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小鼠α和β干扰素基因的细胞类型特异性表达与调控

Cell type specific expression and regulation of murine interferon alpha and beta genes.

作者信息

Hoss-Homfeld A, Zwarthoff E C, Zawatzky R

机构信息

Institute of Virus Research, German Cancer Research Center, Heidelberg, Federal Republic of Germany.

出版信息

Virology. 1989 Dec;173(2):539-50. doi: 10.1016/0042-6822(89)90566-7.

Abstract

The differential and cell type specific expression of various murine IFN alpha genes and IFN beta was examined by S1 nuclease protection assays in M-CSF cultured C57BL/6 mouse bone marrow macrophages and L929 fibroblasts. In Newcastle disease virus (NDV) induced macrophages, IFN beta, alpha 2, alpha 4, and alpha 1 mRNAs were the predominant species, whereas IFN alpha 6 and alpha 9 transcripts accounted for only 5% of total IFN alpha mRNAs. In L929 cells, only IFN beta, alpha 2, and alpha 4 genes were expressed efficiently following NDV induction and IFN alpha 9 mRNA was always below detectable level. Induction of macrophages with the synthetic inducer 10-carboxymethyl-9-acridanone resulted in small amounts of IFN alpha 2, alpha 4, and alpha 6 mRNAs and the IFN beta mRNA level was about 100-fold higher. Macrophages and L929 cells especially differed in the kinetics of IFN gene induction in that macrophages showed a much earlier transient expression of all IFN mRNA species. Additionally, IFN transcripts were degraded much faster in macrophage cultures than in L929cells. The IFN response of macrophages is thus characterized by a highly efficient control, providing a rapid onset and a rapid decline of IFN production, which limits release of IFN to a short time interval.

摘要

通过S1核酸酶保护试验,在巨噬细胞集落刺激因子(M-CSF)培养的C57BL/6小鼠骨髓巨噬细胞和L929成纤维细胞中检测了各种小鼠干扰素α基因和干扰素β的差异表达及细胞类型特异性表达。在新城疫病毒(NDV)诱导的巨噬细胞中,干扰素β、α2、α4和α1 mRNA是主要种类,而干扰素α6和α9转录本仅占总干扰素α mRNA的5%。在L929细胞中,NDV诱导后仅干扰素β、α2和α4基因有效表达,且干扰素α9 mRNA始终低于可检测水平。用合成诱导剂10-羧甲基-9-吖啶酮诱导巨噬细胞,产生少量的干扰素α2、α4和α6 mRNA,而干扰素β mRNA水平约高100倍。巨噬细胞和L929细胞在干扰素基因诱导动力学方面尤其不同,巨噬细胞中所有干扰素mRNA种类均表现出更早的瞬时表达。此外,干扰素转录本在巨噬细胞培养物中的降解速度比在L929细胞中快得多。因此,巨噬细胞的干扰素反应具有高效调控的特点,可使干扰素产生迅速启动并迅速下降,从而将干扰素的释放限制在短时间内。

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