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经典 Wnt 信号通路介导 CD8 T 细胞非细胞溶解抗 HIV-1 活性,并与 HIV-1 临床状态相关。

Canonical Wnts Mediate CD8 T Cell Noncytolytic Anti-HIV-1 Activity and Correlate with HIV-1 Clinical Status.

机构信息

Department of Microbial Pathogens and Immunity, Rush University Medical Center, Chicago, IL 60612.

Division of Infectious Diseases, Rush University Medical Center, Chicago, IL 60612.

出版信息

J Immunol. 2020 Oct 15;205(8):2046-2055. doi: 10.4049/jimmunol.1801379. Epub 2020 Sep 4.

Abstract

CD8 T cells do not rely solely on cytotoxic functions for significant HIV control. Moreover, the noncytotoxic CD8 T cell antiviral response is a primary mediator of natural HIV control such as that seen in HIV elite controllers and long-term nonprogressors that does not require combined antiretroviral therapy. In this study, we investigated the biological factors contributing to the noncytotoxic control of HIV replication mediated by primary human CD8 T cells. We report that canonical Wnt signaling inhibits HIV transcription in an MHC-independent, noncytotoxic manner and that mediators of this pathway correlate with HIV controller clinical status. We show that CD8 T cells express all 19 Wnts and CD8 T cell-conditioned medium (CM) induced canonical Wnt signaling in infected recipient cells while simultaneously inhibiting HIV transcription. Antagonizing canonical Wnt activity in CD8 T cell CM resulted in increased HIV transcription in infected cells. Further, Wnt2b expression was upregulated in HIV controllers versus viremic patients, and in vitro depletion of Wnt2b and/or Wnt9b from CD8 CM reversed HIV inhibitory activity. Finally, plasma concentration of Dkk-1, an antagonist of canonical Wnt signaling, was higher in viremic patients with lower CD4 counts. This study demonstrates that canonical Wnt signaling inhibits HIV and significantly correlates with HIV controller status.

摘要

CD8 T 细胞并非仅依靠细胞毒性功能来实现对 HIV 的有效控制。此外,非细胞毒性 CD8 T 细胞抗病毒反应是自然控制 HIV 的主要介导因素,如在 HIV 精英控制者和长期非进展者中观察到的那样,这种反应不需要联合抗逆转录病毒治疗。在这项研究中,我们研究了导致原发性人 CD8 T 细胞介导的 HIV 复制非细胞毒性控制的生物学因素。我们报告称,经典 Wnt 信号以 MHC 非依赖性、非细胞毒性的方式抑制 HIV 转录,并且该途径的介导物与 HIV 控制者的临床状况相关。我们表明,CD8 T 细胞表达所有 19 种 Wnt,并且 CD8 T 细胞条件培养基 (CM) 在感染的受者细胞中诱导经典 Wnt 信号,同时抑制 HIV 转录。在 CD8 T 细胞 CM 中拮抗经典 Wnt 活性会导致感染细胞中的 HIV 转录增加。此外,与病毒血症患者相比,HIV 控制者中 Wnt2b 的表达上调,并且从 CD8 CM 体外耗竭 Wnt2b 和/或 Wnt9b 可逆转 HIV 抑制活性。最后,Dkk-1(经典 Wnt 信号的拮抗剂)的血浆浓度在病毒血症患者中较高,这些患者的 CD4 计数较低。这项研究表明,经典 Wnt 信号抑制 HIV,并且与 HIV 控制者的状态显著相关。

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