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MEK1/2 inhibition transiently alters the tumor immune microenvironment to enhance immunotherapy efficacy against head and neck cancer.

Manu PrasadJonathan ZoreaSankar JagadeeshanAvital B ShnerbSooraj MathukkadaJebrane BouaoudLucas MichonOfra NovoplanskyMai BadarniLimor CohenKsenia M YegodayevSapir TzadokBarak RotblatLibor BrezinaAndreas MockAndy KarabajakianJérôme FayetteIdan CohenTomer CooksIrit AllonOrr DimitsteinBenzion JoshuaDexin KongElena VoronovMaurizio ScaltritiYaron CarmiCristina Conde-LopezJochen HessIna KurthLuc G T MorrisPierre SaintignyMoshe Elkabets
Published in: Journal for immunotherapy of cancer (2022)
Our findings provide the rationale for testing the trametinib/αPD-1 combination in HNC and highlight the importance of sensitizing tumors to αPD-1 by using MEK1/2 to interfere with the tumor-host interaction. Moreover, we describe the concept that treatment of cancer with a targeted therapy transiently induces an immune-active microenvironment, and supplementation of immunotherapy during this time further activates the antitumor machinery to cause tumor elimination.
Keyphrases
  • stem cells
  • clinical trial
  • pi k akt
  • papillary thyroid
  • squamous cell carcinoma
  • young adults
  • cell proliferation
  • lymph node metastasis