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Functional proteomic profiling of AML predicts response and survival.

机译:AML的功能蛋白质组分析可预测反应和生存率。

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摘要

Because protein function regulates the phenotypic characteristics of cancer, a functional proteomic classification system could provide important information for pathogenesis and prognosis. With the goal of ultimately developing a proteomic-based classification of acute myeloid leukemia (AML), we assayed leukemia-enriched cells from 256 newly diagnosed AML patients, for 51 total and phosphoproteins from apoptosis, cell-cycle, and signal-transduction pathways, using reverse-phase protein arrays. Expression in matched blood and marrow samples were similar for 44 proteins; another 7 had small fold changes (8%-55%), suggesting that functional proteomics of leukemia-enriched cells in the marrow and periphery are similar. Protein expression patterns were independent of clinical characteristics. However, 24 proteins were significantly different between French-American-British subtypes, defining distinct signatures for each. Expression signatures for AML with cytogenetic abnormalities involving -5 or -7 were similar suggesting mechanistic commonalities. Distinct expression patterns for FMS-like tyrosine kinase 3-internal tandem duplication were also identified. Principal component analysis defined 7 protein signature groups, with prognostic information distinct from cytogenetics that correlated with remission attainment, relapse, and overall survival. In conclusion, protein expression profiling patterns in AML correlate with known morphologic features, cytogenetics, and outcome. Confirmation in independent studies may also provide pathophysiologic insights facilitating triage of patients to emerging targeted therapies.
机译:由于蛋白质功能调节癌症的表型特征,因此功能蛋白质组学分类系统可以为发病机理和预后提供重要信息。为了最终建立基于蛋白质组学的急性髓性白血病(AML)分类,我们对256名新诊断的AML患者的富含白血病的细胞进行了分析,分析了凋亡,细胞周期和信号转导途径中的51种总蛋白和磷蛋白,使用反相蛋白质阵列。在匹配的血液和骨髓样本中,44种蛋白质的表达相似。另外7个细胞的折叠变化很小(8%-55%),这表明骨髓和外周血中富含白血病的细胞的功能蛋白质组学相似。蛋白质表达模式与临床特征无关。但是,法裔,美籍,英裔亚型之间有24种蛋白质显着不同,为每种亚种定义了不同的特征。具有涉及-5或-7的细胞遗传学异常的AML的表达特征相似,表明机制的共性。还确定了FMS样酪氨酸激酶3内部串联重复的不同表达模式。主成分分析定义了7个蛋白质特征组,其预后信息不同于与缓解程度,复发和总生存期相关的细胞遗传学信息。总之,AML中的蛋白质表达谱模式与已知的形态学特征,细胞遗传学和预后相关。在独立研究中进行的确认也可能会提供病理生理学见解,以促进对患者进行新的靶向治疗的分类。

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