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针对低免疫原性肿瘤抗原的Th1和Th2细胞克隆在体内启动CD8 + T细胞依赖性肿瘤根除。

Th1 and Th2 cell clones to a poorly immunogenic tumor antigen initiate CD8+ T cell-dependent tumor eradication in vivo.

作者信息

Fallarino F, Grohmann U, Bianchi R, Vacca Carmine, Fioretti M C, Puccetti P

机构信息

Department of Experimental Medicine, University of Perugia, Perugia, Italy.

出版信息

J Immunol. 2000 Nov 15;165(10):5495-501. doi: 10.4049/jimmunol.165.10.5495.

Abstract

Although CD8(+) T cells play a central role as immune effectors, CD4(+) T cells act to control the activation and persistence of the CD8(+) T cell response in autoimmune disease, antiviral immunity, and experimental systems with immunogenic model tumor Ag. However, little information is available on the effects of CD4(+) T cells on the function of endogenous CD8(+) T lymphocytes recognizing authentic tumor rejection Ag with limited immunogenicity. We report here that the prophylactic or postchallenge administration of T helper Th1-type and Th2-type CD4(+) clones specific for an unmutated rejection Ag (murine P815AB, resembling tumor-specific shared Ag in humans) leads to the induction of P815AB-specific reactivity in vivo and concomitant tumor destruction, with quantitative rather than qualitative differences characterizing the antitumor activity of Th1 vs Th2 cells. Because the transferred CD4(+) cells lacked direct antitumor activity in vitro and required the de novo generation of P815AB-specific CD8(+) T cells in vivo, these findings suggest that CD4(+) lymphocytes can enhance the ability of host APC to initiate an endogenous CD8(+) T cell response to authentic, poorly immunogenic tumor rejection Ag.

摘要

尽管CD8(+) T细胞作为免疫效应细胞发挥核心作用,但在自身免疫性疾病、抗病毒免疫以及具有免疫原性模型肿瘤抗原的实验系统中,CD4(+) T细胞可调控CD8(+) T细胞反应的激活和持续存在。然而,关于CD4(+) T细胞对识别具有有限免疫原性的真实肿瘤排斥抗原的内源性CD8(+) T淋巴细胞功能的影响,目前所知甚少。我们在此报告,对未突变的排斥抗原(小鼠P815AB,类似于人类肿瘤特异性共享抗原)具有特异性的辅助性T细胞Th1型和Th2型CD4(+)克隆的预防性或攻毒后给药,可在体内诱导P815AB特异性反应并伴随肿瘤破坏,Th1细胞与Th2细胞的抗肿瘤活性在数量而非质量上存在差异。由于转移的CD4(+)细胞在体外缺乏直接抗肿瘤活性,且在体内需要重新产生P815AB特异性CD8(+) T细胞,这些发现表明CD4(+)淋巴细胞可增强宿主抗原呈递细胞启动针对真实、免疫原性较差的肿瘤排斥抗原的内源性CD8(+) T细胞反应的能力。

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