甲氧基吗啉代阿霉素（FCE 23762-MMRDX）在非小细胞肺癌、肾癌及其他实体瘤患者中的广泛II期和药代动力学研究。

Broad phase II and pharmacokinetic study of methoxy-morpholino doxorubicin (FCE 23762-MMRDX) in non-small-cell lung cancer, renal cancer and other solid tumour patients.

作者信息

Bakker M, Droz J P, Hanauske A R, Verweij J, van Oosterom A T, Groen H J, Pacciarini M A, Domenigoni L, van Weissenbruch F, Pianezzola E, de Vries E G

机构信息

University Hospital Groningen, The Netherlands.

出版信息

Br J Cancer. 1998;77(1):139-46. doi: 10.1038/bjc.1998.22.

DOI:10.1038/bjc.1998.22

PMID:9459159

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2151269/

Abstract

The aim was to perform a broad phase II and pharmacokinetic study of methoxymorpholino-doxorubicin (MMRDX), a drug active against multidrug-resistant tumour cells in vitro when given by i.v. bolus at 1.5 mg m(-2) every 4 weeks, in metastatic or unresectable solid tumour patients with known intrinsic drug resistance. Patients received a maximum of six cycles. Plasma, urine and leucocyte MMRDX and its 13-dihydro metabolite pharmacokinetic analysis was performed in patients without liver metastases. Patients (n = 48, 21 NSCLC, 19 renal cell, three head and neck tumour, three cervical cancer and two adenocarcinoma of unknown primary) received 132 cycles of MMRDX. Common toxicity criteria (CTC) grade III/IV thrombocytopenia (12% of cycles) and neutropenia (27% of cycles) occurred with median nadir on day 22. Transient transaminases elevation > grade III/IV was observed in 7% of cycles, late and prolonged nausea > or = grade II in 34% and vomiting > or = grade II in 39%. In two patients, the left ventricular ejection fraction was reduced > or = 15%. Of 37 evaluable patients, one out of 17 NSCLC had a partial response. Mean (+/- s.d.) MMRDX AUC0-infinity calculated up to 24 h after dosing was 20.4 +/- 6.2 microg h l(-1) (n = 11) and t(1/2, gamma) was 44.2 h. Mean plasma clearance (+/- s.d.) was 37.2 +/- 7.3 l h(-1) m(-2) and volume of distribution 1982 +/- 64 l m(-2). MMRDX leucocyte levels 2 and 24 h after infusion were 450 to 600-fold higher than corresponding MMRDX plasma levels. In urine, 2% of the MMRDX dose was excreted unchanged, and 2% as metabolite. The main side-effects of 1.5 mg m(-2) every 4 weeks of MMRDX are delayed nausea and vomiting and haematological toxicity. MMRDX is characterized by extensive clearance and rapid and extensive distribution into tissues. A low response rate was observed in patients with tumours with intrinsic chemotherapy resistance.

摘要

目的是对甲氧基吗啉代阿霉素（MMRDX）进行一项广泛的II期和药代动力学研究。MMRDX是一种在体外对多药耐药肿瘤细胞有活性的药物，通过静脉推注给药，剂量为1.5mg/m²，每4周一次，用于患有已知内在耐药性的转移性或不可切除实体瘤患者。患者最多接受六个周期的治疗。对无肝转移的患者进行血浆、尿液和白细胞中MMRDX及其13 - 二氢代谢物的药代动力学分析。患者（n = 48，21例非小细胞肺癌、19例肾细胞癌、3例头颈部肿瘤、3例宫颈癌和2例原发灶不明的腺癌）接受了132个周期的MMRDX治疗。常见毒性标准（CTC）III/IV级血小板减少（占周期的12%）和中性粒细胞减少（占周期的27%）出现，最低点中位数在第22天。7%的周期观察到短暂的转氨酶升高>III/IV级，34%的周期出现晚期和持续性恶心≥II级，39%的周期出现呕吐≥II级。两名患者的左心室射血分数降低≥15%。在37例可评估患者中，17例非小细胞肺癌患者中有1例出现部分缓解。给药后24小时内计算的MMRDX平均（±标准差）AUC0 - ∞为20.4±6.2μg·h·l⁻¹（n = 11），t(1/2,γ)为44.2小时。平均血浆清除率（±标准差）为37.2±7.3l·h⁻¹·m⁻²，分布容积为1982±64l·m⁻²。输注后2小时和24小时MMRDX白细胞水平比相应的MMRDX血浆水平高450至600倍。在尿液中，2%的MMRDX剂量以原形排泄，2%以代谢物形式排泄。每4周一次给予1.5mg/m²的MMRDX的主要副作用是延迟性恶心和呕吐以及血液学毒性。MMRDX的特点是清除广泛，迅速且广泛地分布到组织中。在具有内在化疗耐药性的肿瘤患者中观察到低缓解率。