RhCMV expands CCR5+ memory T cells and promotes SIV reservoir seeding in the gut mucosa
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
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
View: Text | PDF
Research Article AIDS/HIV Immunology

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

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.

Authors

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

×

Figure 4

RhCMV serostatus during SIV infection is associated with heightened monocyte activation and increased persistence of CCR5+CD4+ T cells in the gut.

Options: View larger image (or click on image) Download as PowerPoint
RhCMV serostatus during SIV infection is associated with heightened mono...
(A) Histogram and CD169+ monocyte median fluorescence intensity (MFI) by RhCMV serostatus in PBMC. (B) Two-sided Spearman’s correlation between CD169+ monocyte MFI against plasma VL. (C) Plasma IFN-α expression by RhCMV serostatus. (D) %HLA-DR+CD4+ memory T cells across sampled tissue by RhCMV serostatus. (E) %HLA-DR+CD8+ memory T cells across sampled tissue by RhCMV serostatus. (F) %Ki-67+CD4+ memory T cells across sampled tissue by RhCMV serostatus. (G) %Ki-67+CD8+ memory T cells across sampled tissue by RhCMV serostatus. (H) Two-sided Spearman’s correlation between %Ki-67+CD8+ memory T cells against cell-associated SIV DNA. (I) %Ki-67+CD8+ memory T cells by plasma IFN-α above or below 10 pg/mL (>10 and <10 respectively). (J) %CCR5+CD4+ memory T cells across sampled tissue by RhCMV serostatus. (K) %CCR5+CD4+ T cells log2 fold change (FC) pre-SIV mean ± SEM across duodenum and colon by RhCMV serostatus. (L) Two-sided Spearman’s correlation between %CCR5+CD4+ memory cells against cell-associated SIV DNA. (M) %CXCR3+ of CD4+ memory T cells across duodenum and colon by RhCMV serostatus. For all figures RhCMV+ n = 11, RhCMV n = 8. For A, B, DG, I, J, and M error bars represent 1.5 times the interquartile range. Statistical comparison performed using 2-sided Mann-Whitney U test. For B, H, and L shaded area represents 95% confidence interval. LN, lymph node; BM, bone marrow; PBMC, peripheral blood mononuclear cells; * P < 0.05; ** P < 0.01; *** P < 0.001; **** P < 0.0001.