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Conservation of caspase substrates across metazoans suggests hierarchical importance of signaling pathways over specific targets and cleavage site motifs in apoptosis

机译:跨后生动物半胱天冬酶底物的保守性提示信号通路在特定靶标上的重要性以及细胞凋亡中的裂解位点基序

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Caspases, cysteine proteases with aspartate specificity, are key players in programmed cell death across the metazoan lineage. Hundreds of apoptotic caspase substrates have been identified in human cells. Some have been extensively characterized, revealing key functional nodes for apoptosis signaling and important drug targets in cancer. But the functional significance of most cuts remains mysterious. We set out to better understand the importance of caspase cleavage specificity in apoptosis by asking which cleavage events are conserved across metazoan model species. Using N-terminal labeling followed by mass spectrometry, we identified 257 caspase cleavage sites in mouse, 130 in Drosophila, and 50 in Caenorhabditis elegans. The large majority of the caspase cut sites identified in mouse proteins were found conserved in human orthologs. However, while many of the same proteins targeted in the more distantly related species were cleaved in human orthologs, the exact sites were often different. Furthermore, similar functional pathways are targeted by caspases in all four species. Our data suggest a model for the evolution of apoptotic caspase specificity that highlights the hierarchical importance of functional pathways over specific proteins, and proteins over their specific cleavage site motifs.
机译:半胱氨酸蛋白酶,具有天冬氨酸特异性的半胱氨酸蛋白酶是后生动物细胞程序性死亡的关键因素。在人类细胞中已鉴定出数百种凋亡半胱天冬酶底物。一些已经被广泛表征,揭示了凋亡信号传导和癌症中重要药物靶标的关键功能节点。但是大多数裁切的功能意义仍然是神秘的。我们着手询问后生动物模型物种中哪些裂解事件是保守的,从而更好地了解caspase裂解特异性在凋亡中的重要性。使用N端标记,然后进行质谱分析,我们在小鼠中鉴定了257个caspase裂解位点,在果蝇中鉴定了130个,在秀丽隐杆线虫中鉴定了50个。发现在小鼠蛋白质中鉴定的大多数半胱天冬酶切割位点在人类直系同源物中是保守的。然而,尽管在人类直系同源基因中切割了靶向更远亲缘物种的许多相同蛋白质,但确切的位点常常不同。此外,所有四个物种中的半胱天冬酶均靶向相似的功能途径。我们的数据提出了凋亡半胱天冬酶特异性进化的模型,该模型突出了功能性途径对特定蛋白的作用以及蛋白质对特定裂解位点基序的重要性。

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