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Identification of a functional nuclear localization signal within the human USP22 protein

机译:人类USP22蛋白中功能性核定位信号的鉴定

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Ubiquitin-specific processing enzyme 22 (USP22), a member of the deubiquitinase family, is over-expressed in most human cancers and has been implicated in tumorigenesis. Because it is an enzymatic subunit of the human SAGA transcriptional cofactor, USP22 deubiquitylates histone H2A and H2B in the nucleus, thus participating in gene regulation and cell-cycle progression. However, the mechanisms regulating its nuclear translocation have not yet been elucidated. It was here demonstrated that USP22 is imported into the nucleus through a mechanism mediated by nuclear localization signal (NLS). The bipartite NLS sequence KRELELLKHNPKRRKIT (aa152-168), was identified as the functional NLS for its nuclear localization. Furthermore, a short cluster of basic amino acid residues KRRK within this bipartite NLS plays the primary role in nuclear localization and is evolutionarily conserved in USP22 homologues. In the present study, a functional NLS and the minimal sequences required for the active targeting of USP22 to the nucleus were identified. These findings may provide a molecular basis for the mechanism underlying USP22 nuclear trafficking and function.
机译:泛素特异性加工酶22(USP22)是去泛素酶家族的成员,在大多数人类癌症中均过表达,并且与肿瘤发生有关。因为USP22是人类SAGA转录辅因子的酶亚基,所以它使细胞核中的组蛋白H2A和H2B去泛素化,从而参与基因调控和细胞周期进程。但是,尚未阐明调节其核易位的机制。在此证明USP22通过核定位信号(NLS)介导的机制导入核中。两部分NLS序列KRELELLKHNPKRRKIT(aa152-168)被确定为其核定位的功能性NLS。此外,该二分体NLS中的一小簇碱性氨基酸残基KRRK在核定位中起主要作用,并且在USP22同源物中进化上保守。在本研究中,确定了功能性NLS和将USP22主动靶向细胞核所需的最小序列。这些发现可能为USP22核贩运和功能的基础机制提供分子基础。

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