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多胺调节精脒/精脒-N1-乙酰转移酶的翻译。

Polyamine-regulated translation of spermidine/spermine-N1-acetyltransferase.

机构信息

Department of Biochemistry, Temple University School of Medicine, Philadelphia, Pennsylvania, USA.

出版信息

Mol Cell Biol. 2012 Apr;32(8):1453-67. doi: 10.1128/MCB.06444-11. Epub 2012 Feb 21.

Abstract

Rapid synthesis of the polyamine catabolic enzyme spermidine/spermine-N(1)-acetyltransferase (SSAT) in response to increased polyamines is an important polyamine homeostatic mechanism. Indirect evidence has suggested that there is an important control mechanism involving the release of a translational repressor protein that allows the immediate initiation of SSAT protein synthesis without RNA transcription, maturation, or translocation. To identify a repressor protein, we used a mass spectroscopy-based RNA-protein interaction system and found six proteins that bind to the coding region of SSAT mRNA. Individual small interfering RNA (siRNA) experiments showed that nucleolin knockdown enhances SSAT translation. Nucleolin exists in several isoforms, and we report that the isoform that binds to SSAT mRNA undergoes autocatalysis in the presence of polyamines, a result suggesting that there is a negative feedback system that helps control the cellular content of polyamines. Preliminary molecular interaction data show that a nucleolin isoform binds to a 5' stem-loop of the coding region of SSAT mRNA. The glycine/arginine-rich C terminus of nucleolin is required for binding, and the four RNA recognition motif domains are included in the isoform that blocks SSAT translation. Understanding SSAT translational control mechanisms has the potential for the development of therapeutic strategies against cancer and obesity.

摘要

快速合成多胺分解酶精脒/精胺-N(1)-乙酰转移酶(SSAT)以应对多胺的增加是一种重要的多胺动态平衡机制。间接证据表明,存在一种重要的控制机制,涉及释放一种翻译抑制蛋白,允许 SSAT 蛋白合成在没有 RNA 转录、成熟或易位的情况下立即启动。为了鉴定一种抑制蛋白,我们使用了基于质谱的 RNA-蛋白相互作用系统,发现了六种与 SSAT mRNA 编码区结合的蛋白质。单独的小干扰 RNA(siRNA)实验表明,核仁蛋白的敲低增强了 SSAT 的翻译。核仁蛋白存在几种同工型,我们报告说,与 SSAT mRNA 结合的同工型在多胺存在下发生自我催化,这表明存在一种负反馈系统,有助于控制多胺的细胞含量。初步的分子相互作用数据表明,核仁蛋白的一种同工型与 SSAT mRNA 编码区的 5'茎环结合。核仁蛋白富含甘氨酸/精氨酸的 C 端是结合所必需的,并且包含阻止 SSAT 翻译的四个 RNA 识别模体结构域。了解 SSAT 翻译控制机制有可能开发针对癌症和肥胖症的治疗策略。

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