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首页> 外文期刊>Cell Reports >A Conserved Splicing Silencer Dynamically Regulates O-GlcNAc Transferase Intron Retention and O-GlcNAc Homeostasis
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A Conserved Splicing Silencer Dynamically Regulates O-GlcNAc Transferase Intron Retention and O-GlcNAc Homeostasis

机译:保守的剪接沉默子动态调节O-GlcNAc转移酶内含子的保留和O-GlcNAc体内平衡。

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Modification of nucleocytoplasmic proteins with O-GlcNAc regulates a wide variety of cellular processes and has been linked to human diseases. The enzymes O-GlcNAc transferase (OGT) and O-GlcNAcase (OGA) add and remove O-GlcNAc, but the mechanisms regulating their expression remain unclear. Here, we demonstrate that retention of the fourth intron of OGT is regulated in response to O-GlcNAc levels. We further define a conserved intronic splicing silencer (ISS) that is necessary for OGT intron retention. Deletion of the ISS in colon cancer cells leads to increases in OGT, but O-GlcNAc homeostasis is maintained by concomitant increases in OGA protein. However, the ISS-deleted cells are hypersensitive to OGA inhibition in culture and in soft agar. Moreover, growth of xenograft tumors from ISS-deleted cells is compromised in mice treated with an OGA inhibitor. Thus, ISS-mediated regulation of OGT intron retention is a key component in OGT expression and maintaining O-GlcNAc homeostasis.
机译:用O-GlcNAc修饰核质蛋白可调节多种细胞过程,并与人类疾病有关。 O-GlcNAc转移酶(OGT)和O-GlcNAcase(OGA)酶可添加和除去O-GlcNAc,但调节其表达的机制尚不清楚。在这里,我们证明了OGT的第四个内含子的保留受O-GlcNAc水平的调节。我们进一步定义了保守的内含子剪接沉默子(ISS),这对于OGT内含子的保留是必需的。结肠癌细胞中ISS的缺失导致OGT增加,但OGA蛋白的同时增加则维持了O-GlcNAc的体内平衡。但是,ISS缺失的细胞对培养物中和软琼脂中的OGA抑制非常敏感。而且,在用OGA抑制剂处理的小鼠中,来自ISS缺失的细胞的异种移植肿瘤的生长受到损害。因此,ISS介导的OGT内含子保留的调节是OGT表达和维持O-GlcNAc稳态的关键组成部分。

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