首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Lyn-mediated procaspase 8 dimerization blocks apoptotic signaling in B-cell chronic lymphocytic leukemia
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Lyn-mediated procaspase 8 dimerization blocks apoptotic signaling in B-cell chronic lymphocytic leukemia

机译:Lyn介导的procaspase 8二聚化可阻断B细胞慢性淋巴细胞白血病中的凋亡信号传导

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摘要

Lyn, a member of the group of tyrosine kinases named the Src family kinases (SFKs), is overexpressed, associated with an aberrant multiprotein complex and constitutively active in B-cell chronic lymphocytic leukemia (B-CLL) cells, resulting in a high level of tyrosine phosphorylation and contributing to their resistance to apoptosis. By using biochemical and bioinformatics tools, we identified procaspase-8 (procasp8), the caspase-8 zymogen, as a cytosolic target for Lyn in B-CLL cells, the phosphorylation of which at Tyr380 promotes the formation of an inactive procasp8 homodimer. This complex remains segregated in the cytosol and appears to be crucial in mediating the antiapoptotic function of Lyn in this disease. The significance of the Lyn-procasp8 axis in impairing apoptosis in B-CLL cells was further confirmed by pharmacological and genetic inhibition of procasp8, which drastically reduced the apoptosis induced by the SFK inhibitors PP2 and dasatinib. Our data highlight that Lyn's dysregulated expression, activity, and localization in B-CLLs support resistance to cell demise by inhibiting an early player of apoptotic signaling, and potentially broaden the perspectives of developing new strategies for the treatment of this disease.
机译:Lyn,酪氨酸激酶组成员Src家族激酶(SFKs),过表达,与异常的多蛋白复合物相关,在B细胞慢性淋巴细胞性白血病(B-CLL)细胞中具有组成型活性,导致高水平酪氨酸磷酸化作用及其对细胞凋亡的抵抗力通过使用生化和生物信息学工具,我们确定了procaspase-8(procasp8),即caspase-8酶原,是B-CLL细胞中Lyn的胞质靶标,其在Tyr380的磷酸化促进了无活性的procasp8 homodimer的形成。该复合物仍被隔离在细胞质中,似乎在介导Lyn对该疾病的抗凋亡功能中起着至关重要的作用。 Lyn-procasp8轴在削弱B-CLL细胞凋亡中的意义已通过procasp8的药理和遗传抑制作用进一步证实,这可以大大减少SFK抑制剂PP2和dasatinib诱导的凋亡。我们的数据强调,Lyn在B-CLLs中的失调表达,活性和定位可通过抑制凋亡信号的早期参与者来支持对细胞死亡的抵抗力,并有可能拓宽开发这种疾病治疗新策略的视野。

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