AUTHOR=Wang Ya , Schughart Klaus , Pelaia Tiana Maria , Chew Tracy , Kim Karan , Karvunidis Thomas , Knippenberg Ben , Teoh Sally , Phu Amy L. , Short Kirsty R. , Iredell Jonathan , Thevarajan Irani , Audsley Jennifer , Macdonald Stephen , Burcham Jonathon , McLean Anthony , PREDICT-19 consortium , Tang Benjamin , Shojaei Maryam , Ballestrero Alberto , Cripps Allan , Cox Amanda , Phu Amy L , De Maria Andrea , McLean Anthony , Kulasinghe Arutha , Marais Ben , Tang Benjamin , Feng Carl , Chaussabel Damien , Rinchai Darawan , Bedognetti Davide , Zoppoli Gabriele , Gunawan Gunawan , Thevarajan Irani , Audsley Jennifer , Eden John-Sebastian , Iredell Jonathan , Kim Karan , Short Kirsty Renfree , Schughart Klaus , Chakraborty Mandira , Kralovcova Marcela , Nalos Marek , Radic Marko , Matejovic Martin , Shojaei Maryam , Carney Meagan , Bedognetti Michele , Prucha Miroslav , Toufiq Mohammed , Deshpande Nandan , Teluguakula Narasaraju , West Nicholas , Cremonesi Paolo , Britton Philip , Branco Ricardo Garcia , Thiebaut Rodolphe , Bilyy Rostyslav , Teoh Sally , MacDonald Stephen , Sorrell Tania , Karvunidis Thomas , Pelaia Tiana Maria , Kwan Tim , Chew Tracy , Phan Tri Giang , Herwanto Velma , Kuan Win Sen , Wang Ya , Zerbib Yoann TITLE=Blood transcriptome responses in patients correlate with severity of COVID-19 disease JOURNAL=Frontiers in Immunology VOLUME=13 YEAR=2023 URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2022.1043219 DOI=10.3389/fimmu.2022.1043219 ISSN=1664-3224 ABSTRACT=Background

Coronavirus disease 2019 (COVID-19) is an infectious disease caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Infected individuals display a wide spectrum of disease severity, as defined by the World Health Organization (WHO). One of the main factors underlying this heterogeneity is the host immune response, with severe COVID-19 often associated with a hyperinflammatory state.

Aim

Our current study aimed to pinpoint the specific genes and pathways underlying differences in the disease spectrum and outcomes observed, through in-depth analyses of whole blood transcriptomics in a large cohort of COVID-19 participants.

Results

All WHO severity levels were well represented and mild and severe disease displaying distinct gene expression profiles. WHO severity levels 1-4 were grouped as mild disease, and signatures from these participants were different from those with WHO severity levels 6-9 classified as severe disease. Severity level 5 (moderate cases) presented a unique transitional gene signature between severity levels 2-4 (mild/moderate) and 6-9 (severe) and hence might represent the turning point for better or worse disease outcome. Gene expression changes are very distinct when comparing mild/moderate or severe cases to healthy controls. In particular, we demonstrated the hallmark down-regulation of adaptive immune response pathways and activation of neutrophil pathways in severe compared to mild/moderate cases, as well as activation of blood coagulation pathways.

Conclusions

Our data revealed discrete gene signatures associated with mild, moderate, and severe COVID-19 identifying valuable candidates for future biomarker discovery.