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A specific T-cell subset with CD4+/CD38- markers derived from HIV-1 carriers induces apoptosis in healthy donor-derived T-lymphocytes.

作者信息

Kameoka M, Auwanit W, Suzuki S, Horikoshi H, Khlai-Khlam N, Meguro T, Yamada K, Tanaka Y, Yoshihara K, Luftig R B, Ikuta K

机构信息

Section of Serology, Institute of Immunological Science, Hokkaido University, Sapporo, Japan.

出版信息

Virus Res. 1998 Jul;56(1):115-22. doi: 10.1016/s0168-1702(98)00052-5.

Abstract

Apoptosis is an important mechanism of human immunodeficiency virus type 1 (HIV-1)-induced T-cell depletion. Our recent findings revealed mitogenic stimulation-dependent apoptosis induction in healthy donor-derived peripheral blood T-lymphocytes after adsorption with defective HIV-1 particles through acquirement by a subset of CD4+/CD38- cells of specific killer function. Based on these in vitro observations, we have extended the significance of this killing activity of CD4+/CD38- cells directly derived from HIV-1 carriers. The CD4+/CD38- cells from HIV-1-positive individuals showed significantly higher cell-killing activities than those from HIV-1-negative donors by co-culture with allogeneic resting T-cells after mitogenic stimulation. Furthermore, most of the samples induced apoptosis in a Fas-dependent manner. Thus, it is suggested that HIV-1 infection-related apoptosis is triggered by inappropriate activation of a certain resting T-cell subset, presumably due to adsorption with HIV-1 particles.

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