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牛分枝杆菌卡介苗DNA组分的抗肿瘤活性。II. 对各种同基因小鼠肿瘤的影响。

Antitumor activity of the DNA fraction from Mycobacterium bovis BCG. II. Effects on various syngeneic mouse tumors.

作者信息

Shimada S, Yano O, Inoue H, Kuramoto E, Fukuda T, Yamamoto H, Kataoka T, Tokunaga T

出版信息

J Natl Cancer Inst. 1985 Mar;74(3):681-8.

PMID:3856070
Abstract

MY-1, a fraction extracted from BCG and composed of 70.0% DNA and 28.0% RNA, was examined for its antitumor activity against 9 different syngeneic mouse tumors. Tumor regression was induced in almost all of the mice bearing any of five kinds of solid tumors by repeated intralesional injections of 100 micrograms MY-1. When cells of some tumors were inoculated intradermally together with MY-1, tumor growth was suppressed, lung metastases were inhibited, and the survival times of mice bearing 1 of 3 leukemic tumors were prolonged. Repeated sc injections with MY-1 in sites remote from tumor cell inoculation or repeated iv injections were more or less effective against three kinds of solid tumors. Mice inoculated with Lewis lung carcinoma cells in a hind footpad and whose legs were amputated 9 days later were given iv or sc injections of MY-1 every other day (8 times in total), resulting in substantial prolongation of survival. No direct cytotoxicity of MY-1 for these tumors could be shown in three kinds of experiments, which indicates that the antitumor mechanism of MY-1 is host mediated. MY-1 was equally effective in mice with or without presensitization with BCG, whereas BCG was much more effective in BCG-sensitized mice. This finding suggests that a delayed-type hypersensitivity reaction elicited by BCG protein is not required for the antitumor activity of MY-1.

摘要

MY-1是一种从卡介苗中提取的组分,由70.0%的DNA和28.0%的RNA组成,对9种不同的同基因小鼠肿瘤的抗肿瘤活性进行了检测。通过在瘤内反复注射100微克MY-1,几乎所有患有五种实体瘤中任何一种的小鼠都出现了肿瘤消退。当将某些肿瘤的细胞与MY-1一起皮内接种时,肿瘤生长受到抑制,肺转移受到抑制,并且患有三种白血病肿瘤中一种的小鼠的存活时间延长。在远离肿瘤细胞接种部位反复皮下注射MY-1或反复静脉注射对三种实体瘤或多或少有效。在后足垫接种Lewis肺癌细胞且9天后截肢腿部的小鼠每隔一天接受静脉或皮下注射MY-1(共8次),导致存活时间显著延长。在三种实验中均未显示出MY-1对这些肿瘤有直接细胞毒性,这表明MY-1的抗肿瘤机制是由宿主介导的。MY-1在有或没有卡介苗预致敏的小鼠中同样有效,而卡介苗在卡介苗致敏的小鼠中更有效。这一发现表明,MY-1的抗肿瘤活性不需要卡介苗蛋白引发的迟发型超敏反应。

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