Identification of inhibitors of SARS-CoV-2 in-vitro cellular toxicity in human (Caco-2) cells using a large scale drug repurposing collection

Author:

Ellinger Bernhard1,Bojkova Denisa2,Zaliani Andrea1,Cinatl Jindrich2,Claussen Carsten1,Westhaus Sandra2,Reinshagen Jeanette1,Kuzikov Maria1,Wolf Markus1,Geisslinger Gerd3,Gribbon Philip1,Ciesek Sandra2

Affiliation:

1. Fraunhofer Institute for Molecular Biology and Applied Ecology IME, Branch for Translational Medicine & Pharmacology, ScreeningPort, Hamburg, Germany

2. University Hospital Frankfurt, Frankfurt am Main, Germany

3. Pharmazentrum Frankfurt/ZAFES, Institut für Klinische Pharmakologie, Klinikum der Goethe- Universität Frankfurt, Frankfurt am Main, Germany

Abstract

Abstract To identify possible candidates for progression towards clinical studies against SARS-CoV-2, we screened a well-defined collection of 5632 compounds including 3488 compounds which have undergone clinical investigations (marketed drugs, phases 1 -3, and withdrawn) across 600 indications. Compounds were screened for their inhibition of viral induced cytotoxicity using the human epithelial colorectal adenocarcinoma cell line Caco-2 and a SARS-CoV-2 isolate. The primary screen of 5632 compounds gave 271 hits. A total of 64 compounds with IC50 <20 µM were identified, including 19 compounds with IC50 < 1 µM. Of this confirmed hit population, 90% have not yet been previously reported as active against SARS-CoV-2 in-vitro cell assays. Some 37 of the actives are launched drugs, 19 are in phases 1-3 and 10 pre-clinical. Several inhibitors were associated with modulation of host pathways including kinase signaling P53 activation, ubiquitin pathways and PDE activity modulation, with long chain acyl transferases were effective viral inhibitors.

Publisher

Research Square Platform LLC

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