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Targeting of polo-like kinases and their cross talk with Aurora kinases possible therapeutic strategies in human acute myeloid leukemia?

机译:靶向polo样激酶及其与Aurora激酶的相互作用可能是人类急性髓细胞白血病的治疗策略吗?

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Introduction: Five human polo-like kinases (PLKs) have been identified, and PLK1 4 seem to interact with Aurora kinases and act as cell cycle regulators in both normal and malignant human cells. Areas covered: The present review describes i) experimental evidence for a role for PLKs and Aurora kinases in human leukemogenesis and ii) the results from clinical studies of PLK and Aurora kinase inhibitors in the treatment of human acute myeloid leukemia (AML). The review was based on searches in the PubMed and the ClinicalTrials.gov databases. These inhibitors have antiproliferative and proapoptotic effects in AML cells. Hematological and gastrointestinal toxicities are frequently dose limiting, and this may limit the use of these agents in combination with conventional AML therapy. Aurora kinase inhibitors seem to be most effective for patients with high expression of the target kinases, and the same may be true for PLK inhibitors. Expert opinion: PLK inhibition is a promising strategy for the treatment of AML. Future clinical studies have to clarify i) whether this strategy is most effective for certain subsets of patients; ii) whether multikinase inhibitors targeting several cell cycle regulators should be preferred; and iii) how this therapeutic strategy eventually should be combined with conventional antileukemic chemotherapy.
机译:简介:已经鉴定出五个人类polo样激酶(PLK),PLK1 4似乎与Aurora激酶相互作用,并在正常和恶性人类细胞中充当细胞周期调节剂。涵盖的领域:本综述描述了i)PLK和Aurora激酶在人类白血病发生中的作用的实验证据,以及ii)PLK和Aurora激酶抑制剂在治疗人类急性髓性白血病(AML)中的临床研究结果。该评价基于PubMed和ClinicalTrials.gov数据库中的搜索。这些抑制剂在AML细胞中具有抗增殖和凋亡作用。血液和胃肠道毒性通常是剂量限制的,这可能会限制将这些药物与常规AML治疗结合使用。 Aurora激酶抑制剂似乎对目标激酶高表达的患者最有效,PLK抑制剂也可能如此。专家意见:抑制PLK是治疗AML的有前途的策略。未来的临床研究必须阐明:i)该策略是否对某些患者亚组最有效; ii)是否应优先选择靶向多种细胞周期调节剂的多激酶抑制剂; iii)该治疗策略最终应与常规抗白血病化疗结合使用。

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