Identifying SARS-CoV-2 entry inhibitors through drug repurposing screens of SARS-S and MERS-S pseudotyped particles

  1. Catherine Z. Chen
  2. Miao Xu
  3. Manisha Pradhan
  4. Kirill Gorshkov
  5. Jennifer Petersen
  6. Marco R. Straus
  7. Wei Zhu
  8. Paul Shinn
  9. Hui Guo
  10. Min Shen
  11. Carleen Klumpp-Thomas
  12. Samuel G. Michael
  13. Joshua Zimmerberg
  14. Wei Zheng
  15. Gary R. Whittaker
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Abstract

While vaccine development will hopefully quell the global pandemic of COVID-19 caused by SARS-CoV-2, small molecule drugs that can effectively control SARS-CoV-2 infection are urgently needed. Here, inhibitors of spike (S) mediated cell entry were identified in a high throughput screen of an approved drugs library with SARS-S and MERS-S pseudotyped particle entry assays. We discovered six compounds (cepharanthine, abemaciclib, osimertinib, trimipramine, colforsin, and ingenol) to be broad spectrum inhibitors for spike-mediated entry. This work should contribute to the development of effective treatments against the initial stage of viral infection, thus reducing viral burden in COVID-19 patients.

Abstract Figure

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