奥沙利铂诱导的神经病变对晚期胃癌紫杉醇治疗的影响

J. Sato, S. Iwasa, Y. Honma, A. Takashima, N. Okita, Ken Kato, T. Hamaguchi, Y. Yamada, N. Boku
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引用次数: 1

摘要

目的:多项研究表明,氟嘧啶联合奥沙利铂(SOX)作为晚期胃癌一线化疗方案的疗效不低于氟嘧啶联合顺铂。我们回顾性探讨以SOX为一线化疗的晚期胃癌患者后续治疗中二线方案的选择,以及含紫杉醇方案的比例和可行性。材料与方法:回顾性分析奥沙利铂诱导的神经病变对后续方案选择及后续紫杉醇化疗可行性的影响,以S-1 +奥沙利铂一线化疗的晚期胃癌患者为研究对象。结果:共有31名患者参加了评估S-1 +奥沙利铂的2期和3期研究,分析了27名患者(4名患者被认为不合格)。在24例接受二线治疗的患者中,有2例患者由于奥沙利铂引起的神经病变而未选择紫杉醇。16例患者选择紫杉醇作为二线化疗,6例患者选择三线化疗,1例患者选择四线化疗。在接受紫杉醇治疗前,11/10/2/0患者感觉神经病变的严重程度分别为0/1/2/3级,而紫杉醇治疗期间最严重的毒性分别为7/13/1/2患者0/1/2/3级。虽然没有患者因神经病变而需要减少紫杉醇的剂量,但有2例患者在服用紫杉醇4或8次后因3级感觉神经病变而停止使用紫杉醇。结论:奥沙利铂所致的一线化疗神经病变可能影响晚期胃癌患者后续紫杉醇化疗的选择和可行性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Impact of Oxaliplatin-Induced Neuropathy on Subsequent Paclitaxel for Advanced Gastric Cancer
Purpose: Several studies have shown that fluoropyrimidine plus oxaliplatin (SOX) is non-inferior to fluoropyrimidine plus cisplatin as first-line chemotherapy for advanced gastric cancer. We investigated retrospectively the choice of second-line regimen, along with the proportion and feasibility of paclitaxel-containing regimen, in the subsequent treatment of patients with advanced gastric cancer treated with SOX as first-line chemotherapy. Materials and Methods: We retrospectively analyzed the impact of oxaliplatin-induced neuropathy on both the choice of subsequent regimens and feasibility of subsequent chemotherapy with paclitaxel, focusing on patients with advanced gastric cancer who received S-1 plus oxaliplatin as first-line chemotherapy. Results: Twenty-seven from a total of 31 patients enrolled into the phase 2 and phase 3 study assessing S-1 plus oxaliplatin were analyzed (4 patients were deemed ineligible). Among 24 patients that had received second-line treatment, paclitaxel was not selected in 2 patients due to oxaliplatin-induced neuropathy. Paclitaxel was selected as second-line chemotherapy in 16 patients, as third-line chemotherapy in 6 patients and fourth-line chemotherapy in one patient. Severity of sensory neuropathy was grade 0/1/2/3 in 11/10/2/0 patients, respectively, immediately before treatment with paclitaxel, while the worst toxicity profile during paclitaxel treatment was grade 0/1/2/3 in 7/13/1/2 patients, respectively. Although there were no patients requiring dose reductions of paclitaxel due to neuropathy, 2 patients discontinued paclitaxel use due to grade 3 sensory neuropathy after 4 or 8 administrations of paclitaxel. Conclusion: Oxaliplatin-induced neuropathy during first-line chemotherapy may affect the choice and feasibility of subsequent chemotherapy with paclitaxel in advanced gastric cancer patients.
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