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针对B7转染的非转移性肿瘤的细胞毒性T淋巴细胞成熟:B7在肿瘤和宿主抗原呈递细胞上的共刺激作用起关键作用。

Maturation of cytotoxic T lymphocytes against a B7-transfected nonmetastatic tumor: a critical role for costimulation by B7 on both tumor and host antigen-presenting cells.

作者信息

Maric M, Zheng P, Sarma S, Guo Y, Liu Y

机构信息

Department of Pathology and Kaplan Comprehensive Cancer Center, New York, New York 10016, USA.

出版信息

Cancer Res. 1998 Aug 1;58(15):3376-84.

PMID:9699669
Abstract

It is generally believed that CTLs mature in lymphoid organs and then migrate into target tissues to execute their effector functions. This notion, however, is based on studies using antigens that are readily localized in the lymphoid tissue, such as viruses and allogeneic transplants. The site for maturation of CTLs for nonmetastatic tumors has not been determined. Because nonmetastatic tumor cells are not localized in lymphoid tissues, it is questionable whether such tumors are efficient inducers of antitumor CTLs. Here, we report that a nonmetastatic B7+ plasmacytoma induces strong effector CTL response. Thus, it is possible to induce CTLs with strong ex vivo CTL activity in the absence of tumor metastasis. In addition, a detailed kinetic analysis of CD8 T cell recruitment and maturation of CTL activity suggests that antitumor CTLs mature within the tumor rather than in the lymphoid tissues. Interestingly, despite B7-1 expression on tumor cells, induction of effector CTLs also requires costimulation by B7 on host antigen-presenting cells. These findings have important implications for tumor gene therapy and for understanding the mechanism of CTL induction in vivo.

摘要

一般认为,细胞毒性T淋巴细胞(CTL)在淋巴器官中成熟,然后迁移到靶组织中执行其效应功能。然而,这一观点是基于使用易于定位于淋巴组织中的抗原(如病毒和同种异体移植)的研究得出的。非转移性肿瘤的CTL成熟位点尚未确定。由于非转移性肿瘤细胞并不定位于淋巴组织中,因此这类肿瘤是否是抗肿瘤CTL的有效诱导剂值得怀疑。在此,我们报告一种非转移性B7 +浆细胞瘤可诱导强烈的效应CTL反应。因此,在没有肿瘤转移的情况下,有可能诱导出具有强大体外CTL活性的CTL。此外,对CD8 T细胞募集和CTL活性成熟的详细动力学分析表明,抗肿瘤CTL在肿瘤内而非淋巴组织中成熟。有趣的是,尽管肿瘤细胞上表达B7 - 1,但效应CTL的诱导也需要宿主抗原呈递细胞上的B7进行共刺激。这些发现对肿瘤基因治疗以及理解体内CTL诱导机制具有重要意义。

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