Gold R, Giegerich G, Hartung H P, Toyka K V
Department of Neurology, Julius-Maximilians-Universität, Würzburg, Germany.
Proc Natl Acad Sci U S A. 1995 Jun 20;92(13):5850-4. doi: 10.1073/pnas.92.13.5850.
Predominant usage of V beta 8.2 gene segments, encoding a T-cell receptor (TCR) beta chain variable region, has been reported for pathogenic Lewis rat T cells reactive to myelin basic protein (MBP). However, up to 75% of the alpha/beta T cells in a panel of MBP-specific T-cell lines did not display TCR V beta 8.2, V beta 8.5, V beta 10, or V beta 16 elements. To further investigate TCR usage, we sorted the T-cell lines for V beta 8.2- and V beta 10-positive T cells or depleted the lines of cells with these TCRs. V beta 8.2-positive T cells and one of the depleted T-cell lines strongly reacted against the MBP peptide MBP-(68-88). The depleted T-cell line caused marked experimental autoimmune encephalomyelitis (EAE) even in Lewis rats in which endogenous V beta 8.2-positive T cells had been eliminated by neonatal treatment with anti-V beta 8.2 monoclonal antibodies. T-cell hybridomas generated from this line predominantly used V beta 3 TCR genes coexpressed with TCR V alpha 2 transcripts, which were also used by V beta 8.2-positive T cells. Furthermore, V beta 10-positive T cells reactive to MBP-(44-67) were encephalitogenic when injected immediately after positive selection. After induction of EAE by sorted V beta 8.2- or V beta 10-positive T-cell lines, immunocytochemical analysis of the spinal cord tissue showed a predominance of the injected TCR or of nontypable alpha/beta T cells after injection of the depleted line. Our results demonstrate heterogeneity of TCR beta-chain usage even for a single autoantigen in an inbred strain. Moreover, V beta 8.2-positive T cells are not essential for the induction and progression of adoptive-transfer EAE.
据报道,对髓鞘碱性蛋白(MBP)产生反应的致病性Lewis大鼠T细胞主要使用编码T细胞受体(TCR)β链可变区的Vβ8.2基因片段。然而,在一组MBP特异性T细胞系中,高达75%的α/βT细胞未显示TCR Vβ8.2、Vβ8.5、Vβ10或Vβ16元件。为了进一步研究TCR的使用情况,我们对T细胞系进行分选,以获得Vβ8.2阳性和Vβ10阳性T细胞,或去除具有这些TCR的细胞系中的细胞。Vβ8.2阳性T细胞和其中一个去除细胞后的T细胞系对MBP肽MBP-(68-88)有强烈反应。即使在通过用抗Vβ8.皮8.2单克隆抗体进行新生期治疗已消除内源性Vβ8.2阳性T细胞的Lewis大鼠中,去除细胞后的T细胞系仍能引起明显的实验性自身免疫性脑脊髓炎(EAE)。从该细胞系产生的T细胞杂交瘤主要使用与TCR Vα2转录本共表达的Vβ3 TCR基因,Vβ8.2阳性T细胞也使用这些基因。此外,对MBP-(44-67)产生反应的Vβ10阳性T细胞在阳性选择后立即注射时具有致脑炎作用。在用分选的Vβ8.2或Vβ10阳性T细胞系诱导EAE后,对脊髓组织进行免疫细胞化学分析显示,注射后脊髓组织中主要是注射的TCR或无法分型的α/βT细胞。我们的结果表明,即使对于近交系中的单一自身抗原,TCRβ链的使用也存在异质性。此外,Vβ8.2阳性T细胞对于过继转移EAE的诱导和进展并非必不可少。
