Adjunctive ruxolitinib attenuates inflammation and enhances antiparasitic immunity in human volunteers experimentally infected withPlasmodium falciparum

  1. Rebecca Webster
  2. Damian A. Oyong
  3. Azrin N. Abd-Rahman
  4. Adam J. Potter
  5. Reena Mukhiya
  6. Nischal Sahai
  7. Indika Leelasena
  8. Eniko Ujvary
  9. Sue Mathison
  10. Dean W. Andrew
  11. Luzia Bukali
  12. Fabian de Labastida Rivera
  13. Jessica Engel
  14. Megan S.F. Soon
  15. Teija Frame
  16. Julianne Hamelink
  17. Mayimuna Nalubega
  18. Nicholas L. Dooley
  19. Jessica R. Loughland
  20. Tran Nguyen
  21. Yael Rosenberg-Hasson
  22. Sofia Maysel-Auslender
  23. Natalia Sigal
  24. Kira Foygel
  25. Jeremy Gower
  26. Jenny Peters
  27. Ria Woo
  28. Fiona Amante
  29. Timothy N.C. Wells
  30. Stephan Chalon
  31. Joerg J. Moehrle
  32. James S. McCarthy
  33. Geoffrey W. Birrell
  34. Michael D. Edstein
  35. Michael Leipold
  36. Gerlinde Obermoser
  37. Holden Maecker
  38. Christian R. Engwerda
  39. Bridget E Barber
  40. Michelle J. Boyle
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Abstract

Inhibiting the host inflammatory response to malaria represents a potential strategy to improve clinical outcomes and inhibit immunoregulatory pathways that underlie suboptimal development of antiparasitic immunity. Ruxolitinib is a JAK 1/2 inhibitor that reduces inflammatory biomarkers when used in myeloproliferative disorders, and inhibits type-1 interferons and enhances CD4+ T cell immunity when combined with anti-parasitic drugs in animal models. Here we report the results of a double-blind randomised placebo-controlled trial evaluating the ability of ruxolitinib to reduce inflammatory responses and boost anti-parasitic immunity in malaria-naïve volunteers inoculated with blood-stagePlasmodium falciparum. Twenty participants were inoculated, and randomized on day 8 to receive artemether-lumefantrine with either ruxolitinib or placebo. Ninety days later, participants who remained eligible were re-inoculated with a second infection. Ruxolitinib was safe and well-tolerated, and attenuated the host inflammatory response to the initial infection, with reduced post-treatment increases in the inflammatory biomarker CRP, as well as markers of disease severity including angiopoietin-2 and ICAM-1. Further, ruxolitinib enhanced the immune memory response following a second inoculation, with increased plasma levels of HLA-DR and CXCL13, indicating enhanced immune activation and germinal centre responses, respectively. These data support the further evaluation of ruxolitinib as an adjunctive treatment to improve clinical outcomes and boost anti-parasitic immunity in clinical malaria.

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