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American Heart Association

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Final ID: Th0038

Endothelial CD40 Drives EndMT-Induced Inflammation In Atherosclerosis

Abstract Body: Introduction: Atherosclerosis, the underlying cause of cardiovascular disease (CVD), is a lipid-driven chronic inflammatory disease. We have identified the co-stimulatory CD40-CD40L immune checkpoint dyad as a key driver of inflammation during atherosclerosis. CD40 and CD40L exert cell-type divergent functions via different signaling pathways.

Hypothesis: We hypothesize that CD40 on endothelial cell (ECs) induces endothelial-to-mesenchymal transition (EndMT)-mediated vascular inflammation in atherosclerosis.

Methods & Results: Using single cell RNAseq, we found that CD40 (TNFRSF5) is expressed on PDE3A+GJA5+ and KDR+COL15A1+ ECs of advanced human carotid atherosclerotic plaques. CD40 is highly expressed in the endothelial lining of human and mouse atherosclerotic plaques, and colocalizes with the EndMT markers fibronectin and collagen and adhesion molecule ICAM-1. CD40L activation of human aortic endothelial cells (HAECs) results in expression of the EndMT markers fibronectin, vimentin, sm22α, FSP1 and snail. Activation of CD40 in EC induces filamin A dependent translocation of CD40 into lipid rafts, increases TNF-receptor associated factor (TRAFs) -2, -3 and 6 levels, induces Akt signaling and increases expression of VCAM1 and CCL2.

Conclusions: The endothelial cell has been more and more regarded as a cell type that plays a major role in driving inflammation. Our data suggest that the CD40-CD40L axis plays a significant role in EC-mediated inflammation in atherosclerosis by driving EndMT.
  • Dzobo, Kim  ( Mayo Clinic , Rochester , Minnesota , United States )
  • Lerman, Amir  ( MAYO CLINIC , Rochester , Minnesota , United States )
  • Wang, Ying  ( MAYO CLINIC , Rochester , Minnesota , United States )
  • Goncalves, Isabel  ( Lund University , Malmo , Sweden )
  • Simons, Michael  ( YALE UNIV SCHOOL OF MEDICINE , New Haven , Connecticut , United States )
  • Lutgens, Esther  ( MAYO CLINIC , Rochester , Minnesota , United States )
  • Nitz, Katrin  ( Mayo Clinic , Rochester , Minnesota , United States )
  • Sun, Jiangming  ( Lund University , Malmo , Sweden )
  • Shami, Annelie  ( Lund University , Malmo , Sweden )
  • Gialeli, Chrysostomi  ( Lund University , Malmo , Sweden )
  • Barghouth, Mohammad  ( Lund University , Malmo , Sweden )
  • Nardi, Valentina  ( Mayo Clinic , Rochester , Minnesota , United States )
  • Xiong, Yuning  ( MAYO CLINIC , Rochester , Minnesota , United States )
  • Edsfeldt, Andreas  ( Dept of Clin. sciences, Lund Univ , Malmö , Sweden )
  • Author Disclosures:
    Kim Dzobo: DO NOT have relevant financial relationships | Amir Lerman: No Answer | Ying Wang: No Answer | Isabel Goncalves: No Answer | Michael Simons: No Answer | Esther Lutgens: DO NOT have relevant financial relationships | Katrin Nitz: No Answer | Jiangming Sun: No Answer | Annelie Shami: No Answer | Chrysostomi Gialeli: No Answer | Mohammad Barghouth: No Answer | Valentina Nardi: DO NOT have relevant financial relationships | Yuning Xiong: No Answer | Andreas Edsfeldt: No Answer
Meeting Info:
Session Info:

15. Poster Session 3 & Reception

Thursday, 04/24/2025 , 05:00PM - 07:00PM

Poster

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