TREM2 macrophages are associated with enhanced response to PD-1 blockade in human hepatocellular carcinoma

  1. Pauline Hamon
  2. Matthew D. Park
  3. Jessica Le Berichel
  4. Merav Cohen
  5. Brian Y. Soong
  6. Mark Buckup
  7. Clotilde Hennequin
  8. Katherine E. Lindblad
  9. Raphaël Mattiuz
  10. Igor Figueiredo
  11. Alexandra Tabachnikova
  12. Travis Dawson
  13. Darwin D’souza
  14. Leanna Troncoso
  15. Giorgio Ioannou
  16. Colles Price
  17. Nicolas Fernandez
  18. Amir Giladi
  19. Oren Barboy
  20. Zhen Zhao
  21. Sinem Ozbey
  22. Sarah Cappuyns
  23. Amanda Reid
  24. Steven Hamel
  25. Joel Kim
  26. Romain Donne
  27. Christie Chang
  28. Robert Marvin
  29. Hiyab Stefanos
  30. Grace Chung
  31. Raphaël Merand
  32. Laszlo Halasz
  33. Samarth Hegde
  34. Lou M. Guerin
  35. Min Ni
  36. Yi Wei
  37. Gurinder Atwal
  38. Alona Lansky
  39. Hajra Jamal
  40. Nancy Yi
  41. Theodore Chin
  42. Nicola James
  43. Nausicaa Malissen
  44. Fiona Desland
  45. Yonit Lavin
  46. Stephen C. Ward
  47. Maria Isabel Fiel
  48. Rachel Brody
  49. Jeroen Dekervel
  50. Diether Lambrechts
  51. Ephraim Kenigsberg
  52. Edgar Gonzalez-Kozlova
  53. Vladimir Roudko
  54. Alice O. Kamphorst
  55. Jiang He
  56. Marco Colonna
  57. Seunghee Kim-Schulze
  58. Sacha Gnjatic
  59. John C. Lin
  60. Gavin Thurston
  61. Amaia Lujambio
  62. Myron Schwartz
  63. Ido Amit
  64. Thomas U. Marron
  65. Miriam Merad
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Abstract

Macrophages are known to dampen tumor immunity. However, identifying druggable targets that modulate these cells to improve existing immunotherapies has been limited by a dearth of studies identifying macrophages that associate with pathological response to immune checkpoint blockade. To fulfill this unmet clinical need, we leveraged transcriptional and spatial profiling of specimens collected from a Phase II clinical trial studying neoadjuvant PD-1 blockade in patients with hepatocellular carcinoma (HCC). We determined that the intratumoral abundance of TREM2-expressing macrophages and serological levels of soluble TREM2 are elevated in patients who responded to PD-1 blockade, compared to non-responders. We validated these findings in a second HCC cohort and in the IMbrave150 trial. These highlight the robust potential for TREM2 macrophages to predict therapeutic responses of HCC to immunotherapy. Therefore, our study provides a novel basis for the use of TREM2 macrophages to strategize treatment for patients with HCC to maximize therapeutic benefit.

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