Multi-omic longitudinal study reveals immune correlates of clinical course among hospitalized COVID-19 patients

IMPACC Network

doi:10.1016/j.xcrm.2023.101079

Multi-omic longitudinal study reveals immune correlates of clinical course among hospitalized COVID-19 patients

IMPACC Network

Research output: Contribution to journal › Article › peer-review

6 Scopus citations

Abstract

The IMPACC cohort, composed of >1,000 hospitalized COVID-19 participants, contains five illness trajectory groups (TGs) during acute infection (first 28 days), ranging from milder (TG1–3) to more severe disease course (TG4) and death (TG5). Here, we report deep immunophenotyping, profiling of >15,000 longitudinal blood and nasal samples from 540 participants of the IMPACC cohort, using 14 distinct assays. These unbiased analyses identify cellular and molecular signatures present within 72 h of hospital admission that distinguish moderate from severe and fatal COVID-19 disease. Importantly, cellular and molecular states also distinguish participants with more severe disease that recover or stabilize within 28 days from those that progress to fatal outcomes (TG4 vs. TG5). Furthermore, our longitudinal design reveals that these biologic states display distinct temporal patterns associated with clinical outcomes. Characterizing host immune responses in relation to heterogeneity in disease course may inform clinical prognosis and opportunities for intervention.

Original language	English (US)
Article number	101079
Journal	Cell Reports Medicine
Volume	4
Issue number	6
DOIs	https://doi.org/10.1016/j.xcrm.2023.101079
State	Published - Jun 20 2023

Keywords

COVID-19
SARS-CoV-2
immunophenotyping
longitudinal modeling
multi-omics
systems immunology

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

Access to Document

10.1016/j.xcrm.2023.101079

Cite this

@article{33fc7806644b4f74aa74e086c92ec37a,

title = "Multi-omic longitudinal study reveals immune correlates of clinical course among hospitalized COVID-19 patients",

abstract = "The IMPACC cohort, composed of >1,000 hospitalized COVID-19 participants, contains five illness trajectory groups (TGs) during acute infection (first 28 days), ranging from milder (TG1–3) to more severe disease course (TG4) and death (TG5). Here, we report deep immunophenotyping, profiling of >15,000 longitudinal blood and nasal samples from 540 participants of the IMPACC cohort, using 14 distinct assays. These unbiased analyses identify cellular and molecular signatures present within 72 h of hospital admission that distinguish moderate from severe and fatal COVID-19 disease. Importantly, cellular and molecular states also distinguish participants with more severe disease that recover or stabilize within 28 days from those that progress to fatal outcomes (TG4 vs. TG5). Furthermore, our longitudinal design reveals that these biologic states display distinct temporal patterns associated with clinical outcomes. Characterizing host immune responses in relation to heterogeneity in disease course may inform clinical prognosis and opportunities for intervention.",

keywords = "COVID-19, SARS-CoV-2, immunophenotyping, longitudinal modeling, multi-omics, systems immunology",

author = "{IMPACC Network} and Joann Diray-Arce and Slim Fourati and {Doni Jayavelu}, Naresh and Ravi Patel and Cole Maguire and Chang, {Ana C.} and Ravi Dandekar and Jingjing Qi and Lee, {Brian H.} and {van Zalm}, Patrick and Andrew Schroeder and Ernie Chen and Anna Konstorum and Anderson Brito and Gygi, {Jeremy P.} and Alvin Kho and Jing Chen and Shrikant Pawar and Gonzalez-Reiche, {Ana Silvia} and Annmarie Hoch and Milliren, {Carly E.} and Overton, {James A.} and Kerstin Westendorf and James Abraham and Michael Adkisson and Marisa Albert and {Altamirano Torres}, Luz and Bonny Alvarenga and Anderson, {Matthew L.} and Anderson, {Evan J.} and Azlann Arnett and Hiromitsu Asashima and Atkinson, {Mark A.} and Baden, {Lindsey R.} and Brenda Barton and Katherine Beach and Elizabeth Beagle and Becker, {Patrice M.} and Bell, {Matthew R.} and Mariana Bernui and Chris Bime and {Boddapati Kumar}, Arun and Booth, {Leland J.} and Brittney Borresen and Brakenridge, {Scott C.} and Laurel Bristow and Robert Bryant and Calfee, {Carolyn S.} and Hough, {Catherine L.} and Messer, {William B.}",

note = "Publisher Copyright: {\textcopyright} 2023 The Authors",

year = "2023",

month = jun,

day = "20",

doi = "10.1016/j.xcrm.2023.101079",

language = "English (US)",

volume = "4",

journal = "Cell Reports Medicine",

issn = "2666-3791",

publisher = "Cell Press",

number = "6",

}

TY - JOUR

T1 - Multi-omic longitudinal study reveals immune correlates of clinical course among hospitalized COVID-19 patients

AU - IMPACC Network

AU - Diray-Arce, Joann

AU - Fourati, Slim

AU - Doni Jayavelu, Naresh

AU - Patel, Ravi

AU - Maguire, Cole

AU - Chang, Ana C.

AU - Dandekar, Ravi

AU - Qi, Jingjing

AU - Lee, Brian H.

AU - van Zalm, Patrick

AU - Schroeder, Andrew

AU - Chen, Ernie

AU - Konstorum, Anna

AU - Brito, Anderson

AU - Gygi, Jeremy P.

AU - Kho, Alvin

AU - Chen, Jing

AU - Pawar, Shrikant

AU - Gonzalez-Reiche, Ana Silvia

AU - Hoch, Annmarie

AU - Milliren, Carly E.

AU - Overton, James A.

AU - Westendorf, Kerstin

AU - Abraham, James

AU - Adkisson, Michael

AU - Albert, Marisa

AU - Altamirano Torres, Luz

AU - Alvarenga, Bonny

AU - Anderson, Matthew L.

AU - Anderson, Evan J.

AU - Arnett, Azlann

AU - Asashima, Hiromitsu

AU - Atkinson, Mark A.

AU - Baden, Lindsey R.

AU - Barton, Brenda

AU - Beach, Katherine

AU - Beagle, Elizabeth

AU - Becker, Patrice M.

AU - Bell, Matthew R.

AU - Bernui, Mariana

AU - Bime, Chris

AU - Boddapati Kumar, Arun

AU - Booth, Leland J.

AU - Borresen, Brittney

AU - Brakenridge, Scott C.

AU - Bristow, Laurel

AU - Bryant, Robert

AU - Calfee, Carolyn S.

AU - Hough, Catherine L.

AU - Messer, William B.

PY - 2023/6/20

Y1 - 2023/6/20

N2 - The IMPACC cohort, composed of >1,000 hospitalized COVID-19 participants, contains five illness trajectory groups (TGs) during acute infection (first 28 days), ranging from milder (TG1–3) to more severe disease course (TG4) and death (TG5). Here, we report deep immunophenotyping, profiling of >15,000 longitudinal blood and nasal samples from 540 participants of the IMPACC cohort, using 14 distinct assays. These unbiased analyses identify cellular and molecular signatures present within 72 h of hospital admission that distinguish moderate from severe and fatal COVID-19 disease. Importantly, cellular and molecular states also distinguish participants with more severe disease that recover or stabilize within 28 days from those that progress to fatal outcomes (TG4 vs. TG5). Furthermore, our longitudinal design reveals that these biologic states display distinct temporal patterns associated with clinical outcomes. Characterizing host immune responses in relation to heterogeneity in disease course may inform clinical prognosis and opportunities for intervention.

AB - The IMPACC cohort, composed of >1,000 hospitalized COVID-19 participants, contains five illness trajectory groups (TGs) during acute infection (first 28 days), ranging from milder (TG1–3) to more severe disease course (TG4) and death (TG5). Here, we report deep immunophenotyping, profiling of >15,000 longitudinal blood and nasal samples from 540 participants of the IMPACC cohort, using 14 distinct assays. These unbiased analyses identify cellular and molecular signatures present within 72 h of hospital admission that distinguish moderate from severe and fatal COVID-19 disease. Importantly, cellular and molecular states also distinguish participants with more severe disease that recover or stabilize within 28 days from those that progress to fatal outcomes (TG4 vs. TG5). Furthermore, our longitudinal design reveals that these biologic states display distinct temporal patterns associated with clinical outcomes. Characterizing host immune responses in relation to heterogeneity in disease course may inform clinical prognosis and opportunities for intervention.

KW - COVID-19

KW - SARS-CoV-2

KW - immunophenotyping

KW - longitudinal modeling

KW - multi-omics

KW - systems immunology

UR - http://www.scopus.com/inward/record.url?scp=85162133285&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85162133285&partnerID=8YFLogxK

U2 - 10.1016/j.xcrm.2023.101079

DO - 10.1016/j.xcrm.2023.101079

M3 - Article

C2 - 37327781

AN - SCOPUS:85162133285

SN - 2666-3791

VL - 4

JO - Cell Reports Medicine

JF - Cell Reports Medicine

IS - 6

M1 - 101079

ER -

Multi-omic longitudinal study reveals immune correlates of clinical course among hospitalized COVID-19 patients

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this