The humoral immune response after acute infection with HIV-1 is delayed and ineffective. The HIV-1 envelope protein gp120 binds to and signals through integrin a4b7 on T cells. We found that gp120 also bound to and signaled through a4b7 on naive B cells, which resulted in an abortive proliferative response. In primary B cells, signaling by gp120 through a4b7 resulted in increased expression of the immunosuppressive cytokine TGF-b1 and FcRL4, an inhibitory receptor expressed on B cells. Coculture of B cells with HIV-1-infected autologous CD4+ T cells also increased the expression of FcRL4 by B cells. Our findings indicated that in addition to mediating chronic activation of the immune system, viral proteins contributed directly to HIV-1- associated B cell dysfunction. Our studies identify a mechanism whereby the virus may subvert the early HIV-1-specific humoral immune response.
The HIV-1 envelope protein gp120 impairs B cell proliferation by inducing TGF-β1 production and FcRL4 expression
DAVID, Antonio;
2013-01-01
Abstract
The humoral immune response after acute infection with HIV-1 is delayed and ineffective. The HIV-1 envelope protein gp120 binds to and signals through integrin a4b7 on T cells. We found that gp120 also bound to and signaled through a4b7 on naive B cells, which resulted in an abortive proliferative response. In primary B cells, signaling by gp120 through a4b7 resulted in increased expression of the immunosuppressive cytokine TGF-b1 and FcRL4, an inhibitory receptor expressed on B cells. Coculture of B cells with HIV-1-infected autologous CD4+ T cells also increased the expression of FcRL4 by B cells. Our findings indicated that in addition to mediating chronic activation of the immune system, viral proteins contributed directly to HIV-1- associated B cell dysfunction. Our studies identify a mechanism whereby the virus may subvert the early HIV-1-specific humoral immune response.Pubblicazioni consigliate
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