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腺嘌呤激酶膜相关异构体的野生型p53依赖性表达

wt p53 dependent expression of a membrane-associated isoform of adenylate kinase.

作者信息

Collavin L, Lazarevic D, Utrera R, Marzinotto S, Monte M, Schneider C

机构信息

Laboratorio Nazionale Consorzio Interuniversitario Biotecnologie, AREA Science Park, Padriciano 99, 34012 Trieste, Italy.

出版信息

Oncogene. 1999 Oct 21;18(43):5879-88. doi: 10.1038/sj.onc.1202970.

Abstract

Six novel p53-inducible transcripts were recently cloned from Val5, a murine cell line stably expressing a temperature-sensitive p53 allele. One of the isolated clones represented a novel isoform of cytosolic adenylate kinase (AK1), a highly conserved monomeric enzyme involved in cellular homeostasis of adenine nucleotides. The corresponding protein, which we named AK1beta, was specifically induced upon activation of wt p53 in Val5 cells. The AK1beta protein differs from cytoplasmic AK1 by having 18 extra amino acids at the N-terminus. The extra residues in AK1beta provide a consensus signal for N-terminal myristoylation; as expected, AK1beta was shown to localize to the plasma membrane. The human AK1 gene contains several consensus p53 binding sites and we report that p53-dependent induction of the alternative AK1beta transcript also occurs in human cells. By using antisense ablation experiments in Val5 fibroblasts we show that AK1beta plays a relevant role in the establishment of reversible cell-cycle arrest as induced by p53 in these cells. These findings suggest that within a p53-dependent genetic program, a specific isoform of adenylate kinase has a previously undescribed growth-regulatory function, which might not necessarily require its best characterized biochemical activity.

摘要

最近,从Val5(一种稳定表达温度敏感型p53等位基因的小鼠细胞系)中克隆出了6种新的p53诱导转录本。其中一个分离出的克隆代表了胞质腺苷酸激酶(AK1)的一种新亚型,AK1是一种高度保守的单体酶,参与腺嘌呤核苷酸的细胞内稳态。我们将相应的蛋白质命名为AK1β,在Val5细胞中野生型p53激活后会特异性诱导其产生。AK1β蛋白与胞质AK1的不同之处在于其N端有18个额外的氨基酸。AK1β中的这些额外残基提供了一个N端肉豆蔻酰化的共有信号;正如预期的那样,AK1β定位于质膜。人类AK1基因包含几个p53共有结合位点,我们报道在人类细胞中也会发生p53依赖的AK1β转录本的诱导。通过在Val5成纤维细胞中进行反义消融实验,我们表明AK1β在这些细胞中由p53诱导的可逆性细胞周期停滞的建立中发挥了相关作用。这些发现表明,在一个p53依赖的遗传程序中,腺苷酸激酶的一种特定亚型具有一种以前未描述的生长调节功能,这不一定需要其最具特征的生化活性。

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