首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Depletion of cellular polyamines spermidine and spermine causes a total arrest in translation and growth in mammalian cells
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Depletion of cellular polyamines spermidine and spermine causes a total arrest in translation and growth in mammalian cells

机译:细胞多胺亚精胺和精胺的消耗会导致哺乳动物细胞的翻译和生长完全停滞

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摘要

The polyamines, putrescine, spermidine, and spermine, are essential polycations, intimately involved in the regulation of cellular proliferation. Although polyamines exert dynamic effects on the conformation of nucleic acids and macromolecular synthesis in vitro, their specific functions in vivo are poorly understood. We investigated the cellular function of polyamines by overexpression of a key catabolic enzyme, spermidine/spermine N1-acetyltransferase 1 (SAT1) in mammalian cells. Transient cotransfection of HeLa cells with GFP and SAT1 vectors suppressed GFP protein expression without lowering its mRNA level, an indication that the block in GFP expression was not at transcription, but at translation. Fluorescence single-cell imaging also revealed specific inhibition of endogenous protein synthesis in the SAT1 overexpressing cells, without any inhibition of synthesis of DNA or RNA. Overexpression of SAT1 using a SAT1 adenovirus led to rapid depletion of cellular spermidine and spermine, total inhibition of protein synthesis, and growth arrest within 24 h. The SAT1 effect is most likely due to depletion of spermidine and spermine, because stable polyamine analogs that are not substrates for SAT1 restored GFP and endogenous protein synthesis. Loss of polysomes with increased 80S monosomes in the polyamine-depleted cells suggests a direct role for polyamines in translation initiation. Our data provide strong evidence for a primary function of polyamines, spermidine and spermine, in translation in mammalian cells.
机译:多胺,腐胺,亚精胺和亚精胺是必需的聚阳离子,与细胞增殖的调节密切相关。尽管多胺在体外对核酸的构象和大分子合成产生动态影响,但人们对其体内的特定功能了解甚少。我们通过在哺乳动物细胞中过表达关键分解代谢酶亚精胺/亚精胺N 1 -乙酰基转移酶1(SAT1)来研究多胺的细胞功能。 HeLa细胞与GFP和SAT1载体的瞬时共转染可抑制GFP蛋白表达,而不会降低其mRNA水平,这表明GFP表达的阻滞不是在转录时,而是在翻译时。荧光单细胞成像还揭示了SAT1过表达细胞中内源蛋白质合成的特异性抑制,而没有DNA或RNA合成的任何抑制。使用SAT1腺病毒过度表达SAT1会导致细胞亚精胺和亚精胺快速耗竭,完全抑制蛋白质合成,并在24小时内停止生长。 SAT1效应最可能是由于亚精胺和精胺的消耗,因为不是SAT1底物的稳定多胺类似物恢复了GFP和内源性蛋白质的合成。在缺少多胺的细胞中,随着增加的80S单核糖体损失多核糖体,表明多胺在翻译起始中具有直接作用。我们的数据为哺乳动物细胞翻译中多胺,亚精胺和精胺的主要功能提供了有力证据。

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