High-Density Blood Transcriptomics Reveals Precision Immune Signatures of SARS-CoV-2 Infection in Hospitalized Individuals.

Prokop, Jeremy W; Hartog, Nicholas L; Chesla, Dave; Faber, William; Love, Chanise P; Karam, Rachid; Abualkheir, Nelly; Feldmann, Benjamin; Teng, Li; McBride, Tamara; Leimanis, Mara L; English, B Keith; Holsworth, Amanda; Frisch, Austin; Bauss, Jacob; Kalpage, Nathisha; Derbedrossian, Aram; Pinti, Ryan M; Hale, Nicole; Mills, Joshua; Eby, Alexandra; VanSickle, Elizabeth A; Pageau, Spencer C; Shankar, Rama; Chen, Bin; Carcillo, Joseph A; Sanfilippo, Dominic; Olivero, Rosemary; Bupp, Caleb P; Rajasekaran, Surender

Prokop, Jeremy W; Hartog, Nicholas L; Chesla, Dave; Faber, William; Love, Chanise P; Karam, Rachid; Abualkheir, Nelly; Feldmann, Benjamin; Teng, Li; McBride, Tamara; Leimanis, Mara L; English, B Keith; Holsworth, Amanda; Frisch, Austin; Bauss, Jacob; Kalpage, Nathisha; Derbedrossian, Aram; Pinti, Ryan M; Hale, Nicole; Mills, Joshua; Eby, Alexandra; VanSickle, Elizabeth A; Pageau, Spencer C; Shankar, Rama; Chen, Bin; Carcillo, Joseph A; Sanfilippo, Dominic; Olivero, Rosemary; Bupp, Caleb P; Rajasekaran, Surender.

Prokop JW; Department of Pediatrics and Human Development, College of Human Medicine, Michigan State University, Grand Rapids, MI, United States.
Hartog NL; Department of Pharmacology and Toxicology, Michigan State University, East Lansing, MI, United States.
Chesla D; Department of Pediatrics and Human Development, College of Human Medicine, Michigan State University, Grand Rapids, MI, United States.
Faber W; Allergy & Immunology, Spectrum Health, Grand Rapids, MI, United States.
Love CP; Office of Research, Spectrum Health, Grand Rapids, MI, United States.
Karam R; Department of Obstetrics, Gynecology and Reproductive Biology, College of Human Medicine, Michigan State University, Grand Rapids, MI, United States.
Abualkheir N; Physical Sciences, Grand Rapids Community College, Grand Rapids, MI, United States.
Feldmann B; Office of Research, Spectrum Health, Grand Rapids, MI, United States.
Teng L; Ambry Genetics, Aliso Viejo, CA, United States.
McBride T; Ambry Genetics, Aliso Viejo, CA, United States.
Leimanis ML; Ambry Genetics, Aliso Viejo, CA, United States.
English BK; Ambry Genetics, Aliso Viejo, CA, United States.
Holsworth A; Ambry Genetics, Aliso Viejo, CA, United States.
Frisch A; Department of Pediatrics and Human Development, College of Human Medicine, Michigan State University, Grand Rapids, MI, United States.
Bauss J; Pediatric Intensive Care Unit, Helen DeVos Children's Hospital, Grand Rapids, MI, United States.
Kalpage N; Department of Pediatrics and Human Development, College of Human Medicine, Michigan State University, Grand Rapids, MI, United States.
Derbedrossian A; Allergy & Immunology, Spectrum Health, Grand Rapids, MI, United States.
Pinti RM; Department of Pediatrics and Human Development, College of Human Medicine, Michigan State University, Grand Rapids, MI, United States.
Hale N; Department of Pediatrics and Human Development, College of Human Medicine, Michigan State University, Grand Rapids, MI, United States.
Mills J; Department of Pediatrics and Human Development, College of Human Medicine, Michigan State University, Grand Rapids, MI, United States.
Eby A; Department of Pediatrics and Human Development, College of Human Medicine, Michigan State University, Grand Rapids, MI, United States.
VanSickle EA; Department of Pediatrics and Human Development, College of Human Medicine, Michigan State University, Grand Rapids, MI, United States.
Pageau SC; The Department of Chemistry and Biochemistry, Calvin University, Grand Rapids, MI, United States.
Shankar R; Department of Biology, Grand Valley State University, Allendale, MI, United States.
Chen B; Department of Science, Davenport University, Grand Rapids, MI, United States.
Carcillo JA; Allergy & Immunology, Spectrum Health, Grand Rapids, MI, United States.
Sanfilippo D; Office of Research, Spectrum Health, Grand Rapids, MI, United States.
Olivero R; Department of Pediatrics and Human Development, College of Human Medicine, Michigan State University, Grand Rapids, MI, United States.
Bupp CP; Department of Pharmacology and Toxicology, Michigan State University, East Lansing, MI, United States.
Rajasekaran S; Department of Pediatrics and Human Development, College of Human Medicine, Michigan State University, Grand Rapids, MI, United States.

Front Immunol ; 12: 694243, 2021.

Article in English | MEDLINE | ID: covidwho-1337641

ABSTRACT

ABSTRACT

The immune response to COVID-19 infection is variable. How COVID-19 influences clinical outcomes in hospitalized patients needs to be understood through readily obtainable biological materials, such as blood. We hypothesized that a high-density analysis of host (and pathogen) blood RNA in hospitalized patients with SARS-CoV-2 would provide mechanistic insights into the heterogeneity of response amongst COVID-19 patients when combined with advanced multidimensional bioinformatics for RNA. We enrolled 36 hospitalized COVID-19 patients (11 died) and 15 controls, collecting 74 blood PAXgene RNA tubes at multiple timepoints, one early and in 23 patients after treatment with various therapies. Total RNAseq was performed at high-density, with >160 million paired-end, 150 base pair reads per sample, representing the most sequenced bases per sample for any publicly deposited blood PAXgene tube study. There are 770 genes significantly altered in the blood of COVID-19 patients associated with antiviral defense, mitotic cell cycle, type I interferon signaling, and severe viral infections. Immune genes activated include those associated with neutrophil mechanisms, secretory granules, and neutrophil extracellular traps (NETs), along with decreased gene expression in lymphocytes and clonal expansion of the acquired immune response. Therapies such as convalescent serum and dexamethasone reduced many of the blood expression signatures of COVID-19. Severely ill or deceased patients are marked by various secondary infections, unique gene patterns, dysregulated innate response, and peripheral organ damage not otherwise found in the cohort. High-density transcriptomic data offers shared gene expression signatures, providing unique insights into the immune system and individualized signatures of patients that could be used to understand the patient's clinical condition. Whole blood transcriptomics provides patient-level insights for immune activation, immune repertoire, and secondary infections that can further guide precision treatment.

Subject(s)

Blood Proteins/genetics; COVID-19/immunology; Interferon Type I/genetics; Neutrophils/physiology; SARS-CoV-2/physiology; Adult; Aged; Aged, 80 and over; Disease Progression; Female; Gene Expression Profiling; Hospitalization; Humans; Immunity; Immunity, Innate; Male; Middle Aged; Sequence Analysis, RNA; Transcriptome; Young Adult

Keywords

COVID-19; RNAseq; SARS-CoV-2; blood transcriptomics; immune cell deconvolution; immune repertoire; interferon response; secondary infections

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Full text: Available Collection: International databases Database: MEDLINE Main subject: Blood Proteins / Interferon Type I / SARS-CoV-2 / COVID-19 / Neutrophils Type of study: Cohort study / Observational study / Prognostic study Limits: Adult / Aged / Female / Humans / Male / Middle aged / Young adult Language: English Journal: Front Immunol Year: 2021 Document Type: Article Affiliation country: Fimmu.2021.694243

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