Affiliation:
1. Centro Trasfusionale, O.C. Castelfranco Veneto, Treviso, and Istituto di Medicina Clinica dell'Università di Padova, Clinica Medica I, Padova, Italy
Abstract
SUMMARY
In this study we investigated the distribution of the S6F1 antigen, an epitope of the lymphocyte function-associated antigen, on CD8+ T lymphocytes in a series of 15 HIV-1+ and 20 HIV-1- haemophiliac patients. MoAbs recognizing the S6K1 antigen have been claimed to distinguish between killer electors (brightly S6F1+ stained) and suppressor cells (dimly S6K1+ stained) within the CD8+ lymphoid population. In addition, we tried to find a correlation between the spontaneous in vitro immunoglobulin synthesis from patients' peripheral blood lymphocytes and the pattern of S6F1 expression. Although the total number of double-positive CD8+/S6F1+ cells was similar in both HIV-1+ and HIV-1- haemophiliac patients, a significant increase in the CD8+/S6F1+ population bright versus dim was documented in HIV-1-infected with respect to HIV-1 haemophiliacs (bright/dim ratio 3·97 ± 0·61 versus 0·75 ± 0·1, respectively, P < 0·005). This finding was correlated to a significant increase in spontaneous in vitro immunoglobulin production in HIV-1+ subjects compared with control haemophiliacs (P < 0·005). Purified CD8+ lymphocytes from HIV-1+ subjects showed a reduced suppressor activity on mitogen-induced immunoglobulin production. Taken together, these data suggest that HIV-1 infection favours the generation of CD8+/S6F1+ bright cells with putative cytotoxic-associated function, leading to a progressive reduction in the number of CD8+/S6F1+ dim suppressor lymphocytes. This phenomenon may contribute to the polyclonal hypergammaglobulinaemia present in HIV-1+ haemophiliac patients.
Publisher
Oxford University Press (OUP)
Subject
Immunology,Immunology and Allergy
Cited by
5 articles.
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