首页> 外文期刊>BMC Cancer >Multivariate and subgroup analyses of a randomized, multinational, phase 3 trial of decitabine vs treatment choice of supportive care or cytarabine in older patients with newly diagnosed acute myeloid leukemia and poor- or intermediate-risk cytogenetics
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Multivariate and subgroup analyses of a randomized, multinational, phase 3 trial of decitabine vs treatment choice of supportive care or cytarabine in older patients with newly diagnosed acute myeloid leukemia and poor- or intermediate-risk cytogenetics

机译:地西他滨与新诊断为急性髓样白血病且细胞遗传学风险中等或中等风险的老年患者的地西他滨与治疗选择支持治疗或阿糖胞苷的随机,多国,3期临床试验的多变量和亚组分析

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Background Compared with younger patients, older adults with acute myeloid leukemia (AML) generally have poorer survival outcomes and less benefit from clinical trials. A recent phase 3 trial demonstrated a trend toward improved overall survival (OS) with decitabine, a hypomethylating agent, compared with treatment choice of either cytarabine or supportive care (7.7?months, 95% CI: 6.2–9.2 vs 5.0?months, 95% CI: 4.3–6.3, respectively) in older adults with newly diagnosed AML. The current analyses investigated prognostic factors for outcomes in this trial and examined OS and responses in prespecified subgroups. Methods A multivariate Cox proportional hazards model was used to investigate effects of demographic and baseline characteristics, including age, sex, cytogenetic risk, AML type, ECOG Performance Status, geographic region, bone marrow blasts, platelets, and white blood cells on OS, based on mature data. Similar analyses were conducted with a logistic regression model to predict response rates. Prespecified subgroup analyses were performed for OS and response rates, also using mature data. Results Patient characteristics that appeared to negatively influence OS included more advanced age (hazard ratio [HR] 1.560 for ≥75 vs 50% vs ≤50%; p?=?0.0045), low baseline platelet counts (HR 0.775 for each additional 100?×?109/L; p?=?0.0015), and high white blood cell counts (HR 1.256 for each additional 25?×?109/L; p?=?0.0151). Regarding geographic regions, patients from Western Europe had the longest median OS. Response rates favored decitabine for all subgroups investigated, including patients ≥75?years (odds ratio 5.94, p?=?0.0006). Conclusion Response to decitabine in AML is associated with known prognostic factors related to both patient demographics and disease characteristics. Trial registration ClinicalTrials.gov identifier NCT00260832
机译:背景技术与年轻患者相比,患有急性髓细胞性白血病(AML)的老年人通常生存期较差,临床试验获益较少。最近的一项3期试验表明,与阿糖胞苷或支持治疗的治疗选择相比,地西他滨(一种低甲基化剂)改善了总生存(OS)的趋势(7.7?月,95%CI:6.2-9.2与5.0?月,95)。在新诊断为AML的老年人中,CI分别为4.3-6.3%。目前的分析调查了该试验结果的预后因素,并检查了预先确定的亚组的OS和反应。方法采用多元Cox比例风险模型研究人口统计学和基线特征的影响,包括年龄,性别,细胞遗传风险,AML类型,ECOG表现状态,地理区域,骨髓母细胞,血小板和白细胞对OS的影响,基于根据成熟的数据。使用逻辑回归模型进行了类似的分析,以预测响应率。还使用成熟的数据对OS和响应率进行了预先指定的亚组分析。结果似乎对OS产生不利影响的患者特征包括更高的年龄(≥75 vs 50%vs≤50%的危险比[HR] 1.560; p?=?0.0045),低基线血小板计数(每增加100 HR HR 0.775)。 ×?10 9 / L; p?=?0.0015)和高白细胞计数(每增加25?×?10 9 / L HR 1.256; p ?=?0.0151)。就地理区域而言,西欧患者的OS中位数最长。在所有接受调查的亚组中,包括≥75岁的患者,应答率均倾向于地西他滨(比值比为5.94,p = 0.0006)。结论AML中对地西他滨的反应与已知的预后因素有关,该因素与患者的人口统计学特征和疾病特征有关。试验注册ClinicalTrials.gov标识符NCT00260832

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