SARS-CoV-2 innate effector associations and viral load in early nasopharyngeal infection.

Liou, Theodore G; Adler, Frederick R; Cahill, Barbara C; Cox, David R; Cox, James E; Grant, Garett J; Hanson, Kimberly E; Hartsell, Stephen C; Hatton, Nathan D; Helms, My N; Jensen, Judy L; Kartsonaki, Christiana; Li, Yanping; Leung, Daniel T; Marvin, James E; Middleton, Elizabeth A; Osburn-Staker, Sandra M; Packer, Kristyn A; Shakir, Salika M; Sturrock, Anne B; Tardif, Keith D; Warren, Kristi J; Waddoups, Lindsey J; Weaver, Lisa J; Zimmerman, Elizabeth; Paine, Robert

Liou, Theodore G; Adler, Frederick R; Cahill, Barbara C; Cox, David R; Cox, James E; Grant, Garett J; Hanson, Kimberly E; Hartsell, Stephen C; Hatton, Nathan D; Helms, My N; Jensen, Judy L; Kartsonaki, Christiana; Li, Yanping; Leung, Daniel T; Marvin, James E; Middleton, Elizabeth A; Osburn-Staker, Sandra M; Packer, Kristyn A; Shakir, Salika M; Sturrock, Anne B; Tardif, Keith D; Warren, Kristi J; Waddoups, Lindsey J; Weaver, Lisa J; Zimmerman, Elizabeth; Paine, Robert.

Liou TG; Division of Respiratory, Critical Care and Occupational Pulmonary Medicine, Department of Internal Medicine, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Adler FR; Center for Quantitative Biology, University of Utah, Salt Lake City, UT, USA.
Cahill BC; Center for Quantitative Biology, University of Utah, Salt Lake City, UT, USA.
Cox DR; Department of Mathematics and School of Biological Sciences, University of Utah, Salt Lake City, UT, USA.
Cox JE; Division of Respiratory, Critical Care and Occupational Pulmonary Medicine, Department of Internal Medicine, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Grant GJ; Nuffield College, Oxford, UK.
Hanson KE; Department of Biochemistry, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Hartsell SC; Metabolomics, Proteomics and Mass Spectrometry Core, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Hatton ND; Division of Respiratory, Critical Care and Occupational Pulmonary Medicine, Department of Internal Medicine, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Helms MN; Division of Infectious Diseases, Department of Internal Medicine, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Jensen JL; Department of Pathology, University of Utah, Salt Lake City, UT, USA.
Kartsonaki C; ARUP Laboratories, Salt Lake City, UT, USA.
Li Y; Division of Emergency Medicine, Department of Surgery, University of Utah, Salt Lake City, UT, USA.
Leung DT; Division of Respiratory, Critical Care and Occupational Pulmonary Medicine, Department of Internal Medicine, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Marvin JE; Division of Respiratory, Critical Care and Occupational Pulmonary Medicine, Department of Internal Medicine, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Middleton EA; Division of Respiratory, Critical Care and Occupational Pulmonary Medicine, Department of Internal Medicine, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Osburn-Staker SM; Clinical Trial Service Unit & Epidemiological Studies Unit and Medical Research Council Population Health Research Unit, Nuffield Department of Population Health, University of Oxford, Oxford, UK.
Packer KA; Division of Respiratory, Critical Care and Occupational Pulmonary Medicine, Department of Internal Medicine, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Shakir SM; Division of Infectious Diseases, Department of Internal Medicine, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Sturrock AB; Flow Cytometry Core Laboratory, University of Utah Health, Salt Lake City, UT, USA.
Tardif KD; Division of Respiratory, Critical Care and Occupational Pulmonary Medicine, Department of Internal Medicine, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Warren KJ; Metabolomics, Proteomics and Mass Spectrometry Core, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Waddoups LJ; Division of Respiratory, Critical Care and Occupational Pulmonary Medicine, Department of Internal Medicine, School of Medicine, University of Utah, Salt Lake City, UT, USA.
Weaver LJ; Department of Pathology, University of Utah, Salt Lake City, UT, USA.
Zimmerman E; ARUP Laboratories, Salt Lake City, UT, USA.
Paine R; Division of Respiratory, Critical Care and Occupational Pulmonary Medicine, Department of Internal Medicine, School of Medicine, University of Utah, Salt Lake City, UT, USA.

Physiol Rep ; 9(4): e14761, 2021 02.

Article in English | MEDLINE | ID: covidwho-1100463

Preprint
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ABSTRACT

ABSTRACT

COVID-19 causes severe disease with poor outcomes. We tested the hypothesis that early SARS-CoV-2 viral infection disrupts innate immune responses. These changes may be important for understanding subsequent clinical outcomes. We obtained residual nasopharyngeal swab samples from individuals who requested COVID-19 testing for symptoms at drive-through COVID-19 clinical testing sites operated by the University of Utah. We applied multiplex immunoassays, real-time polymerase chain reaction assays and quantitative proteomics to 20 virus-positive and 20 virus-negative samples. ACE-2 transcripts increased with infection (OR =17.4, 95% CI [CI] =4.78-63.8) and increasing viral N1 protein transcript load (OR =1.16, CI =1.10-1.23). Transcripts for two interferons (IFN) were elevated, IFN-λ1 (OR =71, CI =7.07-713) and IFN-λ2 (OR =40.2, CI =3.86-419), and closely associated with viral N1 transcripts (OR =1.35, CI =1.23-1.49 and OR =1.33 CI =1.20-1.47, respectively). Only transcripts for IP-10 were increased among systemic inflammatory cytokines that we examined (OR =131, CI =1.01-2620). We found widespread discrepancies between transcription and translation. IFN proteins were unchanged or decreased in infected samples (IFN-Î³ OR =0.90 CI =0.33-0.79, IFN-λ2,3 OR =0.60 CI =0.48-0.74) suggesting viral-induced shut-off of host antiviral protein responses. However, proteins for IP-10 (OR =3.74 CI =2.07-6.77) and several interferon-stimulated genes (ISG) increased with viral load (BST-1 OR =25.1, CI =3.33-188; IFIT1 OR =19.5, CI =4.25-89.2; IFIT3 OR =245, CI =15-4020; MX-1 OR =3.33, CI =1.44-7.70). Older age was associated with substantial modifications of some effects. Ambulatory symptomatic patients had an innate immune response with SARS-CoV-2 infection characterized by elevated IFN, proinflammatory cytokine and ISG transcripts, but there is evidence of a viral-induced host shut-off of antiviral responses. Our findings may characterize the disrupted immune landscape common in patients with early disease.

Subject(s)

COVID-19/immunology; Immunity, Innate/immunology; Nasopharyngeal Diseases/virology; SARS-CoV-2/immunology; Viral Load/immunology; Adolescent; Adult; Age Factors; Aged; Aged, 80 and over; COVID-19/virology; Child; Cytokines/blood; Enzyme-Linked Immunosorbent Assay; Female; Humans; Male; Middle Aged; Nasopharyngeal Diseases/immunology; RNA, Messenger/genetics; Real-Time Polymerase Chain Reaction; SARS-CoV-2/genetics; Sex Factors; Young Adult

Keywords

SARS-CoV-2; biomarkers; host shut-off; innate immunity; interferon

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Full text: Available Collection: International databases Database: MEDLINE Main subject: Nasopharyngeal Diseases / Viral Load / SARS-CoV-2 / COVID-19 / Immunity, Innate Type of study: Experimental Studies / Prognostic study Limits: Adolescent / Adult / Aged / Child / Female / Humans / Male / Middle aged / Young adult Language: English Journal: Physiol Rep Year: 2021 Document Type: Article Affiliation country: Phy2.14761

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