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Role of post-translational modification of the Y box binding protein 1 in human cancers

机译:Y盒结合蛋白1的翻译后修饰在人类癌症中的作用

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摘要

Y box binding protein-1 (YBX1) belongs to a DNA- and RNA-binding family of transcription factors, containing the highly conserved cold shock domain (CSD). YBX1 is involved in a number of cellular functions including transcription, translation, DNA damage repair etc., and it is upregulated during times of environmental stress. YBX1 is localized in both the cytoplasm and the nucleus. There, its nuclear translocation is observed in a number of cancers and is associated with poor prognosis and disease progression. Additionally, YBX1 expression is upregulated in a variety of cancers, pointing towards its role as a potential oncogene. Under certain circumstances, YBX1 also promotes the expression of multidrug resistance 1 (MDR1) gene, which is involved in the development of drug resistance. Thus, it is critical to understand the mechanism of YBX1 regulation and its downstream effects on promoting cancer development. A number of recent studies have highlighted the mechanisms of YBX1 regulation. Mass spectrometric analyses have reported several post-translational modifications that possibly play an important role in modulating YBX1 function. Phosphorylation is the most widely occurring post-translational modification in YBX1. In vivo analyses of sites like S102 and more recently, S165 illustrate the relationship of post-translational regulation of YBX1 in promoting cell proliferation and tumor growth. This review provides a comprehensive and up-to-date account of post-translational modifications identified in YBX1. This knowledge is a key in allowing us to better understand the mechanism of YBX1 regulation, which will aid in development of novel therapeutic strategies to target YBX1 in many types of cancer in the future.
机译:Y盒结合蛋白1(YBX1)属于转录因子的DNA和RNA结合家族,包含高度保守的冷休克结构域(CSD)。 YBX1参与许多细胞功能,包括转录,翻译,DNA损伤修复等,并且在环境压力期间被上调。 YBX1位于细胞质和细胞核中。在那里,在许多癌症中都观察到了其核易位,并与不良预后和疾病进展相关。此外,YBX1表达在多种癌症中上调,表明其作为潜在癌基因的作用。在某些情况下,YBX1还促进多药耐药性1(MDR1)基因的表达,该基因与耐药性的发展有关。因此,了解YBX1调节机制及其对促进癌症发展的下游影响至关重要。最近的许多研究都强调了YBX1调控的机制。质谱分析报告了几种翻译后修饰,它们可能在调节YBX1功能中起重要作用。磷酸化是YBX1中最广泛发生的翻译后修饰。在对S102等位点的体内分析中,S165阐明了YBX1的翻译后调控与促进细胞增殖和肿瘤生长之间的关系。该评论提供了有关YBX1中确定的翻译后修饰的全面且最新的描述。这些知识是使我们能够更好地了解YBX1调控机制的关键,这将有助于未来针对多种类型癌症靶向YBX1的新型治疗策略的开发。

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