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Novel cytotoxic regimens in gastric cancer

机译:胃癌的新型细胞毒性疗法

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摘要

The docetaxel--cisplatin-5-fluorouracil (TCF) triplet has demonstrated superiority over cisplatin-5-fluorouracil (CF) and subsequently gained approval in the USA and Europe for the treatment of advanced gastric cancer. While this is a major advancement in gastric cancer therapy, there is potential to further improve outcomes by optimizing and building on the TCF regimen. The availability of 'new' cytotoxic agents such as oxaliplatin, irinotecan, capecitabine and S-1, as well as the biological agents, provides many options for modifying the standard TCF regimen, as used in the TAX 325 study. Potential strategies to improve efficacy, tolerability and/or convenience include variations in the dosing schedule, the substitution of cisplatin with oxaliplatin, the substitution of 5-fluorouracil with oral fluoropyrimidines, and the addition of biological agents. Emerging data support the feasibility of these strategies and will be reviewed in this article.
机译:多西他赛-顺铂-5-氟尿嘧啶(TCF)三联体已显示出优于顺铂-5-氟尿嘧啶(CF)的优越性,随后在美国和欧洲获得了用于治疗晚期胃癌的批准。尽管这是胃癌治疗的重大进展,但仍有可能通过优化和建立TCF方案进一步改善治疗效果。如TAX 325研究中所使用的,诸如奥沙利铂,伊立替康,卡培他滨和S-1等“新”细胞毒剂的可用性以及生物剂,为修改标准TCF方案提供了许多选择。改善功效,耐受性和/或便利性的潜在策略包括给药方案的变化,用奥沙利铂替代顺铂,用口服氟嘧啶替代5-氟尿嘧啶以及添加生物制剂。新兴数据支持了这些策略的可行性,并将在本文中进行回顾。

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