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首页> 外文期刊>BMC Genomics >Hyaluronan- and RNA-binding deubiquitinating enzymes of USP17 family members associated with cell viability
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Hyaluronan- and RNA-binding deubiquitinating enzymes of USP17 family members associated with cell viability

机译:与细胞活力相关的USP17家族成员的透明质酸和RNA结合的去泛素化酶

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Background Protein degradation by the ubiquitin system plays a crucial role in numerous cellular signaling pathways. Deubiquitination, a reversal of ubiquitination, has been recognized as an important regulatory step in the ubiquitin-dependent degradation pathway. Results While identifying putative ubiquitin specific protease (USP) enzymes that contain a conserved Asp (I) domain in humans, 4 USP17 subfamily members, highly homologous to DUB-3, have been found (USP17K, USP17L, USP17M, and USP17N), from human chorionic villi. Expression analysis showed that USP17 transcripts are highly expressed in the heart, liver, and pancreas and are expressed moderately in various human cancerous cell lines. Amino acid sequence analysis revealed that they contain the highly conserved Cys, His, and Asp domains which are responsible for the deubiquitinating activity. Biochemical enzyme assays indicated that they have deubiquitinating activity. Interestingly, the sequence analysis showed that these proteins, with exception of USP17N, contain the putative hyaluronan/RNA binding motifs, and cetylpyridinium chloride (CPC)-precipitation analysis confirmed the association between these proteins and intracellular hyaluronan and RNA. Conclusion Here, we report that the overexpression of these proteins, with exception of USP17N, leads to apoptosis, suggesting that the hyaluronan and RNA binding motifs in these enzymes play an important role in regulating signal transduction involved in cell death.
机译:背景技术泛素系统对蛋白质的降解在众多细胞信号通路中起着至关重要的作用。去泛素化是泛素化的逆转,已被认为是泛素依赖性降解途径中的重要调控步骤。结果在鉴定推测的泛素特异性蛋白酶(USP)酶时,该酶在人体内含有一个保守的Asp(I)结构域,发现了4个与DUB-3高度同源的USP17亚家族成员(USP17K,USP17L,USP17M和USP17N),来自人绒毛膜绒毛。表达分析表明,USP17转录本在心脏,肝脏和胰腺中高度表达,在各种人类癌细胞系中中等表达。氨基酸序列分析表明,它们包含高度保守的Cys,His和Asp结构域,这些结构域负责去泛素化活性。生化酶测定表明它们具有去泛素化活性。有趣的是,序列分析表明,除USP17N外,这些蛋白质均含有假定的透明质酸/ RNA结合基序,十六烷基氯化吡啶鎓(CPC)沉淀分析证实了这些蛋白质与细胞内透明质酸和RNA之间的关联。结论在这里,我们报道了这些蛋白的过度表达(除USP17N之外)会导致细胞凋亡,这表明这些酶中的透明质酸和RNA结合基序在调节涉及细胞死亡的信号转导中起重要作用。

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