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大鼠中丝裂霉素C肝动脉灌注与离体肝脏灌注的比较研究。

A comparative study of isolated liver perfusion versus hepatic artery infusion with mitomycin C in rats.

作者信息

Marinelli A, van de Velde C J, Kuppen P J, Franken H C, Souverijn J H, Eggermont A M

机构信息

Department of Surgery, University Hospital, Leiden, The Netherlands.

出版信息

Br J Cancer. 1990 Dec;62(6):891-6. doi: 10.1038/bjc.1990.404.

Abstract

Systemic toxicity is usually the dose-limiting factor in cancer chemotherapy. Regional chemotherapy is therefore an attractive strategy in the treatment of liver metastasis. Two ways of regional chemotherapy, hepatic artery infusion (HAI) and isolated liver perfusion (ILP), were compared investigating the difference in toxicity with tissue and biofluid concentrations of mitomycin C (MMC). In wistar derived WAG rats the maximally tolerated dose of mitomycin C via HAI was 1.2 mg kg-1. Body weight measurements after HAI with doses higher than 1.2 mg kg-1 suggest both an acute and delayed toxic effect of mitomycin C since the time weight curves were triphasic: a rapid weight loss, a steady state and a second fall in weight phase. These rats died due to systemic toxicity. ILP with 4.8 mg kg-1 was associated with no signs of systemic toxicity and only transient mild hepatotoxicity. ILP with 6.0 mg kg-1 was fatal mainly due to hepatic toxicity. The four times higher maximally tolerated dose in ILP resulted in a 4-5 times higher peak concentration of mitomycin C in liver tissue, while the plasma concentration remained significantly lower than in the HAI treated rats. In the tumour tissue a 500% higher concentration of mitomycin C was measured in the ILP with 4.8 mg kg-1 than in HAI with 1.2 mg kg-1 treated rats. We demonstrated that when mitomycin C was administered by ILP a 400% higher dose could be safely administered and resulted in a five times higher tumour tissue concentration. In view of the steep dose-response curve of this alkylating agent this opens new perspectives for the treatment of liver metastasis.

摘要

全身毒性通常是癌症化疗中的剂量限制因素。因此,区域化疗是治疗肝转移的一种有吸引力的策略。比较了两种区域化疗方法,即肝动脉灌注(HAI)和离体肝脏灌注(ILP),研究丝裂霉素C(MMC)在组织和生物流体中的浓度差异及其毒性差异。在源自Wistar的WAG大鼠中,通过HAI给予丝裂霉素C的最大耐受剂量为1.2mg/kg。HAI给予高于1.2mg/kg剂量后测量体重,提示丝裂霉素C具有急性和延迟毒性作用,因为体重随时间变化曲线呈三相:体重快速下降、稳定状态和体重再次下降阶段。这些大鼠死于全身毒性。4.8mg/kg的ILP未出现全身毒性迹象,仅出现短暂轻度肝毒性。6.0mg/kg的ILP主要因肝毒性而致命。ILP中最大耐受剂量高出四倍,导致肝组织中丝裂霉素C的峰值浓度高出4至5倍,而血浆浓度仍显著低于接受HAI治疗的大鼠。在肿瘤组织中,4.8mg/kg的ILP组中丝裂霉素C的浓度比1.2mg/kg的HAI组高出500%。我们证明,当通过ILP给予丝裂霉素C时,可以安全地给予高出400%的剂量,并使肿瘤组织浓度高出五倍。鉴于这种烷化剂陡峭的剂量反应曲线,这为肝转移的治疗开辟了新的前景。

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