RhCMV expands CCR5+ memory T cells and promotes SIV reservoir seeding in the gut mucosa

RhCMV可扩增CCR5+记忆T细胞,并促进SIV病毒库在肠道黏膜中的定植。

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作者:Chrysostomos Perdios,Naveen Suresh Babu,Celeste D Coleman,Anna T Brown,Shevon N Alexander,Matilda J Moström,Carolina Allers,Lara Doyle-Meyers,Christine M Fennessey,Lori A Rowe,Brandon F Keele,Amitinder Kaur,Michael L Freeman,Joseph C Mudd

Abstract

Cytomegalovirus (CMV) is a prevalent β-herpesvirus that persists asymptomatically in immunocompetent hosts. In people with HIV-1 (PWH), CMV is associated with HIV-1 persistence and particular inflammatory-related comorbidities. The true causative role of CMV in HIV-associated pathologies, however, remains unclear given that nearly all PWH are coinfected with CMV. In this study, we examined acute phase immune and virological dynamics in cohorts of SIV-infected rhesus macaques (RMs) that were naturally seropositive or -negative for rhesus CMV (RhCMV). We observed prior to SIV, RhCMV expanded a polyclonal population of target CCR5+CD4+ T cells in gut and lymph nodes that expressed the chemotactic receptor CXCR3 and were largely not specific for RhCMV. Upon SIV infection, RhCMV+ RMs exhibited higher peak viremia and elevated levels of SIV DNA in the upper and lower intestine. Greater seeding of SIV DNA was associated with a maintenance of CCR5-expressing CD4+ T cells that were enriched within the RhCMV+ gut along a CXCR3/CXCL9 chemotactic axis. Overall, the data suggest that RhCMV can promote SIV susceptibility within a diverse, polyclonal pool of CD4+ T cells that are not entirely RhCMV specific.

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