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Matrix Metalloproteinase Inhibitor Marimastat Decreases Peritoneal Spread of Gastric Carcinoma in Nude Mice

机译:基质金属蛋白酶抑制剂Marimastat降低裸鼠胃癌的腹膜扩散

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摘要

Marimastat, a matrix metalloproteinese inhibitor, was examined for the ability to prevent peritoneal dissemination of a human gastric cancer xenograft, TMK–1. Even with novel approaches such as molecular targeting of cancer chemotherapy, peritoneal dissemination of gastric cancer has little sensitivity to anticancer drugs, and it is impossible to inhibit its growth completely. Intraperitoneal injection of TMK–1 into nude mice at 5 × 105 cells/body resulted in carcinomatous peritonitis that mimicked clinical cases. Continuous administration of marimastat (18 mg/kg/day) from 24 h after the tumor inoculation successfully inhibited the growth of peritoneal dissemination nodules. Combined administration of marimastat (18 mg/kg/day) and mitomycin C (MMC, 2 mg/kg) showed synergistic inhibition of growth of peritoneal dissemination, being superior to MMC alone (2 mg/kg). Although marimastat alone could not increase survival tune with statistical significance, combined administration of marimastat and MMC had a survival benefit with statistical significance. The combination of marimastat and MMC increased the preventive effect on peritoneal dissemination. Marimastat seems to be a candidate for the prevention of peritoneal spread of gastric carcinoma.
机译:研究了马立马司他(一种基质金属蛋白抑制剂)的预防人类胃癌异种移植物TMK-1腹膜扩散的能力。即使采用诸如癌症化学疗法的分子靶向的新方法,胃癌的腹膜扩散对抗癌药也几乎没有敏感性,并且不可能完全抑制其生长。腹腔内以5×10 5 细胞/人腹腔注射TMK-1致裸鼠,致癌性腹膜炎与临床病例相似。肿瘤接种成功抑制腹膜播散性结节生长后24小时起连续施用马立马司他(18 mg / kg /天)。 marimastat(18 mg / kg / day)和丝裂霉素C(MMC,2 mg / kg)的联合给药显示协同抑制腹膜扩散的生长,优于单独使用MMC(2 mg / kg)。尽管仅使用马立马司他并不能增加生存率,但具有统计学意义,但联合使用马立马司他和MMC具有生存获益,具有统计意义。马立马司他和MMC的组合增加了对腹膜传播的预防作用。 Marimastat似乎是预防胃癌腹膜扩散的候选药物。

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