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与TiγA+外周血淋巴细胞相比,克隆的CD3+T细胞受体α/β-TiγA-外周血淋巴细胞:γ/δ受体的结构差异和功能异质性。

Cloned CD3+ TcR alpha/beta- Ti gamma A- peripheral blood lymphocytes compared to the Ti gamma A+ counterparts: structural differences of the gamma/delta receptor and functional heterogeneity.

作者信息

Jitsukawa S, Triebel F, Faure F, Miossec C, Hercend T

机构信息

Laboratoire d'Immunologie Cellulaire, Département de Biologie Clinique, Institut Gustave-Roussy, Villejuif, France.

出版信息

Eur J Immunol. 1988 Nov;18(11):1671-9. doi: 10.1002/eji.1830181104.

Abstract

We have assessed the organization of T cell gamma rearranging genes (TRG) in circulating TcR gamma/delta+ lymphocytes which do not express V gamma 9-encoded Ti gamma A+ gamma chain. Following purification of the minor TcR gamma/delta+ Ti gamma A- fraction, cloned cell lines were developed from peripheral blood of 5 individuals. Out of the 26 clones studied, only 3 TcR gamma/delta+ Ti gamma A- cells were found to express a disulfide-linked C1-encoded gamma chain. The remaining 23 Ti gamma A- clones with a C2-encoded nondisulfide-linked receptor were found to display rearrangements of various V genes to J2 segments on both chromosomes; there was no predominance of a unique rearrangement even though the TRG-V3 and -V4 genes belonging to subgroup I were frequently employed. Together, these findings further strengthen the hypothesis that lymphocytes with a C gamma 1 encoded chain are produced earlier in T cell ontogeny than the C gamma 2 counterparts. The "non-major histocompatibility complex (MHC) requiring" (i.e., "natural killer-like") cytotoxicity mediated by many TcR gamma/delta+ Ti gamma A- cells appeared to be very low as compared to that of Ti gamma A+ clones. Yet, treatment by the OKT3 monoclonal antibody revealed a strong lytic potential in the Ti gamma A- lymphocytes with little, if any, natural killer-like activity. Thus, with respect to the latter function, a substantial heterogeneity is found in cells expressing distinct gamma chains. In an attempt to characterize undefined specificities of Ti gamma A- lymphocytes, they were screened against a panel of Epstein-Barr virus-transformed B cell lines homozygous for HLA-DR1 to DR10 determinants; one of the clones was found to recognize DR7. In light of reports from other groups describing class I-related specificities, it is apparent that TcR gamma/delta+ lymphocytes are able, like the TcR alpha/beta+, to recognize and kill target cells through either an MHC-dependent (with involvement of either class I or class II gene products) or a non-MHC-requiring pathway.

摘要

我们评估了循环中不表达Vγ9编码的TiγA⁺γ链的TcRγ/δ⁺淋巴细胞中T细胞γ重排基因(TRG)的组织情况。在纯化出少量TcRγ/δ⁺TiγA⁻组分后,从5名个体的外周血中建立了克隆细胞系。在所研究的26个克隆中,仅发现3个TcRγ/δ⁺TiγA⁻细胞表达二硫键连接的C1编码γ链。其余23个具有C2编码的非二硫键连接受体的TiγA⁻克隆在两条染色体上均显示出各种V基因与J2片段的重排;即使属于I亚组的TRG - V3和 - V4基因被频繁使用,也没有一种独特重排占主导地位。总之,这些发现进一步强化了这样一种假说,即具有Cγ1编码链的淋巴细胞在T细胞个体发育中比Cγ2对应物产生得更早。与TiγA⁺克隆相比,许多TcRγ/δ⁺TiγA⁻细胞介导的“非主要组织相容性复合体(MHC)依赖性”(即“自然杀伤样”)细胞毒性似乎非常低。然而,用OKT3单克隆抗体处理后发现,TiγA⁻淋巴细胞具有很强的裂解潜力,几乎没有自然杀伤样活性。因此,就后一种功能而言,在表达不同γ链的细胞中发现了很大的异质性。为了表征TiγA⁻淋巴细胞未明确的特异性,用一组针对HLA - DR1至DR10决定簇纯合的爱泼斯坦 - 巴尔病毒转化B细胞系对它们进行筛选;发现其中一个克隆识别DR7。根据其他小组描述I类相关特异性的报告,很明显,TcRγ/δ⁺淋巴细胞与TcRα/β⁺一样,能够通过MHC依赖性途径(涉及I类或II类基因产物)或非MHC依赖性途径识别并杀伤靶细胞。

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