Evaluation of Perturbed Iron-homeostasis in a Prospective Cohort of Patients with COVID-19

Overview

Journal Wellcome Open Res

Specialty Biomedical Engineering

Date 2022 Aug 8

PMID 35935705

Authors

Joe N Frost

Fergus Hamilton

David Arnold

Karen T Elvers

Akshay Shah

Andrew E Armitage

Alice Milne

Jorgen McKernon

Marie Attwood

Yi-Ling Chen

Luzheng Xue

Jonathan Youngs

Nicholas M Provine

Tihana Bicanic

Paul Klenerman

Hal Drakesmith

Peter Ghazal

Affiliations

Soon will be listed here.

Abstract

Marked reductions in serum iron concentrations are commonly induced during the acute phase of infection. This phenomenon, termed hypoferremia of inflammation, leads to inflammatory anemia, but could also have broader pathophysiological implications. In patients with coronavirus disease 2019 (COVID-19), hypoferremia is associated with disease severity and poorer outcomes, although there are few reported cohorts. In this study, we leverage a well characterised prospective cohort of hospitalised COVID-19 patients and perform a set of analyses focussing on iron and related biomarkers and both acute severity of COVID-19 and longer-term symptomatology. We observed no associations between acute serum iron and long-term outcomes (including fatigue, breathlessness or quality of life); however, lower haemoglobin was associated with poorer quality of life. We also quantified iron homeostasis associated parameters, demonstrating that among 50 circulating mediators of inflammation IL-6 concentrations were strongly associated with serum iron, consistent with its central role in inflammatory control of iron homeostasis. Surprisingly, we observed no association between serum hepcidin and serum iron concentrations. We also observed elevated erythroferrone concentrations in COVID-19 patients with anaemia of inflammation. These results enhance our understanding of the regulation and pathophysiological consequences of disturbed iron homeostasis during SARS-CoV-2 infection.

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