Mechanistically, AHI1 recruits OTUD1 to deubiquitinate and stabilize Tyk2, while AHI1 reduction downregulates Tyk2 and IFN-I signaling activity in macrophages from both MDD patients and depression model mice. Interestingly, we identified a clinical analgesic meptazinol that effectively stimulates AHI1 expression, thus enhancing IFN-I antiviral defense in depression model mice. Our study promotes the understanding of the signaling mechanisms of depression-mediated antiviral immune dysfunction, and reveals meptazinol as an enhancer of antiviral innate immunity in depressive patients.

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