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Distinct molecular and immune hallmarks of inflammatory arthritis induced by immune checkpoint inhibitors for cancer therapy.

Sang T KimYanshuo ChuMercy MisoiMaria E Suarez-AlmazorJean H TayarHuifang LuMaryam BuniJordan KramerEmma RodriguezZulekha HussainSattva S NeelapuJennifer WangAmishi Yogesh ShahNizar M TannirMatthew T CampbellDon L GibbonsCascone TinaCharles LuGeorge R BlumenscheinMehmet AltanBora LimVincente ValeroMonica E LoghinJanet TuShannon Neville WestinAung NaingGuillermo Garcia ManeroNoha Abdel-WahabHussein A TawbiPatrick HwuIsabella C Glitza OlivaMichael A DaviesSapna Pradyuman PatelJun ZouP Andrew FutrealAdi DiabLinghua WangRoza Nurieva
Published in: Nature communications (2022)
Immune checkpoint inhibitors are associated with immune-related adverse events (irAEs), including arthritis (arthritis-irAE). Management of arthritis-irAE is challenging because immunomodulatory therapy for arthritis should not impede antitumor immunity. Understanding of the mechanisms of arthritis-irAE is critical to overcome this challenge, but the pathophysiology remains unknown. Here, we comprehensively analyze peripheral blood and/or synovial fluid samples from 20 patients with arthritis-irAE, and unmask a prominent Th1-CD8 + T cell axis in both blood and inflamed joints. CX3CR1 hi CD8 + T cells in blood and CXCR3 hi CD8 + T cells in synovial fluid, the most clonally expanded T cells, significantly share TCR repertoires. The migration of blood CX3CR1 hi CD8 + T cells into joints is possibly mediated by CXCL9/10/11/16 expressed by myeloid cells. Furthermore, arthritis after combined CTLA-4 and PD-1 inhibitor therapy preferentially has enhanced Th17 and transient Th1/Th17 cell signatures. Our data provide insights into the mechanisms, predictive biomarkers, and therapeutic targets for arthritis-irAE.
Keyphrases
  • rheumatoid arthritis
  • peripheral blood
  • stem cells
  • bone marrow
  • gene expression
  • dendritic cells
  • cell therapy
  • cell proliferation
  • cell death
  • electronic health record
  • mesenchymal stem cells
  • regulatory t cells