A High-Content Screen for Mucin-1-Reducing Compounds Identifies Fostamatinib as a Candidate for Rapid Repurposing for Acute Lung Injury

Maria Kost‐Alimova; Eriene-Heidi Sidhom; Abhigyan Satyam; Brian T. Chamberlain; Moran Dvela‐Levitt; Michelle Melanson; Seth L. Alper; Jean Santos; Juan Gutierrez; Ayshwarya Subramanian; Patrick J. Byrne; Elizabeth Grinkevich; Estefanía Reyes-Bricio; Choah Kim; Abbe R. Clark; Andrew Watts; Rebecca F. Thompson; Jamie L. Marshall; Juan Lorenzo Pablo; Juliana Coraor; Julie Roignot; Katherine A. Vernon; Keith Keller; Alissa Campbell; Maheswarareddy Emani; Matthew Racette; Silvana Bazúa‐Valenti; Valeria Padovano; Astrid Weins; Stephen P. McAdoo; Frederick W.K. Tam; Luciene Ronco; Florence F. Wagner; George C. Tsokos; Jillian L. Shaw; Anna Greka

doi:10.1016/j.xcrm.2020.100137

A High-Content Screen for Mucin-1-Reducing Compounds Identifies Fostamatinib as a Candidate for Rapid Repurposing for Acute Lung Injury

Maria Kost‐Alimova(Broad Institute), Eriene-Heidi Sidhom(Broad Institute), Abhigyan Satyam(Beth Israel Deaconess Medical Center), Brian T. Chamberlain(Broad Institute), Moran Dvela‐Levitt(Broad Institute), Michelle Melanson(Broad Institute), Seth L. Alper(Broad Institute), Jean Santos(Broad Institute), Juan Gutierrez(Broad Institute), Ayshwarya Subramanian(Broad Institute), Patrick J. Byrne(Broad Institute), Elizabeth Grinkevich(Broad Institute), Estefanía Reyes-Bricio(Broad Institute), Choah Kim(Broad Institute), Abbe R. Clark(Broad Institute), Andrew Watts(Broad Institute), Rebecca F. Thompson(Broad Institute), Jamie L. Marshall(Broad Institute), Juan Lorenzo Pablo(Broad Institute), Juliana Coraor(Broad Institute), Julie Roignot(Broad Institute), Katherine A. Vernon(Broad Institute), Keith Keller(Broad Institute), Alissa Campbell(Broad Institute), Maheswarareddy Emani(Broad Institute), Matthew Racette(Broad Institute), Silvana Bazúa‐Valenti(Broad Institute), Valeria Padovano(Broad Institute), Astrid Weins(Brigham and Women's Hospital), Stephen P. McAdoo(Hammersmith Hospital), Frederick W.K. Tam(Hammersmith Hospital), Luciene Ronco(Broad Institute), Florence F. Wagner(Broad Institute), George C. Tsokos(Beth Israel Deaconess Medical Center), Jillian L. Shaw(Broad Institute), Anna Greka(Broad Institute)

Cell Reports Medicine

October 30, 2020

10.1016/j.xcrm.2020.100137

Cited by 71Open Access

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Abstract

Drug repurposing has the advantage of identifying potential treatments on a shortened timescale. In response to the pandemic spread of SARS-CoV-2, we took advantage of a high-content screen of 3,713 compounds at different stages of clinical development to identify FDA-approved compounds that reduce mucin-1 (MUC1) protein abundance. Elevated MUC1 levels predict the development of acute lung injury (ALI) and acute respiratory distress syndrome (ARDS) and correlate with poor clinical outcomes. Our screen identifies fostamatinib (R788), an inhibitor of spleen tyrosine kinase (SYK) approved for the treatment of chronic immune thrombocytopenia, as a repurposing candidate for the treatment of ALI. In vivo, fostamatinib reduces MUC1 abundance in lung epithelial cells in a mouse model of ALI. In vitro, SYK inhibition by the active metabolite R406 promotes MUC1 removal from the cell surface. Our work suggests fostamatinib as a repurposing drug candidate for ALI.

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