Transplantation of<i>ex vivo</i>expanded endothelial progenitor cells for therapeutic neovascularization

Christoph Kalka(Tufts University), Haruchika Masuda(Tufts University), Tomono Takahashi(Tufts University), Wiltrud M. Kalka-Moll(Tufts University), Marcy Silver(Tufts University), Marianne Kearney(Tufts University), Tong Li(Tufts University), Jeffrey M. Isner(Tufts University), Takayuki Asahara(Tufts University)
Proceedings of the National Academy of Sciences
March 21, 2000
Cited by 1,853Open Access
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Abstract

Animal studies and preliminary results in humans suggest that lower extremity and myocardial ischemia can be attenuated by treatment with angiogenic cytokines. The resident population of endothelial cells that is competent to respond to an available level of angiogenic growth factors, however, may potentially limit the extent to which cytokine supplementation enhances tissue neovascularization. Accordingly, we transplanted human endothelial progenitor cells (hEPCs) to athymic nude mice with hindlimb ischemia. Blood flow recovery and capillary density in the ischemic hindlimb were markedly improved, and the rate of limb loss was significantly reduced. Ex vivo expanded hEPCs may thus have utility as a "supply-side" strategy for therapeutic neovascularization.


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