The fatal trajectory of pulmonary COVID-19 is driven by lobular ischemia and fibrotic remodelling

BACKGROUND: COVID-19 is characterized by a heterogeneous clinical presentation, ranging from mild symptoms to severe courses of disease. 9–20% of hospitalized patients with severe lung disease die from COVID-19 and a substantial number of survivors develop long-COVID. Our objective was to provide co...

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Autores principales: Ackermann, Maximilian, Kamp, Jan C., Werlein, Christopher, Walsh, Claire L., Stark, Helge, Prade, Verena, Surabattula, Rambabu, Wagner, Willi L., Disney, Catherine, Bodey, Andrew J., Illig, Thomas, Leeming, Diana J., Karsdal, Morten A., Tzankov, Alexandar, Boor, Peter, Kühnel, Mark P., Länger, Florian P., Verleden, Stijn E., Kvasnicka, Hans M., Kreipe, Hans H., Haverich, Axel, Black, Stephen M., Walch, Axel, Tafforeau, Paul, Lee, Peter D., Hoeper, Marius M., Welte, Tobias, Seeliger, Benjamin, David, Sascha, Schuppan, Detlef, Mentzer, Steven J., Jonigk, Danny D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9535314/
https://www.ncbi.nlm.nih.gov/pubmed/36206625
http://dx.doi.org/10.1016/j.ebiom.2022.104296
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author Ackermann, Maximilian
Kamp, Jan C.
Werlein, Christopher
Walsh, Claire L.
Stark, Helge
Prade, Verena
Surabattula, Rambabu
Wagner, Willi L.
Disney, Catherine
Bodey, Andrew J.
Illig, Thomas
Leeming, Diana J.
Karsdal, Morten A.
Tzankov, Alexandar
Boor, Peter
Kühnel, Mark P.
Länger, Florian P.
Verleden, Stijn E.
Kvasnicka, Hans M.
Kreipe, Hans H.
Haverich, Axel
Black, Stephen M.
Walch, Axel
Tafforeau, Paul
Lee, Peter D.
Hoeper, Marius M.
Welte, Tobias
Seeliger, Benjamin
David, Sascha
Schuppan, Detlef
Mentzer, Steven J.
Jonigk, Danny D.
author_facet Ackermann, Maximilian
Kamp, Jan C.
Werlein, Christopher
Walsh, Claire L.
Stark, Helge
Prade, Verena
Surabattula, Rambabu
Wagner, Willi L.
Disney, Catherine
Bodey, Andrew J.
Illig, Thomas
Leeming, Diana J.
Karsdal, Morten A.
Tzankov, Alexandar
Boor, Peter
Kühnel, Mark P.
Länger, Florian P.
Verleden, Stijn E.
Kvasnicka, Hans M.
Kreipe, Hans H.
Haverich, Axel
Black, Stephen M.
Walch, Axel
Tafforeau, Paul
Lee, Peter D.
Hoeper, Marius M.
Welte, Tobias
Seeliger, Benjamin
David, Sascha
Schuppan, Detlef
Mentzer, Steven J.
Jonigk, Danny D.
author_sort Ackermann, Maximilian
collection PubMed
description BACKGROUND: COVID-19 is characterized by a heterogeneous clinical presentation, ranging from mild symptoms to severe courses of disease. 9–20% of hospitalized patients with severe lung disease die from COVID-19 and a substantial number of survivors develop long-COVID. Our objective was to provide comprehensive insights into the pathophysiology of severe COVID-19 and to identify liquid biomarkers for disease severity and therapy response. METHODS: We studied a total of 85 lungs (n = 31 COVID autopsy samples; n = 7 influenza A autopsy samples; n = 18 interstitial lung disease explants; n = 24 healthy controls) using the highest resolution Synchrotron radiation-based hierarchical phase-contrast tomography, scanning electron microscopy of microvascular corrosion casts, immunohistochemistry, matrix-assisted laser desorption ionization mass spectrometry imaging, and analysis of mRNA expression and biological pathways. Plasma samples from all disease groups were used for liquid biomarker determination using ELISA. The anatomic/molecular data were analyzed as a function of patients’ hospitalization time. FINDINGS: The observed patchy/mosaic appearance of COVID-19 in conventional lung imaging resulted from microvascular occlusion and secondary lobular ischemia. The length of hospitalization was associated with increased intussusceptive angiogenesis. This was associated with enhanced angiogenic, and fibrotic gene expression demonstrated by molecular profiling and metabolomic analysis. Increased plasma fibrosis markers correlated with their pulmonary tissue transcript levels and predicted disease severity. Plasma analysis confirmed distinct fibrosis biomarkers (TSP2, GDF15, IGFBP7, Pro-C3) that predicted the fatal trajectory in COVID-19. INTERPRETATION: Pulmonary severe COVID-19 is a consequence of secondary lobular microischemia and fibrotic remodelling, resulting in a distinctive form of fibrotic interstitial lung disease that contributes to long-COVID. FUNDING: This project was made possible by a number of funders. The full list can be found within the Declaration of interests / Acknowledgements section at the end of the manuscript.
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spelling pubmed-95353142022-10-07 The fatal trajectory of pulmonary COVID-19 is driven by lobular ischemia and fibrotic remodelling Ackermann, Maximilian Kamp, Jan C. Werlein, Christopher Walsh, Claire L. Stark, Helge Prade, Verena Surabattula, Rambabu Wagner, Willi L. Disney, Catherine Bodey, Andrew J. Illig, Thomas Leeming, Diana J. Karsdal, Morten A. Tzankov, Alexandar Boor, Peter Kühnel, Mark P. Länger, Florian P. Verleden, Stijn E. Kvasnicka, Hans M. Kreipe, Hans H. Haverich, Axel Black, Stephen M. Walch, Axel Tafforeau, Paul Lee, Peter D. Hoeper, Marius M. Welte, Tobias Seeliger, Benjamin David, Sascha Schuppan, Detlef Mentzer, Steven J. Jonigk, Danny D. eBioMedicine Articles BACKGROUND: COVID-19 is characterized by a heterogeneous clinical presentation, ranging from mild symptoms to severe courses of disease. 9–20% of hospitalized patients with severe lung disease die from COVID-19 and a substantial number of survivors develop long-COVID. Our objective was to provide comprehensive insights into the pathophysiology of severe COVID-19 and to identify liquid biomarkers for disease severity and therapy response. METHODS: We studied a total of 85 lungs (n = 31 COVID autopsy samples; n = 7 influenza A autopsy samples; n = 18 interstitial lung disease explants; n = 24 healthy controls) using the highest resolution Synchrotron radiation-based hierarchical phase-contrast tomography, scanning electron microscopy of microvascular corrosion casts, immunohistochemistry, matrix-assisted laser desorption ionization mass spectrometry imaging, and analysis of mRNA expression and biological pathways. Plasma samples from all disease groups were used for liquid biomarker determination using ELISA. The anatomic/molecular data were analyzed as a function of patients’ hospitalization time. FINDINGS: The observed patchy/mosaic appearance of COVID-19 in conventional lung imaging resulted from microvascular occlusion and secondary lobular ischemia. The length of hospitalization was associated with increased intussusceptive angiogenesis. This was associated with enhanced angiogenic, and fibrotic gene expression demonstrated by molecular profiling and metabolomic analysis. Increased plasma fibrosis markers correlated with their pulmonary tissue transcript levels and predicted disease severity. Plasma analysis confirmed distinct fibrosis biomarkers (TSP2, GDF15, IGFBP7, Pro-C3) that predicted the fatal trajectory in COVID-19. INTERPRETATION: Pulmonary severe COVID-19 is a consequence of secondary lobular microischemia and fibrotic remodelling, resulting in a distinctive form of fibrotic interstitial lung disease that contributes to long-COVID. FUNDING: This project was made possible by a number of funders. The full list can be found within the Declaration of interests / Acknowledgements section at the end of the manuscript. Elsevier 2022-10-04 /pmc/articles/PMC9535314/ /pubmed/36206625 http://dx.doi.org/10.1016/j.ebiom.2022.104296 Text en © 2022 The Author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Articles
Ackermann, Maximilian
Kamp, Jan C.
Werlein, Christopher
Walsh, Claire L.
Stark, Helge
Prade, Verena
Surabattula, Rambabu
Wagner, Willi L.
Disney, Catherine
Bodey, Andrew J.
Illig, Thomas
Leeming, Diana J.
Karsdal, Morten A.
Tzankov, Alexandar
Boor, Peter
Kühnel, Mark P.
Länger, Florian P.
Verleden, Stijn E.
Kvasnicka, Hans M.
Kreipe, Hans H.
Haverich, Axel
Black, Stephen M.
Walch, Axel
Tafforeau, Paul
Lee, Peter D.
Hoeper, Marius M.
Welte, Tobias
Seeliger, Benjamin
David, Sascha
Schuppan, Detlef
Mentzer, Steven J.
Jonigk, Danny D.
The fatal trajectory of pulmonary COVID-19 is driven by lobular ischemia and fibrotic remodelling
title The fatal trajectory of pulmonary COVID-19 is driven by lobular ischemia and fibrotic remodelling
title_full The fatal trajectory of pulmonary COVID-19 is driven by lobular ischemia and fibrotic remodelling
title_fullStr The fatal trajectory of pulmonary COVID-19 is driven by lobular ischemia and fibrotic remodelling
title_full_unstemmed The fatal trajectory of pulmonary COVID-19 is driven by lobular ischemia and fibrotic remodelling
title_short The fatal trajectory of pulmonary COVID-19 is driven by lobular ischemia and fibrotic remodelling
title_sort fatal trajectory of pulmonary covid-19 is driven by lobular ischemia and fibrotic remodelling
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9535314/
https://www.ncbi.nlm.nih.gov/pubmed/36206625
http://dx.doi.org/10.1016/j.ebiom.2022.104296
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