Literature DB >> 33630927

Transcriptomic profiling and genomic mutational analysis of Human coronavirus (HCoV)-229E -infected human cells.

Nehemya Friedman1,2, Jasmine Jacob-Hirsch3,4, Yaron Drori1,2, Eyal Eran3,4, Nitzan Kol3,4, Omri Nayshool3,4, Ella Mendelson1,2, Gideon Rechavi3,4, Michal Mandelboim1,2.   

Abstract

Human coronaviruses (HCoVs) cause mild to severe respiratory infection. Most of the common cold illnesses are caused by one of four HCoVs, namely HCoV-229E, HCoV-NL63, HCoV-HKU1 and HCoV-OC43. Several studies have applied global transcriptomic methods to understand host responses to HCoV infection, with most studies focusing on the pandemic severe acute respiratory syndrome coronavirus (SARS-CoV), Middle East respiratory syndrome CoV (MERS-CoV) and the newly emerging SARS-CoV-2. In this study, Next Generation Sequencing was used to gain new insights into cellular transcriptomic changes elicited by alphacoronavirus HCoV-229E. HCoV-229E-infected MRC-5 cells showed marked downregulation of superpathway of cholesterol biosynthesis and eIF2 signaling pathways. Moreover, upregulation of cyclins, cell cycle control of chromosomal replication, and the role of BRCA1 in DNA damage response, alongside downregulation of the cell cycle G1/S checkpoint, suggest that HCoV-229E may favors S phase for viral infection. Intriguingly, a significant portion of key factors of cell innate immunity, interferon-stimulated genes (ISGs) and other transcripts of early antiviral response genes were downregulated early in HCoV-229E infection. On the other hand, early upregulation of the antiviral response factor Apolipoprotein B mRNA editing enzyme catalytic subunit 3B (APOBEC3B) was observed. APOBEC3B cytidine deaminase signature (C-to-T) was previously observed in genomic analysis of SARS-CoV-2 but not HCoV-229E. Higher levels of C-to-T mutations were found in countries with high mortality rates caused by SARS-CoV-2. APOBEC activity could be a marker for new emerging CoVs. This study will enhance our understanding of commonly circulating HCoVs and hopefully provide critical information about still-emerging coronaviruses.

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Year:  2021        PMID: 33630927      PMCID: PMC7906355          DOI: 10.1371/journal.pone.0247128

Source DB:  PubMed          Journal:  PLoS One        ISSN: 1932-6203            Impact factor:   3.240


  72 in total

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2.  APOBEC-mediated editing of viral RNA.

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Review 3.  Continuous and Discontinuous RNA Synthesis in Coronaviruses.

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Journal:  Annu Rev Virol       Date:  2015-11       Impact factor: 10.431

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Journal:  J Biol Chem       Date:  2004-10-04       Impact factor: 5.157

6.  ViPR: an open bioinformatics database and analysis resource for virology research.

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Review 7.  Interferon-stimulated genes and their antiviral effector functions.

Authors:  John W Schoggins; Charles M Rice
Journal:  Curr Opin Virol       Date:  2011-12       Impact factor: 7.090

8.  Characterization of the Lipidomic Profile of Human Coronavirus-Infected Cells: Implications for Lipid Metabolism Remodeling upon Coronavirus Replication.

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9.  HCFC2 is needed for IRF1- and IRF2-dependent Tlr3 transcription and for survival during viral infections.

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10.  Human Coronavirus Infections in Israel: Epidemiology, Clinical Symptoms and Summer Seasonality of HCoV-HKU1.

Authors:  Nehemya Friedman; Hadar Alter; Musa Hindiyeh; Ella Mendelson; Yonat Shemer Avni; Michal Mandelboim
Journal:  Viruses       Date:  2018-09-21       Impact factor: 5.048

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  8 in total

Review 1.  The potential role of COVID-19 in the induction of DNA damage.

Authors:  Pablo Pánico; Patricia Ostrosky-Wegman; Ana María Salazar
Journal:  Mutat Res Rev Mutat Res       Date:  2022-01-19       Impact factor: 7.015

2.  Structure-Based Design of First-Generation Small Molecule Inhibitors Targeting the Catalytic Pockets of AID, APOBEC3A, and APOBEC3B.

Authors:  Justin J King; Faezeh Borzooee; Junbum Im; Mahdi Asgharpour; Atefeh Ghorbani; Cody P Diamond; Heather Fifield; Lesley Berghuis; Mani Larijani
Journal:  ACS Pharmacol Transl Sci       Date:  2021-07-19

3.  Nitric-oxide enriched plasma-activated water inactivates 229E coronavirus and alters antiviral response genes in human lung host cells.

Authors:  Nagendra Kumar Kaushik; Pradeep Bhartiya; Neha Kaushik; Yungoh Shin; Linh Nhat Nguyen; Jang Sick Park; Doyoung Kim; Eun Ha Choi
Journal:  Bioact Mater       Date:  2022-05-08

4.  Differing coronavirus genres alter shared host signaling pathways upon viral infection.

Authors:  Diana Cruz-Pulido; Wilberforce Zachary Ouma; Scott P Kenney
Journal:  Sci Rep       Date:  2022-06-13       Impact factor: 4.996

5.  Impacts of p97 on Proteome Changes in Human Cells during Coronaviral Replication.

Authors:  Kai-Wen Cheng; Shan Li; Feng Wang; Nallely M Ruiz-Lopez; Nadia Houerbi; Tsui-Fen Chou
Journal:  Cells       Date:  2021-10-29       Impact factor: 6.600

6.  Flavonols and dihydroflavonols inhibit the main protease activity of SARS-CoV-2 and the replication of human coronavirus 229E.

Authors:  Yue Zhu; Frank Scholle; Samantha C Kisthardt; De-Yu Xie
Journal:  Virology       Date:  2022-04-12       Impact factor: 3.513

7.  Cross-GWAS coherence test at the gene and pathway level.

Authors:  Daniel Krefl; Sven Bergmann
Journal:  PLoS Comput Biol       Date:  2022-09-26       Impact factor: 4.779

8.  Commentary on "Poor evidence for host-dependent regular RNA editing in the transcriptome of SARS-CoV-2".

Authors:  F Martignano; S Di Giorgio; G Mattiuz; S G Conticello
Journal:  J Appl Genet       Date:  2022-03-12       Impact factor: 2.653

  8 in total

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