Abstract
Abstract The efficacy of HIV vaccines relies on potent antibody (Ab) responses at major transmission sites such as the female genital tract (FGT). CD4+ T follicular helper (TFH) cells, specialized in providing B cell help in germinal centers (GCs) of secondary lymphoid organs, play an important role in initial stages of HIV-specific Ab responses. Here we investigated SIV-specific T and B cell responses and FGT immunity in Rhesus macaques following mucosal priming with Ad5hr-SIV(Env/gag/nef) vectors at wks 0 & 13 and intramuscular boosting with SIV gp120 in alum at wks 26 & 38. Lymph nodes (LNs) were collected pre-vaccination and 3–4 days post-2nd prime and post-2nd boost. Vaginal washes were obtained prior to and 3 wks post-immunizations. GC TFH and B cell frequencies positively correlated post-2nd prime (p=0.04; r=0.6) suggesting an effect of early TFH cells in GCs. GC SIV-specific TFH cells were significantly enhanced post-2nd boost (p=0.01). BCL6 upregulation was also seen in GC-TFH cells at this time, confirming the GC phenotype of TFH cells. GC SIV-specific memory B cell levels were higher post-2nd boost compared to post-prime (p=0.03) indicating efficient SIV-specific B cell generation. GC B cells post-2nd prime and boost strongly associated with SIV-specific IgG levels in vaginal washes (p=0.03, r=0.7; p=0.002, r=0.8). GC centrocytes are critical for long-lasting Ab secreting cells. GC centrocytes post 2nd prime and boost tended to correlate with vaginal wash SIV-specific IgG levels (p=0.06, p=0.05; r=0.6 for both). Overall, our vaccine regimen elicited GC T and B cell responses that supported SIV-specific humoral immunity in the FGT suggesting further development of replicating mucosal Ad-vaccines is warranted for females as well as males.
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