Extracellular nucleotides play an important role in thrombosis and inflammation, triggering a range of effects such as platelet activation and recruitment, endothelial cell activation, and vasoconstriction. CD39, the major vascular nucleoside triphosphate diphosphohydrolase (NTPDase), converts ATP and ADP to AMP, which is further degraded to the antithrombotic and anti-inflammatory mediator adenosine. Deletion of CD39 renders mice exquisitely sensitive to vascular injury, and CD39-null cardiac xenografts show reduced survival. Conversely, upregulation of CD39 by somatic gene transfer or administration of soluble NTPDases has major benefits in models of transplantation and inflammation. In this study we examined the consequences of transgenic expression of human CD39 (hCD39) in mice. Importantly, these mice displayed no overt spontaneous bleeding tendency under normal circumstances. The hCD39 transgenic mice did, however, exhibit impaired platelet aggregation, prolonged bleeding times, and resistance to systemic thromboembolism. Donor hearts transgenic for hCD39 were substantially protected from thrombosis and survived longer in a mouse cardiac transplant model of vascular rejection. These thromboregulatory manifestations in hCD39 transgenic mice suggest important therapeutic potential in clinical vascular disease and in the control of serious thrombotic events that compromise the survival of porcine xenografts in primates.
Karen M. Dwyer, Simon C. Robson, Harshal H. Nandurkar, Duncan J. Campbell, Hilton Gock, Lisa J. Murray-Segal, Nella Fisicaro, Tharun B. Mysore, Elzbieta Kaczmarek, Peter J. Cowan, Anthony J.F. d’Apice
Title and authors | Publication | Year |
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Impaired natriuretic response to high-NaCl diet plus aldosterone infusion in mice overexpressing human CD39, an ectonucleotidase (NTPDase1)
Y Zhang, SC Robson, KL Morris, KM Heiney, KM Dwyer, BK Kishore, CM Ecelbarger |
American journal of physiology. Renal physiology | 2015 |
Bortezomib, C1-Inhibitor and Plasma Exchange Do Not Prolong the Survival of Multi-Transgenic GalT-KO Pig Kidney Xenografts in Baboons: Multi-Transgenic GalT-KO Kidney Xenograft
SL Bas-Bernardet, X Tillou, J Branchereau, N Dilek, N Poirier, M Châtelais, B Charreau, D Minault, J Hervouet, K Renaudin, C Crossan, L Scobie, Y Takeuchi, M Diswall, ME Breimer, N Klar, MR Daha, P Simioni, SC Robson, MB Nottle, EJ Salvaris, PJ Cowan, AJ d'Apice, DH Sachs, K Yamada, I Lagutina, R Duchi, A Perota, G Lazzari, C Galli, E Cozzi, JP Soulillou, B Vanhove, G Blancho |
American Journal of Transplantation | 2015 |
In vitro Study of a Novel Stent Coating Using Modified CD39 Messenger RNA to Potentially Reduce Stent Angioplasty-Associated Complications
MK Abraham, A Nolte, R Reus, A Behring, D Zengerle, M Avci-Adali, JD Hohmann, K Peter, C Schlensak, HP Wendel, S Krajewski, I Ahrens |
PloS one | 2015 |
Use of genetically-engineered pig donors in islet transplantation
R Bottino |
World Journal of Transplantation | 2015 |
Simultaneous Overexpression of Functional Human HO-1, E5NT and ENTPD1 Protects Murine Fibroblasts against TNF-α-Induced Injury In Vitro
A Cinti, MD Giorgi, E Chisci, C Arena, G Galimberti, L Farina, C Bugarin, I Rivolta, G Gaipa, RT Smolenski, MG Cerrito, M Lavitrano, R Giovannoni, AT Slominski |
PloS one | 2015 |