| Literature DB >> 30219203 |
Lindsay K Nicholson1, Harsh Pratap1, Elisabeth Bowers1, Elise Gunzburger2, Srinivasa R Bandi3, Edward M Gardner4, Brent E Palmer3, Timothy Wright5, John Kittelson6, Edward N Janoff7.
Abstract
Identifying HIV-1-associated B cell defects and responses to activation may direct interventions to circumvent their impaired antibody responses to infection and vaccines. Among 34 viremic HIV-1-infected and 20 seronegative control adults, we measured baseline frequencies and activation of B and T cell subsets, expression of activation-induced cytidine deaminase (AID), potential determinants of B cell activation in vivo and B and T cell responses in vitro. At baseline, HIV-1 infection was associated with increased IgM memory and decreased anergic cell frequencies, as well as increased activation in all 10 B cell subsets compared with controls. HIV-1 status, TFH activation, and BAFF were significant potential drivers of B cell activation. Despite high baseline activation among HIV-1-infected subjects, stimulation in vitro with combined surrogates for antigen (anti-IgM), cognate (CD40 ligand) and soluble T cell factors (IL-4) elicited comparable B cell activation, transitions from naïve to class-switched memory cells and AID expression in both groups. In summary, viremic HIV-1 infection perturbs circulating B cell subsets and activation at each stage of B cell maturation. However, that appropriate stimulation of B cells elicits effective activation and maturation provides impetus for advancing vaccine development to prevent secondary infections by circumventing early B cell defects. Published by Elsevier GmbH.Entities:
Keywords: B cells; Cellular activation; Cellular immunology; HIV; T cells
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Year: 2018 PMID: 30219203 PMCID: PMC6264910 DOI: 10.1016/j.imbio.2018.08.007
Source DB: PubMed Journal: Immunobiology ISSN: 0171-2985 Impact factor: 3.144