Gut microbiota: a new factor modulating the immunizing potential of viral and cancer vaccines

  1. Laurence Zitvogel
  2. Agathe Carrier
  3. Paolo Manghi
  4. Carolina Alves Costa Silva
  5. Imran Lahmar
  6. Roxanne Birebent
  7. Deborah Suissa
  8. Caroline Laheurte
  9. Gerty Schreibelt
  10. Louis Lemant
  11. Jean-Eudes FAHRNER
  12. Eric de Sousa
  13. Franck Berthier
  14. Juliette Villemonteix
  15. Mathieu Chevalier
  16. Gianmarco Piccinno
  17. Didier Hocquet
  18. Isabelle Lebhar
  19. Markus Maeurer
  20. Sophie Caillat-Zucman
  21. Guido Kroemer
  22. Lisa Derosa
  23. Odile Launay
  24. Encouse Golden
  25. Kalijn Bol
  26. I. Jolanda M. De Vries
  27. Olivier Adotévi
  28. Nicola Segata
  29. Silvia Formenti
  30. Sebastian Kobold
  31. Dietmar Pieper
  32. Marius Vital
  33. Antonio Santos-Peral
  34. Magdalena Zaucha
  35. María García-Bengoa
  36. Julia Thorn-Seshold
  37. Helen Stirling
  38. Simon Rothenfusser
  39. Valerio Iebba
  40. Andrew Almonte
  41. Nadim Ajami
  42. Michael White
  43. Pranoti Sahasrabhojane
  44. Yasmine Hoballah
  45. Jillian Losh
  46. Carolyn DePinho
  47. Eleonora Dondossola
  48. Jennifer Wargo
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Abstract

Vaccines represent a major public health intervention against infectious diseases and potentially cancer. Surrogate markers of vaccine efficacy usually rely on neutralizing antibody titers afflicted by high interindividual variabilities. Automated multiplexed T cell assays currently allow to test the clinical relevance of T lymphocyte responses during vaccine rollout. We examined cellular and/or humoral immune responses in five independent cohorts of health care workers, young healthy individuals and patients with cancer (melanoma or lung cancer) receiving various immunizing formulations (non-replicating, viral/tumoral, mRNA/peptides/cellular/viral particles). Here we show that about 20% of vaccinees to non-replicating formulations fail to mount protective antibody and Th1/Tc1 responses while 9% receiving a live vaccine were hyperresponders. Vaccine outliers could at least in part be attributed to gut dysbiosis at baseline, evaluated by shotgun metagenomics-based machine learning or the TOPOSCORE. These findings highlight the requirement of diagnostic tools to identify intestinal dysbiosis, as well as microbiota-centered interventions to optimize the efficiency of mass vaccinations.

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