Author:
Shi Zhonghua,Bogaards Sylvia J P,Conijn Stefan,Onderwater Yeszamin,Espinosa Pedro,Bink Diewertje I,van den Berg Marloes,van de Locht Martijn,Bugiani Marianna,van der Hoeven Hans,Boon Reinier A,Heunks Leo,Ottenheijm Coen A C
Abstract
IntroductionThe diaphragm is the main muscle of inspiration, and its dysfunction contributes to adverse clinical outcomes in critically ill patients. We recently reported the infiltration of SARS-CoV-2, and the development of fibrosis, in the diaphragm of critically ill patients with COVID-19. In the current study, we aimed to characterise myofiber structure in the diaphragm of critically ill patients with COVID-19.MethodsDiaphragm muscle specimens were collected during autopsy from patients who died of COVID-19 in three academic medical centres in the Netherlands in April and May 2020 (n=27). We studied diaphragm myofiber gene expression and structure and compared the findings obtained to those of deceased critically ill patients without COVID-19 (n=10).ResultsMyofibers of critically ill patients with COVID-19 showed on average larger cross-sectional area (slow-twitch myofibers: 2441±229 vs 1571±309 µm2; fast-twitch myofibers: 1966±209 vs 1225±222 µm2). Four critically ill patients with COVID-19 showed extremely large myofibers, which were splitting and contained many centralised nuclei. RNA-sequencing data revealed differentially expressed genes involved in muscle regeneration.ConclusionDiaphragm of critically ill patients with COVID-19 has distinct myopathic features compared with critically ill patients without COVID-19, which may contribute to the ongoing dyspnoea and fatigue in the patients surviving COVID-19 infection.
Funder
National Institutes of Health - Heart Lung and Blood Institute
Subject
Pulmonary and Respiratory Medicine
Cited by
7 articles.
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