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SUMO proteomics to decipher the SUMO-modified proteome regulated by various diseases

机译:SUMO蛋白质组学解读了各种疾病调节的SUMO改性蛋白质组

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Small ubiquitin-like modifier (SUMO1-3) conjugation is a posttranslational protein modification whereby SUMOs are conjugated to lysine residues of target proteins. SUMO conjugation can alter the activity, stability, and function of target proteins, and thereby modulate almost all major cellular pathways. Many diseases are associated with SUMO conjugation, including heart failure, arthritis, cancer, degenerative diseases, and brain ischemia/stroke. It is, therefore, of major interest to characterize the SUMO-modified proteome regulated by these disorders. SUMO proteomics analysis is hampered by low levels of SUMOylated proteins. Several strategies have, therefore, been developed to enrich SUMOylated proteins from cell/tissue extracts. These include proteomics analysis on cells expressing epitope-tagged SUMO isoforms, use of monoclonal SUMO antibodies for immunoprecipitation and epitope-specific peptides for elution, and affinity purification with peptides containing SUMO interaction motifs to specifically enrich polySUMOylated proteins. Recently, two mouse models were generated and characterized that express tagged SUMO isoforms, and allow purification of SUMOylated proteins from complex organ extracts. Ultimately, these new analytical tools will help to decipher the SUMO-modified proteome regulated by various human diseases, and thereby, identify new targets for preventive and therapeutic purposes.
机译:小泛素样改性剂(SUMO1-3)缀合是一种后期蛋白质修饰,由此SUMOS与靶蛋白的赖氨酸残基缀合。 SUMO缀合可以改变靶蛋白的活性,稳定性和功能,从而调节几乎所有主要的细胞途径。许多疾病与Sumo缀合有关,包括心力衰竭,关节炎,癌症,退行性疾病和脑缺血/中风。因此,主要兴趣表征这些疾病调节的SUMO改性蛋白质组。 SUMO蛋白质组学分析受到低水平的雄性蛋白质的阻碍。因此,已经开发了几种策略以富集来自细胞/组织提取物的雄性蛋白质。这些包括对表达表位标记的SUMO同种型的细胞的蛋白质组学分析,使用单克隆相扑抗体用于洗脱的免疫沉淀和表位特异性肽,以及用含有SUMO相互作用基序的肽的亲和纯化,以特异性富含多糖化蛋白。最近,产生了两种小鼠模型并表征了表达标记的Sumo同种型,并允许从复杂的器官提取物中纯化Somobated蛋白。最终,这些新的分析工具将有助于破译各种人类疾病调节的Sumo改性蛋白质组,从而识别用于预防性和治疗目的的新目标。

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