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生物还原细胞毒性药物SR 4233增强黄酮乙酸对小鼠癌的抗肿瘤作用

Enhancement of the antitumor effect of flavone acetic acid by the bioreductive cytotoxic drug SR 4233 in a murine carcinoma.

作者信息

Sun J R, Brown J M

机构信息

Department of Radiation Oncology, Stanford University School of Medicine, California 94305.

出版信息

Cancer Res. 1989 Oct 15;49(20):5664-70.

PMID:2790784
Abstract

Flavone acetic acid (FAA, NSC 347512) is a new anticancer drug currently undergoing clinical investigation. Although the precise mechanism for its broad spectrum of activity against transplanted murine solid tumors is unknown, it has been reported that FAA reduces tumor blood flow and produces hemorrhagic necrosis. We have confirmed this finding with the murine transplanted carcinoma SCCVII: 200 mg/kg FAA reduced tumor blood flow to 20-30% of normal for 1-2 days as determined by rubidium 86 extraction. In an attempt to exploit the tumor hypoxia produced by FAA, we have combined it with the novel bioreductive drug SR 4233, a benzotriazine dioxide with high selective toxicity for hypoxic cells. Marked enhancement of the antitumor effect of FAA (200 mg/kg) was observed when it was combined with SR 4233 (0.1 and 0.2 mmol/kg). This was seen using tumor cell survival, regrowth delay, and histological endpoints, with the best results obtained when the two agents were injected simultaneously. These data suggest that targeting bioreductive cytotoxic agents to tumors by producing tumor hypoxia may be a valid way of increasing the tumor cell killing of these agents.

摘要

黄酮醋酸(FAA,NSC 347512)是一种目前正在进行临床研究的新型抗癌药物。尽管其对移植性小鼠实体瘤具有广谱活性的确切机制尚不清楚,但据报道FAA可减少肿瘤血流并导致出血性坏死。我们用小鼠移植癌SCCVII证实了这一发现:通过铷86提取测定,200mg/kg的FAA可使肿瘤血流在1-2天内降至正常水平的20%-30%。为了利用FAA产生的肿瘤缺氧状态,我们将其与新型生物还原药物SR 4233联合使用,SR 4233是一种对缺氧细胞具有高选择性毒性的二氧化苯并三嗪。当FAA(200mg/kg)与SR 4233(0.1和0.2mmol/kg)联合使用时,观察到FAA的抗肿瘤作用显著增强。这在肿瘤细胞存活、再生长延迟和组织学终点方面都有体现,当两种药物同时注射时效果最佳。这些数据表明,通过产生肿瘤缺氧状态将生物还原细胞毒性药物靶向肿瘤可能是增强这些药物对肿瘤细胞杀伤作用的有效方法。

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