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干扰素对可移植大鼠结肠腺癌的治疗:肿瘤部位的重要性。

Interferon treatment of a transplantable rat colon adenocarcinoma: importance of tumor site.

作者信息

Marquet R L, Westbroek D L, Jeekel J

出版信息

Int J Cancer. 1984 May 15;33(5):689-92. doi: 10.1002/ijc.2910330521.

Abstract

The effect of partially purified rat interferon ( RIFN ) was evaluated in CC531 colon tumor-bearing rats. Tumor CC531 is a DMH-induced, transplantable adenocarcinoma exhibiting weak immunogenicity. When small tumor fragments were implanted under the renal capsule, daily treatment with RIFN for 5 days led to a highly significant (p less than 0.001) inhibition of tumor growth, measured 7 days after implantation. Cyclic treatment with RIFN (10(5) units/kg/day, for 7 days in weeks 2, 4, 6 and 8) significantly retarded the development of artificial lung metastases, induced by intravenous (i.v.) injection of 5 X 10(5) colon tumor cells. The median survival time was 177 days in the RIFN group as compared to 116 days in the control group. Three of eight animals treated with RIFN showed no sign of lung metastases when they were killed 250 days after tumor cell injection. The same cyclic RIFN treatment which was effective in the lung metastases model had no influence on the growth of liver metastases evoked by the intraportal injection of 5 X 10(5) tumor cells. Laparotomy performed at days 30 and 50 after inoculation revealed equal numbers of liver metastases in the RIFN -treated group and the control group. The mean survival times obtained in the two groups were 96 +/- 20 days and 108 +/- 14 days, respectively (0.05 less than p less than 0.10). The results indicate that (1) there is no inherent resistance of this solid tumor to RIFN therapy and (2) the effect of RIFN treatment is determined by the site of tumor development. The finding that the liver can provide a protective environment against tumor immunity may have important clinical implications.

摘要

在携带CC531结肠肿瘤的大鼠中评估了部分纯化的大鼠干扰素(RIFN)的作用。肿瘤CC531是一种由二甲基肼诱导的、可移植的腺癌,免疫原性较弱。当将小肿瘤碎片植入肾包膜下时,在植入后7天测量,每天用RIFN治疗5天导致肿瘤生长受到高度显著抑制(p<0.001)。用RIFN进行循环治疗(10⁵单位/千克/天,在第2、4、6和8周各治疗7天)显著延缓了通过静脉注射5×10⁵个结肠肿瘤细胞诱导的人工肺转移的发展。RIFN组的中位生存时间为177天,而对照组为116天。在肿瘤细胞注射后250天处死的8只接受RIFN治疗的动物中,有3只没有肺转移的迹象。在肺转移模型中有效的相同循环RIFN治疗对门静脉注射5×10⁵个肿瘤细胞引起的肝转移生长没有影响。接种后第30天和第50天进行的剖腹手术显示,RIFN治疗组和对照组的肝转移数量相等。两组的平均生存时间分别为96±20天和108±14天(0.05<p<0.10)。结果表明:(1)这种实体瘤对RIFN治疗没有内在抗性;(2)RIFN治疗的效果取决于肿瘤发展的部位。肝脏可以提供一个对抗肿瘤免疫的保护环境这一发现可能具有重要的临床意义。

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