Litcius/Paper detail

Alloreactive memory CD4 T cells promote transplant rejection by engaging DCs to induce innate inflammation and CD8 T cell priming

Irene Saha, Amanpreet Singh Chawla, Ana Paula B N Oliveira, Eileen E. Elfers, Kathrynne A. Warrick, Hannah E. Meibers, Viral G. Jain, Thomas Hagan, Jonathan D. Katz, Chandrashekhar Pasare

2024Proceedings of the National Academy of Sciences13 citationsDOIOpen Access PDF

Abstract

Alloreactive memory T cells have been implicated as central drivers of transplant rejection. Perplexingly, innate cytokines, such as IL-6, IL-1β, and IL-12, are also associated with rejection of organ transplants. However, the pathways of innate immune activation in allogeneic transplantation are unclear. While the role of microbial and cell death products has been previously described, we identified alloreactive memory CD4 T cells as the primary triggers of innate inflammation. Memory CD4 T cells engaged MHC II-mismatched dendritic cells (DCs), leading to the production of innate inflammatory cytokines. This innate inflammation was independent of several pattern recognition receptors and was primarily driven by TNF superfamily ligands expressed by alloreactive memory CD4 T cells. Blocking of CD40L and TNFα resulted in dampened inflammation, and mice genetically deficient in these molecules exhibited prolonged survival of cardiac allografts. Furthermore, myeloid cell and CD8 T cell infiltration into cardiac transplants was compromised in both CD40L- and TNFα-deficient recipients. Strikingly, we found that priming of naive alloreactive CD8 T cells was dependent on licensing of DCs by memory CD4 T cells. This study unravels the key mechanisms by which alloreactive memory CD4 T cells contribute to destructive pathology and transplant rejection.

Topics & Concepts

Priming (agriculture)Cytotoxic T cellInflammationInnate immune systemImmunological memoryImmunologyCD8Cell biologyBiologyImmune systemImmunityBiochemistryIn vitroBotanyGerminationImmune Cell Function and InteractionPhagocytosis and Immune RegulationNeuroinflammation and Neurodegeneration Mechanisms
Alloreactive memory CD4 T cells promote transplant rejection by engaging DCs to induce innate inflammation and CD8 T cell priming | Litcius