| Abstract: |
Abstract: The major histocompatibility complex (MHC) class II antigens (Ags) are known to carry the major stimulating determinants of the primary mixed lymphocyte reactions (MLR). We investigated the mechanism of generating HLA class I‐directed alloreactive T‐cells in primary MLR. With the use of class II‐deficient EBV‐transformed B‐lymphoblastoid cell lines (B‐LCLs) derived from patients with bare lymphocyte syndrome (BLS), we have demonstrated in the present study that class I disparity alone can trigger primary MLR in the absence of exogenous IL‐2. The CD8+ T cells were primary MLR‐responsive cells, and the CD4+ T cells seem to play no role in primary MLR when class II alloantigens are not involved in stimulation. Addition of autologous macrophages did not influence the primary MLR response. The primary MLR was completely blocked by anti‐class I or anti‐CD8 antibodies but not by anti‐class II or anti‐CD4 antibodies. The MLC‐generated CD8+ T cells exhibited cytolytic activity as well as proliferative responses. The proliferative response of the CD8+ T cells was specifically directed against class I antigens, demonstrated by proliferatlire assays; and the helper‐independent CD8+. T cells were generated only when the activation of CD4+ T cells did not occur. This observation suggests that functional recruitment of T‐cell receptor (TCR) repertoire is under active regulation, and the suppression of CD8+ T‐cell helper recruitment appears to be dictated by the CD4+ T‐cell subset. Further analysis of the primed T‐cell specificities showed that alloreactivity of the CD8+ T cells was mostly accounted for by the HLA‐B Ags. The higher alloreactivity against the HLA‐B Ags may probably be due to the high frequency of HLA‐B‐directed T‐cell clones, and the high frequency is probably due to their higher sequence variability in HLA‐B than in the HLA‐A and HLA‐C Ags. Copyright © 1990, Wiley Blackwell. All rights reserved |
| Keywords: |
human cell; cd8 antigen; cell line; b lymphocyte; b-lymphocytes; t lymphocyte receptor; lymphocyte activation; lymphocyte culture test, mixed; cell culture; t-lymphocytes, cytotoxic; histocompatibility antigens class i; cytotoxicity, immunologic; t-lymphocytes, helper-inducer; hla a antigen; hla b antigen; hla c antigen; hla-d antigens; alloantigen; hla antigens; t lymphocyte activation; mixed lymphocyte reaction; clone; human; priority journal; article; support, u.s. gov't, p.h.s.
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