Phase I evaluation of coumarin (1,2-benzopyrone) and cimetidine in patients with advanced malignancies.

Molecular biotherapy Pub Date : 1991-09-01
M E Marshall, K Butler, A Fried
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Abstract

Fifty-four patients with advanced malignancies were treated on this phase I trial of coumarin and cimetidine. The dose of coumarin was escalated, with three patients treated at each dose level, while the cimetidine dose was held constant at 300 mg four times daily. Patients received coumarin alone as a single daily oral dose for 14 days; on day 15, cimetidine was added and both drugs were continued until progression of disease. This trial was initiated with patients receiving coumarin at 400 mg daily and closed at 7 g daily with four of five patients on this dose experiencing nausea and vomiting. Treatment was generally well tolerated over a wide range of coumarin doses. Symptomatic side effects were few, mild, and usually self limited. Side effects included insomnia, nausea, vomiting, diarrhea, and dizziness. Two patients withdrew from therapy because of daily nausea and vomiting. Typically, nausea, vomiting, and dizziness occurred 2.5-3 hours after a dose of coumarin. In most patients, these side effects abated spontaneously with continuation of therapy. There was no significant hematologic or renal toxicity. Hepatotoxicity occurred in only one patient and was manifested by asymptomatic abnormal elevations of serum hepatic transaminases. This toxicity was reversible upon interruption of therapy. Objective tumor regressions were observed in six patients with renal cell carcinoma. Responses occurred at coumarin doses ranging from 600 mg to 5 g daily. Coumarin is a relatively nontoxic, oral, outpatient therapy that warrants further investigations for the treatment of human malignancies. Because of its low toxicity, there is potential for combining coumarin with chemotherapeutic and/or biological agents in an attempt to improve on efficacy.(ABSTRACT TRUNCATED AT 250 WORDS)

香豆素(1,2-苯并吡酮)和西咪替丁在晚期恶性肿瘤患者中的I期评价。
54名晚期恶性肿瘤患者接受了香豆素和西咪替丁的I期临床试验。香豆素的剂量逐渐增加,每个剂量水平治疗3名患者,而西咪替丁的剂量保持不变,每天4次,每次300毫克。患者接受香豆素单独治疗,每天口服一次,持续14天;第15天,加入西咪替丁,两种药物持续使用,直到疾病进展。这项试验开始时,患者每天服用400毫克香豆素,结束时每天服用7克香豆素,服用该剂量的5名患者中有4名出现恶心和呕吐。在大范围香豆素剂量下,治疗通常耐受良好。症状性副作用很少,轻微,通常是自限性的。副作用包括失眠、恶心、呕吐、腹泻和头晕。2例患者因每日恶心呕吐而退出治疗。通常,服用香豆素2.5-3小时后会出现恶心、呕吐和头晕。在大多数患者中,这些副作用随着治疗的继续而自发减轻。没有明显的血液或肾脏毒性。仅1例患者出现肝毒性,表现为血清肝转氨酶无症状异常升高。这种毒性在治疗中断后是可逆的。目的观察6例肾细胞癌的肿瘤消退情况。香豆素的剂量为每天600毫克至5克。香豆素是一种相对无毒,口服,门诊治疗,值得进一步研究治疗人类恶性肿瘤。由于香豆素的低毒性,有可能与化疗和/或生物制剂联合使用以提高疗效。(摘要删节250字)
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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