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Clinical Trials and Observations: Expression of ARC (apoptosis repressor with caspase recruitment domain) an antiapoptotic protein is strongly prognostic in AML

机译:临床试验和观察:抗凋亡蛋白ARC(具有caspase募集结构域的凋亡抑制因子)的表达在AML中具有强烈的预后

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摘要

Regulators of apoptosis in acute myeloid leukemia (AML) have been extensively studied and are considered excellent therapeutic targets. Apoptosis repressor with caspase recruitment domain (ARC), an antiapoptotic protein originally found to be involved in apoptosis of cardiac cells, was recently demonstrated to be overexpressed in several solid tumors. To assess its importance in AML, we profiled ARC expression in 511 newly diagnosed AML patients using a validated robust reverse-phase protein array and correlated ARC levels with clinical outcomes. ARC was variably expressed in samples from patients with AML. ARC level was not associated with cytogenetic groups or with FLT-3 mutation status. However, patients with low or medium ARC protein levels had significantly better outcomes than those with high ARC levels: longer overall survival (median, 53.9 or 61.6 vs 38.9 weeks, P = .0015) and longer remission duration (median, 97.6 or 44.7 vs 31.1 weeks, P = .0007). Multivariate analysis indicated that ARC was a statistically significant independent predictor of survival in AML (P = .00013). Inhibition of ARC promoted apoptosis and sensitized cytosine arabinoside-induced apoptosis in OCI-AML3 cells. These results suggest that ARC expression levels are highly prognostic in AML and that ARC is a potential therapeutic target in AML.
机译:急性髓细胞性白血病(AML)中凋亡的调节剂已被广泛研究,被认为是极好的治疗靶标。具有半胱天冬酶募集域(ARC)的凋亡抑制因子,一种最初被发现与心脏细胞凋亡有关的抗凋亡蛋白,最近被证明在几种实体瘤中过表达。为了评估其在AML中的重要性,我们使用经过验证的可靠的逆相蛋白质阵列分析了511名新诊断的AML患者的ARC表达,并将ARC水平与临床结果相关联。 ARC在来自AML患者的样本中有不同的表达。 ARC水平与细胞遗传学组或FLT-3突变状态无关。但是,低或中等ARC蛋白水平的患者比高ARC水平的患者具有更好的预后:更长的总生存期(中位53.9或61.6 vs 38.9周,P = 0.0015)和更长的缓解时间(中位97.6或44.7 vs 31.1周,P = .0007)。多变量分析表明,ARC是AML生存率的统计学上重要的独立预测因子(P = .00013)。 ARC的抑制促进了OCI-AML3细胞的凋亡和敏化的胞嘧啶阿拉伯糖苷诱导的凋亡。这些结果表明ARC表达水平在AML中是高度预后的,并且ARC是AML中潜在的治疗靶标。

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