Actionable druggable genome-wide Mendelian randomization identifies repurposing opportunities for COVID-19

  1. Liam Gaziano
  2. Claudia Giambartolomei
  3. Alexandre C Pereira
  4. Anna Gaulton
  5. Daniel C Posner
  6. Sonja A Swanson
  7. Yuk-Lam Ho
  8. Sudha K Iyengar
  9. Nicole M Kosik
  10. Marijana Vujkovic
  11. David R Gagnon
  12. A PatrĂ­cia Bento
  13. Pedro Beltrao
  14. Inigo Barrio-Hernandez
  15. Lars Rönnblom
  16. Niklas Hagberg
  17. Christian Lundtoft
  18. Claudia Langenberg
  19. Maik Pietzner
  20. Dennis Valentine
  21. Elias Allara
  22. Praveen Surendran
  23. Stephen Burgess
  24. Jing Hua Zhao
  25. James E Peters
  26. Bram P Prins
  27. John Danesh
  28. Poornima Devineni
  29. Yunling Shi
  30. Kristine E Lynch
  31. Scott L DuVall
  32. Helene Garcon
  33. Lauren O Thomann
  34. Jin J Zhou
  35. Bryan R Gorman
  36. Jennifer E Huffman
  37. Christopher J O’Donnell
  38. Philip S Tsao
  39. Jean C Beckham
  40. Saiju Pyarajan
  41. Sumitra Muralidhar
  42. Grant D Huang
  43. Rachel Ramoni
  44. Adriana M Hung
  45. Kyong-Mi Chang
  46. Yan V Sun
  47. Jacob Joseph
  48. Andrew R Leach
  49. Todd L Edwards
  50. Kelly Cho
  51. J Michael Gaziano
  52. Adam S Butterworth
  53. Juan P Casas
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Abstract

Drug repurposing provides a rapid approach to meet the urgent need for therapeutics to address COVID-19. To identify therapeutic targets relevant to COVID-19, we conducted Mendelian randomization (MR) analyses, deriving genetic instruments based on transcriptomic and proteomic data for 1,263 actionable proteins that are targeted by approved drugs or in clinical phase of drug development. Using summary statistics from the Host Genetics Initiative and the Million Veteran Program, we studied 7,554 patients hospitalized with COVID-19 and >1 million controls. We found significant Mendelian randomization results for three proteins (ACE2: P= 1.6×10 −6 , IFNAR2: P= 9.8×10 −11 , and IL-10RB: P= 1.9×10 −14 ) using cis -eQTL genetic instruments that also had strong evidence for colocalization with COVID-19 hospitalization. To disentangle the shared eQTL signal for IL10RB and IFNAR2 , we conducted phenome-wide association scans and pathway enrichment analysis, which suggested that IFNAR2 is more likely to play a role in COVID-19 hospitalization. Our findings prioritize trials of drugs targeting IFNAR2 and ACE2 for early management of COVID-19.

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