S-1 plus docetaxel combination: another adjuvant treatment option for stage III gastric cancer

H. Jeung, S. Noh
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引用次数: 0

Abstract

© Digestive Medicine Research. All rights reserved. Dig Med Res 2022 | https://dx.doi.org/10.21037/dmr-22-50 Despite decades of declining prevalence, gastric cancer (GC) still accounts for over 770,000 cancer-related mortalities worldwide (1). A common therapeutic approach for the treatment of GC involves gastric resection plus with D2 lymph node dissection. However, even following radical surgery, recurrence is typical in the case of locally advanced GC (stage II–III). Postoperative adjuvant chemotherapy trials, which were conducted mainly in Asian patients, confirmed a significant improvement in the survival rate in the adjuvant chemotherapy compared with observation only in resectable GC. Therefore, this surgery-first approach has been strengthened in Asian nations where hematogenous and peritoneal recurrences are common (2). The Japanese ACTS-GC trial was the first positive phase III outcome to address adjuvant chemotherapy with S-1, an oral fluoropyrimidine, as being superior to the “surgery alone” (3). In this trial, 1,059 patients with stage II (excluding T1) or stage III GCs according to the Japanese classification were randomly assigned to the ‘surgery-only’ arm or ‘S-1 treatment’ arm, in which S-1 was administered for a year following D2 gastrectomy. At 3 years, recurrencefree survival (RFS) was 72% in the S-1 arm and 60% in the surgery-only arm [hazard ratio (HR) =0.62; 95% confidence interval (CI): 0.50–0.77; P<0.001], and the overall 3-year survival rates were 80% and 70%, respectively (HR =0.68; 95% CI: 0.52–0.87; P=0.003). However, subgroup analysis revealed that S-1 could only prolong survival in patients with early disease stages (stage II or IIIA) and was unable to prevent hematogenous dissemination (3). Moreover, S-1 is also not widely available worldwide. As a result, in order to improve the clinical outcome, particularly in a more advanced stage IIIB state, it was required to look for a better alternative option, such as one based on a pharmaceutical doublet. In this regard, JACCRO GC-07 study provided an intriguing alternative to S-1 monotherapy (4). The study’s objective was to address whether S-1 plus docetaxel doublet was superior to S-1 alone following R0 resection of pathologic stage III GC. The third English edition of the Japanese Classification of Gastric Carcinoma, which includes stage IIIA (T2N3, T3N2, T4aN1), stage IIIB (T3N3, T4aN2, T4bN0, T4bN1), or stage IIIC (T4aN3, T4bN2, T4bN3), was used to define pathologic stage III GC (5). To briefly summarize the treatment schedule, S-1 was delivered on days 1 through 14 of the first course’s 3-week cycle. After that, patients received intravenous infusions of docetaxel (40 mg/m body surface area) on the first day of each cycle and S-1 (days 1 through 14 of a 3-week cycle) throughout the second to seventh cycle. Patients in the S-1 group received S-1 from days 1 to 28 of a 6-week up to 1 year. The investigators had planned to enroll 1,100 patients between 2013 and 2017, and the second interim analysis was published in 2019 when the number of events reached 216 among 915 enrolled patients. The research revealed that the S-1 plus docetaxel group (n=456) had Editorial Commentary
S-1 +多西紫杉醇联合治疗:III期胃癌的另一种辅助治疗选择
©消化医学研究。版权所有。尽管几十年来患病率不断下降,但胃癌(GC)仍在全球范围内造成超过77万例与癌症相关的死亡(1)。治疗胃癌的常用治疗方法包括胃切除术加D2淋巴结清扫。然而,即使在根治性手术后,局部晚期胃癌(II-III期)的复发也是典型的。主要在亚洲患者中进行的术后辅助化疗试验证实,与仅观察可切除胃癌患者相比,辅助化疗可显著提高生存率。因此,这种手术优先的方法在亚洲国家得到了加强,因为这些国家的血液和腹膜复发很常见(2)。日本ACTS-GC试验是第一个用S-1(一种口服氟嘧啶)辅助化疗优于“单独手术”的III期阳性结果(3)。1059例II期(不包括T1期)或III期GCs患者被随机分配到“仅手术”组或“S-1治疗”组,其中S-1治疗组在D2胃切除术后给予1年。3年时,S-1组无复发生存率(RFS)为72%,单纯手术组为60%[风险比(HR) =0.62;95%置信区间(CI): 0.50-0.77;P<0.001],总3年生存率分别为80%和70% (HR =0.68;95% ci: 0.52-0.87;P = 0.003)。然而,亚组分析显示,S-1仅能延长疾病早期(II期或IIIA期)患者的生存期,不能阻止血液传播(3)。此外,S-1在全球范围内也没有广泛应用。因此,为了改善临床结果,特别是在更晚期的IIIB阶段,需要寻找更好的替代选择,例如基于药物双重药物的选择。在这方面,JACCRO GC-07研究为S-1单药治疗提供了一个有趣的替代方案(4)。该研究的目的是解决在R0切除病理III期GC后,S-1加多西他赛双药是否优于S-1单独治疗。第三版英文版《日本胃癌分类》,包括IIIA期(T3N3、T3N2、T4aN1)、IIIB期(T3N3、T4aN2、T4bN0、T4bN1)或IIIC期(T4aN3、T4bN2、T4bN3),用于定义病理III期GC(5)。为了简要总结治疗方案,S-1在第一个疗程的3周周期的第1天至第14天给予。之后,患者在每个周期的第一天静脉输注多西紫杉醇(40 mg/m体表面积),在第二至第七周期(3周周期的第1至第14天)静脉输注S-1。S-1组患者从6周至1年的第1天至28天接受S-1治疗。研究人员计划在2013年至2017年期间招募1100名患者,第二次中期分析于2019年发表,当时915名入组患者中发生的事件数量达到216例。研究发现S-1 +多西紫杉醇组(n=456)有编辑评论
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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