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恶性胸膜间皮瘤化疗的当前概念

Current concepts in chemotherapy for malignant pleural mesothelioma.

作者信息

Sørensen Jens Benn

机构信息

Department of Oncology, Finsen Centre, National University Hospital, Copenhagen, Denmark.

出版信息

Clin Respir J. 2008 Apr;2(2):74-9. doi: 10.1111/j.1752-699X.2008.00046.x.

Abstract

OBJECTIVES

The aim of this study was to provide an overview of the most active single agents and combination regimens in malignant pleural mesothelioma (MPM).

DATA SOURCE

Literature on English-language trials in humans was searched on Medline until October 2007. Indexing terms were malignant pleural mesothelioma and chemotherapy.

STUDY SELECTIONS

Trials with > or =15 patients and with data on activity were included.

RESULTS

Detorubicin and pirarubicin have response rates (RRs) of 22%-26%, epirubicin of 5%-15%, docetaxel of 5%-23% and vinorelbine of 24%. Other active agents were ifosfamide (3%-24%) and mitomycin C (21%). Carboplatin and cisplatin have an overall RR of 11% in three studies and 17% in four studies, respectively. Antimetabolites were active, including methotrexate (37%), raltitrexed (21%), edatrexate (16%-25%) and pemetrexed (15%). With respect to combination chemotherapy regimens, only cisplatin with either pemetrexed or raltitrexed has been compared with other substances, in both cases to cisplatin monotherapy. Both showed a survival advantage, which was statistically significant in the trial including pemetrexed, suggesting that chemotherapy improved survival in MPM. No studies have compared chemotherapy with the best supportive care alone, and none has compared different combination chemotherapy regimens with each other.

CONCLUSIONS

A number of single-agent cytotoxics posess moderate activity against MPM. A number of platinum-based combination chemotherapy regimens show similar activities, but none has been compared with another combination. Cisplatin with either raltitrexed or pemetrexed has improved survival compared with cisplatin alone, and may be used as a reference treatment in randomized trials. Targeted agents should be explored in order to further improve the outcome.

摘要

目的

本研究旨在概述恶性胸膜间皮瘤(MPM)中最有效的单药及联合治疗方案。

数据来源

检索Medline中截至2007年10月的英文人体试验文献。检索词为恶性胸膜间皮瘤和化疗。

研究选择

纳入患者≥15例且有活性数据的试验。

结果

去甲柔红霉素和吡柔比星的缓解率(RRs)为22% - 26%,表柔比星为5% - 15%,多西他赛为5% - 23%,长春瑞滨为24%。其他活性药物有异环磷酰胺(3% - 24%)和丝裂霉素C(21%)。在三项研究中卡铂和顺铂的总体RR分别为11%,在四项研究中分别为17%。抗代谢药物有活性,包括甲氨蝶呤(37%)、雷替曲塞(21%)、依达曲沙(16% - 25%)和培美曲塞(15%)。关于联合化疗方案,仅顺铂联合培美曲塞或雷替曲塞与其他药物进行了比较,两种情况均与顺铂单药治疗比较。两者均显示出生存优势,在包含培美曲塞的试验中具有统计学意义,提示化疗可改善MPM患者的生存。尚无研究将化疗与单纯最佳支持治疗进行比较,也没有比较不同联合化疗方案之间的差异。

结论

多种单药细胞毒性药物对MPM具有中等活性。多种铂类联合化疗方案显示出相似活性,但未相互比较。顺铂联合雷替曲塞或培美曲塞与顺铂单药相比可改善生存,可作为随机试验的参考治疗方案。应探索靶向药物以进一步改善治疗效果。

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