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针对小鼠和人类肿瘤的长期细胞系及淋巴样克隆的开发:癌症过继性免疫治疗的一种新方法。

Development of long-term cell lines and lymphoid clones reactive against murine and human tumors: a new approach to the adoptive immunotherapy of cancer.

作者信息

Rosenberg S A, Eberlein T J, Grimm E A, Lotze M T, Mazumder A, Rosenstein M

出版信息

Surgery. 1982 Aug;92(2):328-36.

PMID:6980492
Abstract

We have investigated the use of T-cell growth factor (TCGF) to isolate and grow, in long-term culture, lymphoid cells with immunologic reactivity directed against syngeneic murine and autologous human tumors. Splenocytes from mice immune to a methylcholanthrene-induced sarcoma were expanded in TCGF, both before and after in vitro mixed lymphocyte-tumor cultures, and expressed high levels of cytotoxicity for fresh syngeneic solid tumor cells. Cloned lines have been isolated with a high level of specific lysis for the immunizing tumor. Similar studies of cytotoxic reactivity to a syngeneic FBL-3 lymphoma have given rise to long-term cytotoxic cell lines growing in TCGF capable of curing mice with disseminated lymphoma in adoptive transfer studies. Exposure to TCGF, of human peripheral lymphoid cells from cancer-bearing patients, results in the development of cytotoxicity to autologous fresh tumor. We have used clonal analysis by limiting dilution techniques to isolate individual cloned cells with this autologous antitumor reactivity. Infusion to autologous cytotoxic cells expanded 10,000-fold in TCGF and labeled with 111In into three cancer patients resulted in cell localization initially to the lung and subsequently to the liver and spleen. The application of these techniques for the cloning and expansion of antitumor T-lymphoid cells in TCGF has offered a new approach to adoptive immunotherapy.

摘要

我们研究了利用T细胞生长因子(TCGF)来分离和长期培养具有针对同基因小鼠肿瘤和自体人类肿瘤免疫反应性的淋巴细胞。对甲基胆蒽诱导的肉瘤免疫的小鼠脾细胞,在体外混合淋巴细胞-肿瘤培养之前和之后,在TCGF中进行扩增,并对新鲜的同基因实体瘤细胞表现出高水平的细胞毒性。已分离出对免疫肿瘤具有高水平特异性裂解作用的克隆系。对同基因FBL-3淋巴瘤细胞毒性反应的类似研究,产生了在TCGF中生长的长期细胞毒性细胞系,在过继转移研究中能够治愈患有播散性淋巴瘤的小鼠。将荷癌患者的人外周淋巴细胞暴露于TCGF,会导致对自体新鲜肿瘤产生细胞毒性。我们已使用有限稀释技术进行克隆分析,以分离具有这种自体抗肿瘤反应性的单个克隆细胞。将在TCGF中扩增10000倍并用铟-111标记的自体细胞毒性细胞注入三名癌症患者体内,结果细胞最初定位于肺部,随后定位于肝脏和脾脏。这些在TCGF中克隆和扩增抗肿瘤T淋巴细胞的技术应用,为过继免疫疗法提供了一种新方法。

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