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人类细胞中β-干扰素基因表达的两级调控

Two levels of regulation of beta-interferon gene expression in human cells.

作者信息

Raj N B, Pitha P M

出版信息

Proc Natl Acad Sci U S A. 1983 Jul;80(13):3923-7. doi: 10.1073/pnas.80.13.3923.

Abstract

We cloned alpha- and beta-interferon cDNA and used them as specific probes to determine the relative levels of interferon mRNA in human fibroblasts cells induced with poly(rI).poly(rC) or Newcastle disease virus to synthesize interferon. Both inducers activated only the beta-interferon gene; however, the half life of beta-interferon mRNA in cells induced with virus was substantially longer than in poly(rI).poly(rC)-induced cells. The transcription rate of beta-interferon RNA sequences was examined in nuclei isolated from poly(rI).poly(rC)-induced cells; it was found that the induction leads to transcriptional activation of the beta-interferon gene and that the shutoff period when no interferon synthesis or cytoplasmic betamRNA are detected. Thus, the synthesis of beta interferon in poly(rI).poly-(rC)-induced human fibroblasts is controlled both by activation of transcription of the beta-interferon gene and by alteration of the beta-interferon mRNA stability.

摘要

我们克隆了α-和β-干扰素cDNA,并将它们用作特异性探针,以确定在用聚(rI)·聚(rC)或新城疫病毒诱导合成干扰素的人成纤维细胞中干扰素mRNA的相对水平。两种诱导剂均仅激活β-干扰素基因;然而,病毒诱导的细胞中β-干扰素mRNA的半衰期比聚(rI)·聚(rC)诱导的细胞中的长得多。在从聚(rI)·聚(rC)诱导的细胞中分离出的细胞核中检测了β-干扰素RNA序列的转录率;发现诱导导致β-干扰素基因的转录激活,并且在未检测到干扰素合成或细胞质βmRNA的关闭期。因此,聚(rI)·聚(rC)诱导的人成纤维细胞中β-干扰素的合成受β-干扰素基因转录激活和β-干扰素mRNA稳定性改变的控制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/26d4/394171/f760a401b4bb/pnas00639-0053-a.jpg

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