B cell activation during HIV-1 infection. II. Cell-to-cell interactions and cytokine requirement.

A Amadori, R Zamarchi, ML Veronese… - … (Baltimore, Md.: 1950 …, 1991 - journals.aai.org
A Amadori, R Zamarchi, ML Veronese, M Panozzo, A Barelli, A Borri, M Sironi, F Colotta
Journal of immunology (Baltimore, Md.: 1950), 1991journals.aai.org
This study examined the mechanisms underlying the intense activation of HIV-1-specific B
cells observed in peripheral blood of HIV-1-infected subjects. Spontaneous in vitro synthesis
of anti-HIV-1 antibodies, as well as total Ig production, were dramatically reduced by
accessory cell, but not T cell removal. This fall was counteracted by addition of rIL-6, but not
other cytokines, to monocyte-depleted cultures; moreover, antisera against IL-6 suppressed
spontaneous anti-HIV-1 antibody synthesis in a dose-dependent manner. Although IL-6 …
Abstract
This study examined the mechanisms underlying the intense activation of HIV-1-specific B cells observed in peripheral blood of HIV-1-infected subjects. Spontaneous in vitro synthesis of anti-HIV-1 antibodies, as well as total Ig production, were dramatically reduced by accessory cell, but not T cell removal. This fall was counteracted by addition of rIL-6, but not other cytokines, to monocyte-depleted cultures; moreover, antisera against IL-6 suppressed spontaneous anti-HIV-1 antibody synthesis in a dose-dependent manner. Although IL-6 apparently sustained HIV-1-specific B cell activation, no increase in serum IL-6 levels was observed; PBMC from seropositive subjects did not produce increased amounts of IL-6 in vitro, compared to seronegative controls, both spontaneously and in the presence of LPS stimulation; finally, no constitutive expression of IL-6 gene could be documented in freshly isolated PBMC. These findings indicate that IL-6 may play a central role in HIV-1-specific B cell activation in seropositive patients, and further stress the importance of this cytokine during HIV-1 infection.
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