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联合中枢神经系统抑制剂对大鼠腹水肝癌的抗肿瘤作用。

Combination antitumor effect with central nervous system depressants on rat ascites hepatomas.

作者信息

Koshiura R, Miyamoto K, Sanae F

出版信息

Gan. 1980 Feb;71(1):45-51.

PMID:7380136
Abstract

Combined effect of twenty-one central nervous system depressants with several antitumor agents was studied in the in vitro and in vivo experimental systems, using rat ascites hepatoma call lines, AH13 and AH44, sensitive and insensitive to alkylating agents, respectively. Reserpine remarkably enhanced the cytotoxic effect of 1-(gamma-chloropropyl)-2-chloromethylpiperidine hydrobromide (CAP-2) both on AH13 and AH44 cells. In the in vivo combined experiments, reserpine also synergistically enhanced the life-prolonging effect of CAP-2 on AH13-bearing rats and, although CAP-2 was not potent on the prolongation of life span of AH44-bearing rats and reserpine was also ineffective at the doses examined, the life span of tumor-bearing rats receiving the combined administration was apparently prolonged compared with control groups. Thus, there was a parallelism between in vitro and in vivo experiments. These findings suggested that the antitumor-enhancing effect of reserpine might be due to the direct action on the tumor cells, and a possible mechanism that reserpine inhibited the DNA damage-repairing activity of the cells was contradictory. Other mechanisms are also discussed.

摘要

在体外和体内实验系统中,使用对烷化剂敏感和不敏感的大鼠腹水肝癌细胞系AH13和AH44,研究了21种中枢神经系统抑制剂与几种抗肿瘤药物的联合作用。利血平显著增强了1-(γ-氯丙基)-2-氯甲基哌啶氢溴酸盐(CAP-2)对AH13和AH44细胞的细胞毒性作用。在体内联合实验中,利血平还协同增强了CAP-2对荷AH13大鼠的延长寿命作用,尽管CAP-2对荷AH44大鼠的寿命延长作用不强,且在所检测剂量下利血平也无效,但与对照组相比,联合给药的荷瘤大鼠的寿命明显延长。因此,体外和体内实验之间存在平行关系。这些发现表明,利血平的抗肿瘤增强作用可能是由于其对肿瘤细胞的直接作用,而利血平抑制细胞DNA损伤修复活性这一可能机制存在矛盾。还讨论了其他机制。

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