急性髓系白血病对DEAD盒RNA解旋酶DDX5的获得性依赖。
Acquired dependence of acute myeloid leukemia on the DEAD-box RNA helicase DDX5.
作者信息
Mazurek Anthony, Park Youngkyu, Miething Cornelius, Wilkinson John E, Gillis Jesse, Lowe Scott W, Vakoc Christopher R, Stillman Bruce
机构信息
Cold Spring Harbor Laboratory, 1 Bungtown Road, Cold Spring Harbor, NY 11724, USA.
Memorial Sloan-Kettering Cancer Center, 415 E. 68(th) Street, Box 373, New York, NY 10065, USA.
出版信息
Cell Rep. 2014 Jun 26;7(6):1887-99. doi: 10.1016/j.celrep.2014.05.019. Epub 2014 Jun 5.
Abstract
Acute myeloid leukemia (AML) therapy involves compounds that are cytotoxic to both normal and cancer cells, and relapsed AML is resistant to subsequent chemotherapy. Thus, agents are needed that selectively kill AML cells with minimal toxicity. Here, we report that AML is dependent on DDX5 and that inhibiting DDX5 expression slows AML cell proliferation in vitro and AML progression in vivo but is not toxic to cells from normal bone marrow. Inhibition of DDX5 expression in AML cells induces apoptosis via induction of reactive oxygen species (ROS). This apoptotic response can be blocked either by BCL2 overexpression or treatment with the ROS scavenger N-acetyl-L-cysteine. Combining DDX5 knockdown with a BCL2 family inhibitor cooperates to induce cell death in AML cells. By inhibiting DDX5 expression in vivo, we show that DDX5 is dispensable for normal hematopoiesis and tissue homeostasis. These results validate DDX5 as a potential target for blocking AML.
摘要
急性髓系白血病(AML)的治疗涉及对正常细胞和癌细胞均具有细胞毒性的化合物,而复发性AML对后续化疗具有抗性。因此,需要能够以最小毒性选择性杀死AML细胞的药物。在此,我们报告AML依赖于DDX5,抑制DDX5表达可减缓AML细胞在体外的增殖以及AML在体内的进展,但对正常骨髓细胞无毒。抑制AML细胞中的DDX5表达通过诱导活性氧(ROS)来诱导细胞凋亡。这种凋亡反应可通过BCL2过表达或用ROS清除剂N-乙酰-L-半胱氨酸处理来阻断。将DDX5敲低与BCL2家族抑制剂联合使用可协同诱导AML细胞死亡。通过在体内抑制DDX5表达,我们表明DDX5对于正常造血和组织稳态是可有可无的。这些结果证实DDX5是阻断AML的潜在靶点。
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