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MELK is an oncogenic kinase essential for mitotic progression in basal-like breast cancer cells

机译:MELK是一种对基底样乳腺癌细胞有丝分裂进程必不可少的致癌激酶

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摘要

Despite marked advances in breast cancer therapy, basal-like breast cancer (BBC), an aggressive subtype of breast cancer usually lacking estrogen and progesterone receptors, remains difficult to treat. In this study, we report the identification of MELK as a novel oncogenic kinase from an in vivo tumorigenesis screen using a kinome-wide open reading frames (ORFs) library. Analysis of clinical data reveals a high level of MELK overexpression in BBC, a feature that is largely dependent on FoxM1, a master mitotic transcription factor that is also found to be highly overexpressed in BBC. Ablation of MELK selectively impairs proliferation of basal-like, but not luminal breast cancer cells both in vitro and in vivo. Mechanistically, depletion of MELK in BBC cells induces caspase-dependent cell death, preceded by defective mitosis. Finally, we find that Melk is not required for mouse development and physiology. Together, these data indicate that MELK is a normally non-essential kinase, but is critical for BBC and thus represents a promising selective therapeutic target for the most aggressive subtype of breast cancer.>DOI:
机译:尽管乳腺癌治疗取得了显着进展,但是基底样乳腺癌(BBC)是一种通常缺乏雌激素和孕激素受体的侵袭性乳腺癌亚型,仍然难以治疗。在这项研究中,我们报告了使用全基因组开放阅读框(ORF)库从体内肿瘤发生筛选中鉴定出MELK作为一种新型致癌激酶。临床数据分析显示,BBC中MELK的表达水平较高,这一功能主要取决于FoxM1,FoxM1是一种有丝分裂的转录因子,在BBC中也高度表达。 MELK的切除在体外和体内都选择性地损害了基底样而不是管腔型乳腺癌细胞的增殖。从机理上讲,BBC细胞中MELK的消耗会诱导caspase依赖性细胞死亡,然后出现有丝分裂。最后,我们发现Melk对于鼠标发育和生理而言不是必需的。总之,这些数据表明MELK是通常非必需的激酶,但对BBC至关重要,因此代表了针对最具攻击性的乳腺癌亚型的有希望的选择性治疗靶标。> DOI:

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