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一种新型二芳基磺酰脲类抗癌药物的临床药理学

Clinical pharmacology of a novel diarylsulfonylurea anticancer agent.

作者信息

Taylor C W, Alberts D S, Ketcham M A, Satterlee W G, Holdsworth M T, Plezia P M, Peng Y M, McCloskey T M, Roe D J, Hamilton M

机构信息

Department of Internal Medicine, University of Arizona College of Medicine, Tucson 85724.

出版信息

J Clin Oncol. 1989 Nov;7(11):1733-40. doi: 10.1200/JCO.1989.7.11.1733.

Abstract

LY186641 (diarylsulfonylurea, [DSU]) is a novel anticancer agent because of its unique diarylsulfonylurea chemical structure, broad-spectrum antisolid-tumor activity in preclinical models, presumed novel mechanism of action and preclinical toxicities of methemoglobinemia (Met Hgb) and decreased red blood cell (RBC) survival. In this study, the in vitro drug sensitivity of human tumors as well as clinical pharmacology and toxicology of DSU in patients with cancer were examined. DSU was administered orally, daily for 7 days with a 3-week treatment cycle. Dose-limiting toxicities were Met Hgb and RBC hemolysis. The maximum-tolerated dose was found to be 1,200 mg/m2/d for 7 days. In pharmacokinetic studies, DSU was found to have a prolonged serum half-life (approximately 30 hours) and a large area under the plasma disappearance curve (8,883.3 micrograms.hr/mL at 1,200 mg/m2/d). A partial remission was observed in one patient with refractory ovarian cancer. In conclusion, DSU can be safely administered to cancer patients and does display antitumor activity. Potential means of obviating the toxicities of this compound are discussed.

摘要

LY186641(二芳基磺酰脲,[DSU])是一种新型抗癌药物,因其独特的二芳基磺酰脲化学结构、临床前模型中的广谱抗实体瘤活性、推测的新作用机制以及高铁血红蛋白血症(Met Hgb)和红细胞(RBC)存活降低的临床前毒性。在本研究中,检测了人类肿瘤的体外药物敏感性以及DSU在癌症患者中的临床药理学和毒理学。DSU口服给药,每天一次,共7天,治疗周期为3周。剂量限制性毒性为高铁血红蛋白血症和红细胞溶血。发现最大耐受剂量为1200mg/m²/天,持续7天。在药代动力学研究中,发现DSU的血清半衰期延长(约30小时),血浆消除曲线下面积较大(在1200mg/m²/天时为8883.3微克·小时/毫升)。一名难治性卵巢癌患者出现部分缓解。总之,DSU可以安全地给予癌症患者,并且确实显示出抗肿瘤活性。讨论了消除该化合物毒性的潜在方法。

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