髓样细胞白血病-1是三阴性乳腺癌中一种重要的凋亡存活因子。
Myeloid cell leukemia-1 is an important apoptotic survival factor in triple-negative breast cancer.
作者信息
Goodwin C M, Rossanese O W, Olejniczak E T, Fesik S W
机构信息
Department of Pharmacology, Vanderbilt University School of Medicine, Nashville, TN, USA.
Department of Biochemistry, Vanderbilt University School of Medicine, Nashville, TN, USA.
出版信息
Cell Death Differ. 2015 Dec;22(12):2098-106. doi: 10.1038/cdd.2015.73. Epub 2015 Jun 5.
Breast cancer is the second-most frequently diagnosed malignancy in US women. The triple-negative breast cancer (TNBC) subtype, which lacks expression of the estrogen receptor, progesterone receptor and human epidermal growth factor receptor-2, afflicts 15% of patients and is refractory to current targeted therapies. Like many cancers, TNBC cells often deregulate programmed cell death by upregulating anti-apoptotic proteins of the B-cell CLL/lymphoma 2 (Bcl-2) family. One family member, myeloid cell leukemia-1 (Mcl-1), is commonly amplified in TNBC and correlates with a poor clinical prognosis. Here we show the effect of silencing Mcl-1 and Bcl-2-like protein 1 isoform 1 (Bcl-xL) expression on viability in a panel of seventeen TNBC cell lines. Cell death was observed in a subset upon Mcl-1 knockdown. In contrast, Bcl-xL knockdown only modestly reduced viability, indicating that Mcl-1 is a more important survival factor. However, dual silencing of both Mcl-1 and Bcl-xL reduced viability in most cell lines tested. These proliferation results were recapitulated by BH3 profiling experiments. Treatment with a Bcl-xL and Bcl-2 peptide had only a moderate effect on any of the TNBC cell lines, however, co-dosing an Mcl-1-selective peptide with a peptide that inhibits Bcl-xL and Bcl-2 was effective in each line tested. Similarly, the selective Bcl-xL inhibitor WEHI-539 was only weakly cytotoxic across the panel, but sensitization by Mcl-1 knockdown markedly improved its EC50. ABT-199, which selectively inhibits Bcl-2, did not synergize with Mcl-1 knockdown, indicating the relatively low importance of Bcl-2 in these lines. Mcl-1 sensitivity is not predicted by mRNA or protein levels of a single Bcl-2 family member, except for only a weak correlation for Bak and Bax protein expression. However, a more comprehensive index composed of Mcl-1, Bcl-xL, Bim, Bak and Noxa protein or mRNA expression correlates well with Mcl-1 sensitivity in TNBC and can also predict Mcl-1 dependency in non-small cell lung cancer cell lines.
乳腺癌是美国女性中第二常见的确诊恶性肿瘤。三阴性乳腺癌(TNBC)亚型缺乏雌激素受体、孕激素受体和人表皮生长因子受体2的表达,影响15%的患者,并且对当前的靶向治疗无效。与许多癌症一样,TNBC细胞通常通过上调B细胞淋巴瘤/白血病-2(Bcl-2)家族的抗凋亡蛋白来解除程序性细胞死亡的调控。该家族的一个成员,髓样细胞白血病-1(Mcl-1),在TNBC中通常会扩增,并且与不良的临床预后相关。在这里,我们展示了沉默Mcl-1和Bcl-2样蛋白1亚型1(Bcl-xL)表达对一组17种TNBC细胞系活力的影响。在一部分细胞中,敲低Mcl-1后观察到细胞死亡。相比之下,敲低Bcl-xL仅适度降低了细胞活力,表明Mcl-1是更重要的生存因子。然而,同时沉默Mcl-1和Bcl-xL在大多数测试细胞系中降低了细胞活力。这些增殖结果通过BH3谱分析实验得到了验证。用Bcl-xL和Bcl-2肽处理对任何TNBC细胞系只有中等程度的影响,然而,将Mcl-1选择性肽与抑制Bcl-xL和Bcl-2的肽联合给药在每个测试细胞系中都有效。同样,选择性Bcl-xL抑制剂WEHI-539在整个细胞系中细胞毒性较弱,但通过敲低Mcl-1使其致敏显著改善了其半数有效浓度(EC50)。选择性抑制Bcl-2的ABT-199与敲低Mcl-1没有协同作用,表明Bcl-2在这些细胞系中的重要性相对较低。除了Bak和Bax蛋白表达仅有微弱的相关性外,单个Bcl-2家族成员的mRNA或蛋白水平并不能预测Mcl-1的敏感性。然而,由Mcl-1、Bcl-xL、Bim、Bak和Noxa蛋白或mRNA表达组成的更全面的指标与TNBC中Mcl-1的敏感性密切相关,并且还可以预测非小细胞肺癌细胞系中对Mcl-1的依赖性。
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