Severe COVID-19 is Characterised by Inflammation and Immature Myeloid Cells Early in Disease Progression

Overview

Journal Heliyon

Specialty Social Sciences

Date 2022 Apr 7

PMID 35386227

Authors

Liam Townsend

Adam H Dyer

Aifric Naughton

Sultan Imangaliyev

Jean Dunne

Rachel Kiersey

Dean Holden

Aoife Mooney

Deirdre Leavy

Katie Ridge

Jamie Sugrue

Mubarak Aldoseri

Jo Hannah Kelliher

Martina Hennessy

Declan Byrne

Paul Browne

Christopher L Bacon

Catriona Doyle

Ruth ORiordan

Anne-Marie McLaughlin

Ciaran Bannan

Ignacio Martin-Loeches

Arthur White

Rachel M McLoughlin

Colm Bergin

Nollaig M Bourke

Cliona OFarrelly

Niall Conlon

Cliona Ni Cheallaigh

Affiliations

Soon will be listed here.

Abstract

SARS-CoV-2 infection causes a wide spectrum of disease severity. Identifying the immunological characteristics of severe disease and the risk factors for their development are important in the management of COVID-19. This study aimed to identify and rank clinical and immunological features associated with progression to severe COVID-19 in order to investigate an immunological signature of severe disease. One hundred and eight patients with positive SARS-CoV-2 PCR were recruited. Routine clinical and laboratory markers were measured, as well as myeloid and lymphoid whole-blood immunophenotyping and measurement of the pro-inflammatory cytokines IL-6 and soluble CD25. All analysis was carried out in a routine hospital diagnostic laboratory. Univariate analysis demonstrated that severe disease was most strongly associated with elevated CRP and IL-6, loss of DLA-DR expression on monocytes and CD10 expression on neutrophils. Unbiased machine learning demonstrated that these four features were strongly associated with severe disease, with an average prediction score for severe disease of 0.925. These results demonstrate that these four markers could be used to identify patients developing severe COVID-19 and allow timely delivery of therapeutics.

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