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通过克隆的同种特异性人Th细胞扩增改变的自身反应性细胞溶解性T淋巴细胞反应。

Amplification of altered self-reactive cytolytic T lymphocyte responses by cloned, allospecific human Th cells.

作者信息

Friedman S M, Green A, Russo C, Posnett D N, Diffley D, Crow M K

机构信息

Department of Medicine, Hospital for Special Surgery, New York, New York 10021.

出版信息

J Clin Invest. 1988 Nov;82(5):1722-30. doi: 10.1172/JCI113786.

Abstract

The effect of a cloned allospecific human Th cell, termed 86, on the in vitro generation of altered self-reactive cytolytic T lymphocytes (CTL) was investigated. Utilizing the induction of hapten altered self-reactive CTL as a model for virus or tumor-specific cell-mediated immunity, we determined that the presence of small numbers of clone 86 cells markedly amplified the generation of hapten altered self-reactive CTL. The killer cells induced belong to the CD4-, CD8+ subset, are specific for the hapten-modified autologous stimulator cells present in culture, and are MHC class I restricted. The CTL induced under these culture conditions are readily expanded in the presence of IL-2 with maintenance of efficient and specific altered self-killing. Of interest, clone 86 cells preferentially enhance the growth of CD8+ T cells and selectively amplify altered self-cytolysis but not NK cell activity. Although in vitro clone 86 cells mediate help for CTL generation via the production of lymphokines (IL-4 but little IL-2), one can envision immunotherapeutic strategies for human disease that involve the adoptive transfer of Th cells functionally analogous to clone 86.

摘要

研究了一种名为86的克隆同种异体人Th细胞对体外产生改变的自身反应性细胞毒性T淋巴细胞(CTL)的影响。利用半抗原诱导的改变的自身反应性CTL作为病毒或肿瘤特异性细胞介导免疫的模型,我们确定少量克隆86细胞的存在显著增强了半抗原改变的自身反应性CTL的产生。诱导产生的杀伤细胞属于CD4-、CD8+亚群,对培养物中存在的半抗原修饰的自体刺激细胞具有特异性,并且受MHC I类限制。在这些培养条件下诱导的CTL在IL-2存在下易于扩增,并维持高效和特异性的改变的自身杀伤作用。有趣的是,克隆86细胞优先促进CD8+T细胞的生长,并选择性地增强改变的自身细胞溶解作用,但不增强NK细胞活性。虽然体外克隆86细胞通过产生淋巴因子(IL-4但几乎不产生IL-2)介导对CTL产生的辅助作用,但人们可以设想针对人类疾病的免疫治疗策略,其中涉及过继转移功能类似于克隆86的Th细胞。

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