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p53改变是原代BALB/c小鼠胚胎成纤维细胞自发永生化过程中的常见事件。

p53 alteration is a common event in the spontaneous immortalization of primary BALB/c murine embryo fibroblasts.

作者信息

Harvey D M, Levine A J

机构信息

Department of Molecular Biology, Lewis Thomas Laboratory, Princeton University, New Jersey 08544-1014.

出版信息

Genes Dev. 1991 Dec;5(12B):2375-85. doi: 10.1101/gad.5.12b.2375.

DOI:10.1101/gad.5.12b.2375
PMID:1752433
Abstract

It has been shown previously that mutant p53 can act as an immortalizing gene when cotransfected into primary rat embryo fibroblasts along with a selectable marker. To determine whether a mutation at the p53 locus is a common event in the pathways leading to spontaneous cellular immortalization, 11 clonally derived BALB/c murine embryo fibroblast lines were established by passage on a 3T3 schedule and examined for p53 alterations. By the following criteria, all 11 independently established lines contain at least one mutant allele of p53. Seven of these lines have a PAb240-reactive p53 species and exhibit an extended p53 half-life as determined by pulse-chase analysis. The p53 protein species in a subset of these lines is also capable of complex formation with the constitutive heat shock protein hsc70. p53 cytoplasmic DNAs (cDNAs) from several of these lines have been cloned by reverse transcription of cytoplasmic RNA followed by PCR amplification, and the mutations have been mapped by DNA sequence analysis. Point mutation in conserved domains of p53 appears to be a common alteration in these lines, although one established line carries a 24-bp in-frame deletion of p53. The remaining four cell lines do not express detectable p53 protein. For each line there is a different molecular event underlying the lack of p53 expression: (1) deletion of at least the first 6 exons of both p53 alleles; (2) expression of a single p53 mRNA encoding a stop codon at amino acid position 173; (3) no detectable p53 mRNA; and (4) greatly diminished expression of p53 mRNA. These findings indicate that p53 alteration commonly occurs in spontaneously immortalized BALB/c mouse embryo fibroblasts passaged on a 3T3 schedule and, therefore, may be an important event for the immortalization process.

摘要

先前的研究表明,突变型p53与一个选择标记共转染到原代大鼠胚胎成纤维细胞中时,可作为一个永生化基因发挥作用。为了确定p53基因座的突变在导致细胞自发永生化的途径中是否是一个常见事件,通过按3T3培养程序传代建立了11个克隆衍生的BALB/c小鼠胚胎成纤维细胞系,并检测p53的改变情况。按照以下标准,所有11个独立建立的细胞系均含有至少一个p53突变等位基因。其中7个细胞系具有PAb240反应性p53蛋白,并且通过脉冲追踪分析确定其p53半衰期延长。这些细胞系中的一部分,其p53蛋白还能够与组成型热休克蛋白hsc70形成复合物。通过对细胞质RNA进行逆转录,随后进行PCR扩增,克隆了其中几个细胞系的p53细胞质DNA(cDNA),并通过DNA序列分析确定了突变位点。p53保守结构域中的点突变似乎是这些细胞系中的常见改变,尽管有一个建立的细胞系携带p53的24个碱基对的框内缺失。其余4个细胞系未检测到可表达的p53蛋白。对于每个细胞系,p53表达缺失背后都存在不同的分子事件:(1)两个p53等位基因的至少前6个外显子缺失;(2)单个p53 mRNA的表达,该mRNA在氨基酸位置173编码一个终止密码子;(3)未检测到p53 mRNA;(4)p53 mRNA的表达大幅减少。这些发现表明,p53改变在按3T3培养程序传代的自发永生化BALB/c小鼠胚胎成纤维细胞中普遍存在,因此可能是永生化过程中的一个重要事件。

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Genes Dev. 1991 Dec;5(12B):2375-85. doi: 10.1101/gad.5.12b.2375.
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