BET inhibition blocks inflammation-induced cardiac dysfunction and SARS-CoV-2 infection

Mills, R.J.; Humphrey, S.J.; Fortuna, P.R.J.; Lor, M.; Foster, S.R.; Quaife-Ryan, G.A.; Johnston, R.L.; Dumenil, T.; Bishop, C.; Rudraraju, R.; Rawle, D.J.; Le, T.; Zhao, W.; Lee, L.; Mackenzie-Kludas, C.; Mehdiabadi, N.R.; Halliday, C.; Gilham, D.; Fu, L.; Nicholls, S.J.; et al.

Please use this identifier to cite or link to this item: https://hdl.handle.net/2440/130538

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Type:	Journal article
Title:	BET inhibition blocks inflammation-induced cardiac dysfunction and SARS-CoV-2 infection
Author:	Mills, R.J. Humphrey, S.J. Fortuna, P.R.J. Lor, M. Foster, S.R. Quaife-Ryan, G.A. Johnston, R.L. Dumenil, T. Bishop, C. Rudraraju, R. Rawle, D.J. Le, T. Zhao, W. Lee, L. Mackenzie-Kludas, C. Mehdiabadi, N.R. Halliday, C. Gilham, D. Fu, L. Nicholls, S.J. et al.
Citation:	Cell, 2021; 184(8):2167-2182.e22
Publisher:	Elsevier BV
Issue Date:	2021
ISSN:	0092-8674 1097-4172
Statement of Responsibility:	Richard J. Mills, Sean J. Humphrey, Patrick R.J. Fortuna, Mary Lor, Simon R. Foster, Gregory A. Quaife-Ryan, Rebecca L. Johnston, Troy Dumenil, Cameron Bishop, Rajeev Rudraraju, Daniel J. Rawle, Thuy Le, Wei Zhao, Leo Lee, Charley Mackenzie-Kludas, Neda R. Mehdiabadi, Christopher Halliday, Dean Gilham, Li Fu, Stephen J. Nicholls, Jan Johansson, Michael Sweeney, Norman C.W. Wong, Ewelina Kulikowski, Kamil A. Sokolowski, Brian W.C. Tse, Lynn Devilee, Holly K. Voges, Liam T. Reynolds, Sophie Krumeich, Ellen Mathieson, Dad Abu-Bonsrah, Kathy Karavendzas, Brendan Griffen, Drew Titmarsh, David A. Elliott, James McMahon, Andreas Suhrbier, Kanta Subbarao, Enzo R. Porrello, Mark J. Smyth, Christian R. Engwerda, Kelli P.A. MacDonald, Tobias Bald, David E. James, and James E. Hudson
Abstract:	Cardiac injury and dysfunction occur in COVID-19 patients and increase the risk of mortality. Causes are ill defined but could be through direct cardiac infection and/or inflammation-induced dysfunction. To identify mechanisms and cardio-protective drugs, we use a state-of-the-art pipeline combining human cardiac organoids with phosphoproteomics and single nuclei RNA sequencing. We identify an inflammatory "cytokine-storm", a cocktail of interferon gamma, interleukin 1β, and poly(I:C), induced diastolic dysfunction. Bromodomain-containing protein 4 is activated along with a viral response that is consistent in both human cardiac organoids (hCOs) and hearts of SARS-CoV-2-infected K18-hACE2 mice. Bromodomain and extraterminal family inhibitors (BETi) recover dysfunction in hCOs and completely prevent cardiac dysfunction and death in a mouse cytokine-storm model. Additionally, BETi decreases transcription of genes in the viral response, decreases ACE2 expression, and reduces SARS-CoV-2 infection of cardiomyocytes. Together, BETi, including the Food and Drug Administration (FDA) breakthrough designated drug, apabetalone, are promising candidates to prevent COVID-19 mediated cardiac damage.
Keywords:	Inflammation; COVID-19; organoids; heart; drug discovery; Bromodomain and extraterminal family inhibitors
Rights:	© 2021 Elsevier Inc.
DOI:	10.1016/j.cell.2021.03.026
Grant ID:	http://purl.org/au-research/grants/nhmrc/1132519 http://purl.org/au-research/grants/nhmrc/1173958 http://purl.org/au-research/grants/nhmrc/1173880
Published version:	http://dx.doi.org/10.1016/j.cell.2021.03.026
Appears in Collections:	Aurora harvest 4 Medicine publications

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