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Concomitant or delayed anti-TNF differentially impact on immune-related adverse events and antitumor efficacy after anti-CD40 therapy.

Celia Jacoberger-FoissacStephen J BlakeJing LiuElizabeth McDonaldHannah TriscottKyohei NakamuraMark J SmythMichele W L Teng
Published in: Journal for immunotherapy of cancer (2021)
Our results suggest concomitant rather than delayed anti-TNF is most effective in reducing biochemical and physical irAEs induced by anti-CD40, although it had the potential to negatively impact antitumor efficacy. Furthermore, our findings highlight the utility of our mouse model to assess the severity of irAEs induced by novel immunotherapeutic agents and evaluate whether their toxicity and antitumor efficacy can be uncoupled.
Keyphrases
  • mouse model
  • rheumatoid arthritis
  • mental health
  • oxidative stress
  • nk cells
  • bone marrow
  • mesenchymal stem cells
  • cell therapy
  • climate change