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呼肠孤病毒感染诱导细胞转录物的稳定性和上调,这些转录物编码 TGF-β 信号转导的调节剂。

Reovirus infection induces stabilization and up-regulation of cellular transcripts that encode regulators of TGF-β signaling.

机构信息

Program in Infection and Immunity, Division of Infectious Diseases and International Medicine, Department of Medicine, University of Minnesota, Minneapolis, Minnesota, United States of America.

Institute for Molecular Virology Training Program, Graduate Program in Comparative and Molecular Bioscience, University of Minnesota, Minneapolis, Minnesota, United States of America.

出版信息

PLoS One. 2018 Sep 27;13(9):e0204622. doi: 10.1371/journal.pone.0204622. eCollection 2018.

Abstract

Reovirus infection induces dramatic changes in host mRNA expression. We utilized oligonucleotide microarrays to measure cellular mRNA decay rates in mock- or reovirus-infected murine L929 cells to determine if changes in host mRNA expression are a consequence of reovirus-induced alterations in cellular mRNA stability. Our analysis detected a subset of cellular transcripts that were coordinately induced and stabilized following infection with the reovirus isolates c87 and c8, strains that led to an inhibition of cellular translation, but not following infection with Dearing, a reovirus isolate that did not negatively impact cellular translation. The induced and stabilized transcripts encode multiple regulators of TGF- β signaling, including components of the Smad signaling network and apoptosis/survival pathways. The coordinate induction, through mRNA stabilization, of multiple genes that encode components of TGF-β signaling pathways represents a novel mechanism by which the host cell responds to reovirus infection.

摘要

呼肠孤病毒感染会引起宿主 mRNA 表达的显著变化。我们利用寡核苷酸微阵列来测量模拟或呼肠孤病毒感染的鼠 L929 细胞中的细胞 mRNA 降解率,以确定宿主 mRNA 表达的变化是否是呼肠孤病毒诱导的细胞 mRNA 稳定性改变的结果。我们的分析检测到一组细胞转录本,它们在感染呼肠孤病毒分离株 c87 和 c8 后被协调诱导和稳定,这两种分离株会抑制细胞翻译,但感染 Dearing 后不会,Dearing 是一种不会对细胞翻译产生负面影响的呼肠孤病毒分离株。被诱导和稳定的转录本编码 TGF-β 信号的多个调节剂,包括 Smad 信号网络和凋亡/存活途径的成分。通过 mRNA 稳定来协调诱导多个基因,这些基因编码 TGF-β 信号通路的成分,代表了宿主细胞对呼肠孤病毒感染的一种新的反应机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9c3f/6160134/185644adb33c/pone.0204622.g001.jpg

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