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一种有效的Th2型记忆反应继发于CD8 +淋巴细胞驱动及嗜酸性粒细胞介导的对经基因工程改造以释放IL-4的自发性小鼠乳腺腺癌的排斥反应。

An efficient Th2-type memory follows CD8+ lymphocyte-driven and eosinophil-mediated rejection of a spontaneous mouse mammary adenocarcinoma engineered to release IL-4.

作者信息

Pericle F, Giovarelli M, Colombo M P, Ferrari G, Musiani P, Modesti A, Cavallo F, Di Pierro F, Novelli F, Forni G

机构信息

CNR Center for Immunogenetics and Experimental Oncology University of Turin, Italy.

出版信息

J Immunol. 1994 Dec 15;153(12):5659-73.

PMID:7989764
Abstract

A retroviral infection was used to introduce the cDNA coding for mouse IL-4 into the parental cells of a spontaneous adenocarcinoma of BALB/c mice (TS/A-pc). Four clones releasing between 5 to 40 U of IL-4 (10(5) cells) in 48 h culture were selected. The secretion of IL-4 does not affect their in vitro growth, whereas their ability to form tumor in vivo inversely correlates with the amount of IL-4 secreted. Although morphologic observation suggested that the rejection of clone D5.40 cells (releasing 40 U of IL-4) depends on eosinophil cytolysis, lymphocyte depletion experiments showed that this required CD8+ lymphocyte guidance. Mice that had rejected D5.40 cells were immune to a subsequent challenge with TS/A-pc. This memory rests on the interaction between noncytotoxic lymphocytes, eosinophils, and IgG1 and IgE anti-TS/A Abs. Comparison of these memory mechanisms with those elicited by IL-2 gene-transduced TS/A cells shows that the kind of cytokine released by the tumor cells determines the type of response. This Th2 memory seems to be more efficient in protecting against a subsequent challenge of TS/A-pc than the Th1-type memory elicited by IL-2 gene-transduced TS/A cells.

摘要

利用逆转录病毒感染将编码小鼠白细胞介素4(IL-4)的cDNA导入BALB/c小鼠自发性腺癌(TS/A-pc)的亲代细胞中。挑选出4个克隆,在48小时培养中每10^5个细胞释放5至40单位的IL-4。IL-4的分泌不影响它们的体外生长,而它们在体内形成肿瘤的能力与分泌的IL-4量呈负相关。虽然形态学观察表明克隆D5.40细胞(释放40单位IL-4)的排斥依赖于嗜酸性粒细胞溶解,但淋巴细胞清除实验表明这需要CD8+淋巴细胞的引导。已排斥D5.40细胞的小鼠对随后的TS/A-pc攻击具有免疫力。这种记忆依赖于非细胞毒性淋巴细胞、嗜酸性粒细胞以及IgG1和IgE抗TS/A抗体之间的相互作用。将这些记忆机制与IL-2基因转导的TS/A细胞引发的记忆机制进行比较表明,肿瘤细胞释放的细胞因子类型决定了反应类型。这种Th2记忆在保护机体免受随后的TS/A-pc攻击方面似乎比IL-2基因转导的TS/A细胞引发的Th1型记忆更有效。

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An efficient Th2-type memory follows CD8+ lymphocyte-driven and eosinophil-mediated rejection of a spontaneous mouse mammary adenocarcinoma engineered to release IL-4.一种有效的Th2型记忆反应继发于CD8 +淋巴细胞驱动及嗜酸性粒细胞介导的对经基因工程改造以释放IL-4的自发性小鼠乳腺腺癌的排斥反应。
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