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热休克基因与早期腺病毒基因的共同调控:细胞中类似E1A活性的证据。

Common control of the heat shock gene and early adenovirus genes: evidence for a cellular E1A-like activity.

作者信息

Imperiale M J, Kao H T, Feldman L T, Nevins J R, Strickland S

出版信息

Mol Cell Biol. 1984 May;4(5):867-74. doi: 10.1128/mcb.4.5.867-874.1984.

Abstract

We have employed an antiserum specific to the 70-kilodalton human heat shock protein and a cDNA clone specific to the mRNA for this protein to analyze the expression of the gene under noninducing conditions. Expression of the heat shock gene can be detected in the absence of heat induction, and this uninduced level of expression depends greatly on the particular cell type. For instance, the basal expression of the heat shock gene is at least 50 times higher in HeLa cells than in WI38 cells at both the mRNA and protein levels. We have previously shown that the inducer of transcription of the early adenovirus genes, the E1A gene product, also induces the heat shock gene, suggesting that these genes may be subject to the same regulation. We have, therefore, investigated the control of the adenovirus genes in relation to the cellular control of the heat shock gene. We find that human cells that allow a high level of uninduced expression of the heat shock gene (i.e., HeLa cells) also allow expression of the early adenovirus genes in the absence of the E1A inducer. The same is also true for the mouse F9 teratocarcinoma cell line. F9 stem cells, which constitutively express the heat shock protein, allow early adenovirus gene expression in the absence of E1A; upon differentiation induced by retinoic acid and cyclic AMP, the cells become restrictive and early viral gene expression requires the E1A gene product. Coordinately, upon differentiation there is also a loss of heat shock protein expression.

摘要

我们使用了一种针对70千道尔顿人热休克蛋白的抗血清和一个针对该蛋白mRNA的cDNA克隆,以分析该基因在非诱导条件下的表达情况。在没有热诱导的情况下,热休克基因的表达也能被检测到,而且这种未诱导状态下的表达水平在很大程度上取决于特定的细胞类型。例如,在mRNA和蛋白质水平上,HeLa细胞中热休克基因的基础表达比WI38细胞中至少高50倍。我们之前已经表明,早期腺病毒基因转录的诱导物,即E1A基因产物,也能诱导热休克基因,这表明这些基因可能受到相同的调控。因此,我们研究了腺病毒基因的调控与热休克基因的细胞调控之间的关系。我们发现,允许热休克基因高水平未诱导表达的人类细胞(即HeLa细胞),在没有E1A诱导物的情况下也能表达早期腺病毒基因。小鼠F9畸胎瘤细胞系也是如此。组成型表达热休克蛋白的F9干细胞,在没有E1A的情况下允许早期腺病毒基因表达;在用视黄酸和环磷酸腺苷诱导分化后,细胞变得具有限制性,早期病毒基因表达需要E1A基因产物。相应地,在分化过程中热休克蛋白的表达也会丧失。

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