邓清明1 李登进1 张林2,3.西妥昔单抗联合FOLFIRI 方案治疗晚期胃癌的疗效观察[J].,2012,12(10):1897-1901 |
西妥昔单抗联合FOLFIRI 方案治疗晚期胃癌的疗效观察 |
Effects of Cetuximab Combined with Modified FOLFIRI on AdvancedGastric Cancer in Second-line Treatment |
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DOI: |
中文关键词: 西妥昔单 胃癌 二线治疗 FOLFIRI 方案 |
英文关键词: Cetuximab Alone Gastric Cancer Second-Line Treatment FOLFIRI Program |
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中文摘要: |
目的:观察西妥昔单抗联合FOLFIRI 方案用于一线治疗失败的局部晚期或转移性胃癌患者,观察其疗效和不良反应,并观察
其与疗效和预后的相关性。方法:每2 疗程评价肿瘤病灶情况,观察不良反应,随访肿瘤进展情况及生存期。按照实体瘤疗效评
价标准(Response Evaluatione Criteria in solid Tumors,RECIST)进行肿瘤缓解评估,按照国立癌症研究所常见不良事件评价标准
3.0 版(NCI 一CTCAE3.0)进行不良事件分级。计算肿瘤缓解率、中位至疾病进展时间和中位总生存期。结果:在38 例至少完成了
2 个周期治疗并进行了疗效评价的患者中,观察到1 例完全缓解(CR),占0.03%;13 例部分缓解(PR),占34.00%;总的缓解率
(ORR=CR+PR)为37.00%。疾病稳定(SD)的患者有20 例,占53.00%;疾病控制率(Disease Control Rate,DCR=CR+PR+SD)为
89.00 %;疾病进展(PD)的患者为4 例,占11.00 %。本研究方案总体安全性良好,未发生一例治疗相关性死亡。其中III/IV 度粒细
胞减少的发生率为52.5%,粒缺性发热的发生率为13.1%,III/IV 度度贫血的发生率为29.5%,III/IV 度度血小板下降的发生率为
8.2%。III/IV 度非血液学毒性包括恶心(8.2%),呕吐(6.6%),口腔炎(1.6%),腹泻(6.6%),感染(4.9%),乏力(4.9%),肠梗阻(6.6%),转氨
酶升高(l.6%),过敏反应(l.6%)和皮疹(9.8%)。结论:本研究显示在晚期胃癌患者的二线治疗中西妥昔单抗联合FOLFIRI 是一个安
全有效的方案,需要进一步的研究寻找有效的生物标记物。 |
英文摘要: |
Objective: To observe the effects of Cetuximab combined with modified FOLFIRI on advanced gastric cancer in
second-line treatment and evaluate its efficacy and adverse reactions, and to investigate the relationship between its efficacy and
prognosis. Methods: Tumor lesions and adverse reactions were observed every 2 cycles of treatment, and the progress of tumor and
survival were followed up. Tumor remission assessment were performed in accordance with Response Evaluation Criteria in solid
Tumors (RECIST) and the adverse event were classified according to the Common adverse events evaluation criteria version 3.0 (NCI a
CTCAE3.0) by National Cancer Institute. Calculate the tumor remission rate, median time to progression and median overall survival.
Results: Among the 38 patients who completed at least 2 cycles of treatment and received efficacy evaluation, one case was observed in
complete remission (CR), accounting for 0.03%; 13 cases were in partial remission (PR), accounting for 34.00%; the overall remission
rate (ORR = CR + PR) was 37.00%. 20 cases were in status of stable disease (SD), accounting for 53.00%; disease control rate (Disease
Control Rate, DCR = CR + PR + SD) was 89.00%. Disease progression (PD) was occurred in 4 cases, accounting for 11.00%. The overall
safety is good, for no case of treatment-related death occurred. The III / IV neutropenia incidence was 52.5%, incidence of febrile due to
particle missing 13.1%, incidence of III / IV degree severe anemia 29.5%, incidence of III / IV degree of thrombocytopenia decline 8.2%.
III / IV degree of non-hematologic toxicity included nausea (8.2%), vomiting (6.6%), stomatitis (1.6%), diarrhea (6.6%), infection (4.9%),
fatigue (4.9%), ileus (6.6 %), elevated aminotransferases (l.6%), allergic reactions (l.6%) and rash (9.8%). Conclusion: This study showed
that Cetuximab combined with modified FOLFIRI is a safe and effective program in second-line treatment of advanced gastric cancer
patients. It is required to further research and find its effective biomarkers. |
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