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首页> 外文期刊>International journal of hematologic oncology. >Targeted therapies in the treatment of adult acute myeloid leukemias: current status and future perspectives
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Targeted therapies in the treatment of adult acute myeloid leukemias: current status and future perspectives

机译:针对性疗法治疗成人急性髓性白血病:现状和未来的观点

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摘要

The rapid advancement of next-generation sequencing techniques and the identification of molecular driver events responsible for leukemia development are opening the door to new pharmacologic-targeted agents to tailor treatment of acute myeloid leukemia (AML) in individual patients. However, the use of targeted therapies in AML has met with only modest success. Molecular studies have identified AML subsets characterized by driver mutational events, such as NPM1, FLT3-ITD and IDH1-2 mutations, and have provided preclinical evidence that the targeting of these mutant molecules could represent a valuable therapeutic strategy. Recent studies have provided the first pieces of evidence that FLT3 targeting in FLT3-mutant AMLs, IDH1/2 inhibition in IDH-mutant AMLs and targeting membrane molecules preferentially expressed on leukemic progenitor/stem cells, such as CD33 and CD123, represent a clinically valuable strategy.
机译:下一代测序技术的快速进步和负责白血病发展的分子驱动事件的鉴定是对新的药物靶向剂的门打开,以定制个别患者的急性髓性白血病(AML)的治疗。 然而,在AML中使用有针对性的疗法仅符合适度的成功。 分子研究已经鉴定了由驾驶员突变事件的AML子集,例如NPM1,FLT3-ITD和IDH1-2突变,并且提供了这些突变分子对这些突变分子的靶向的临床前证据可以代表一种有价值的治疗策略。 最近的研究提供了第一件证据,即FLT3靶向FLT3-突变体AML,IDH1 / 2抑制在IDH-突变体AML和优先在白血病祖细胞/干细胞(如CD33和CD123)中的靶向膜分子,代表临床价值 战略。

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