首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Selinexor is effective in acquired resistance to ibrutinib and synergizes with ibrutinib in chronic lymphocytic leukemia
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Selinexor is effective in acquired resistance to ibrutinib and synergizes with ibrutinib in chronic lymphocytic leukemia

机译:Selinexor有效地对伊布洛替尼的抗性,并在慢性淋巴细胞白血病中促进伊布鲁西布促进

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Despite the therapeutic efficacy of ibrutinib in chronic lymphocytic leukemia (CLL), complete responses are infrequent, and acquired resistance to Bruton agammaglobulinemia tyrosine kinase (BTK) inhibition is being observed in an increasing number of patients. Combination regimens that increase frequency of complete remissions, accelerate time to remission, and overcome single agent resistance are of considerable interest. We previously showed that the XPO1 inhibitor selinexor is proapoptotic in CLL cells and disrupts B-cell receptor signaling via BTK depletion. Herein we show the combination of selinexor and ibrutinib elicits a synergistic cytotoxic effect in primary CLL cells and increases overall survival compared with ibrutinib alone in a mouse model of CLL. Selinexor is effective in cells isolated from patients with prolonged lymphocytosis following ibrutinib therapy. Finally, selinexor is effective in ibrutinib-refractory mice and in a cell line harboring the BTK C481S mutation. This is the first report describing the combined activity of ibrutinib and selinexor in CLL, which represents a new treatment paradigm and warrants further evaluation in clinical trials of CLL patients including those with acquired ibrutinib resistance.
机译:尽管Ibrutinib在慢性淋巴细胞白血病(CLL)中的治疗效果,但完全应答罕见,并且在越来越多的患者中,正在观察到对伯顿时氨酸蛋白血症酪氨酸激酶(BTK)抑制的抗性。增加完全剩余频率的组合方案,加速缓解时间,并克服单一的药物抗性具有相当大的兴趣。之前,我们据表明,XPO1抑制剂Selinexor在CLL细胞中促使溶液,并通过BTK耗尽破坏B细胞受体信号传导。在此,我们展示苯胺克洛和伊布洛替尼的组合在初级CLL细胞中引发了协同细胞毒性效应,与单独的CLL小鼠模型中单独的伊布洛尼布相比增加了整体存活。塞雷宁克洛斯在伊布勒替尼治疗后延长淋巴细胞增多患者分离的细胞中是有效的。最后,塞里宁克洛斯在伊布勒替尼 - 难治小鼠中是有效的,并且在涉及BTK C481S突变的细胞系中。这是第一报告,描述CLL中伊布洛替尼和塞里宁克罗宁的组合活性,这代表了一种新的治疗范式,并认证CLL患者的临床试验中的进一步评估,包括具有所获得的伊布勒替尼抗性的CLL患者。

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