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首页> 外文期刊>Current drug targets-The International journal for timely in-depth reviews on drug targets >Proteomics in acute myelogenous leukaemia (AML): methodological strategies and identification of protein targets for novel antileukaemic therapy.
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Proteomics in acute myelogenous leukaemia (AML): methodological strategies and identification of protein targets for novel antileukaemic therapy.

机译:急性骨髓性白血病(AML)中的蛋白质组学:新抗肿瘤药物治疗的方法策略和蛋白质靶标的鉴定。

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摘要

Enduring efforts into determination of the molecular biological status of acute myelogenous leukaemia (AML), a stem cell disease characterised by distinct blastic differentiation blocks and their extensive growth, continue to provide us with prognostically important information for more than half of all patients. In subsets of AML, molecular diagnostics rigorously guide the clinician toward the choice of optimal therapy. The in-depth characterization of leukemogenesis associated genetic alterations, such as the combined presence of activating mutations of tyrosine kinases together with altered transcription factors, and the documented impact of these mutations upon prognosis of AML, suggests AML as a primary candidate for pioneering proof-of-principle studies with new high throughput protein analysis techniques. This review aims to introduce the reader to proteomic methodology, e.g. two-dimensional polyacrylamide gel electrophoresis, mass spectrometry, SELDI and protein arrays. Examples of its use, including single cell phosphoprotein profiling in risk stratification, the probing of cellular effects of conventional chemotherapeutics and novel target determination are presented. Based on original proteomic analysis of AML, molecular characteristics of AML, in addition to knowledge of conventional therapeutics and novel drugs, we attempt to forecast the influence of proteomics in therapy development for AML.
机译:努力确定急性骨髓性白血病(AML)的分子生物学状态,这是一种以明显的幼稚分化块及其广泛生长为特征的干细胞疾病,继续为我们提供了超过一半患者的预后重要信息。在AML的子集中,分子诊断严格指导临床医生选择最佳疗法。白血病生成相关基因改变的深入表征,例如酪氨酸激酶激活突变与转录因子改变的结合存在,以及这些突变对AML预后的记录影响,表明AML是开创性证据的主要候选人-新的高通量蛋白质分析技术进行原理研究。这篇综述旨在向读者介绍蛋白质组学方法,例如二维聚丙烯酰胺凝胶电泳,质谱,SELDI和蛋白质阵列。介绍了其用途的实例,包括风险分层中的单细胞磷酸化蛋白谱分析,常规化学疗法对细胞作用的探测以及新型靶标的确定。基于AML的原始蛋白质组学分析,AML的分子特征,除了传统疗法和新药的知识外,我们尝试预测蛋白质组学在AML疗法开发中的影响。

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