Increased yield of endothelial cells from peripheral blood for cell therapies and tissue engineering

Peripheral blood-derived endothelial cells (pBD-ECs) are an attractive tool for cell therapies and tissue engineering, but have been limited by their low isolation yield. We increase pBD-EC yield via administration of the chemokine receptor type 4 antagonist AMD3100, as well as via a diluted whole b...

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Veröffentlicht in:Regenerative medicine 2015-05, Vol.10 (4), p.447-460
Hauptverfasser: Jamiolkowski, Ryan M, Kang, Sa Do, Rodriguez, AnnMarie K, Haseltine, Justin M, Galinat, Lauren J, Jantzen, Alexandra E, Carlon, Tim A, Darrabie, Marcus D, Arciniegas, Antonio J, Mantilla, Jose G, Haley, N Rebecca, Noviani, Maria, Allen, Jason D, Stabler, Thomas V, Frederiksen, James W, Alzate, Oscar, Keil, Lukas G, Liu, Siyao, Lin, Fu-Hsiung, Truskey, George A, Achneck, Hardean E
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Sprache:eng
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Zusammenfassung:Peripheral blood-derived endothelial cells (pBD-ECs) are an attractive tool for cell therapies and tissue engineering, but have been limited by their low isolation yield. We increase pBD-EC yield via administration of the chemokine receptor type 4 antagonist AMD3100, as well as via a diluted whole blood incubation (DWBI). Porcine pBD-ECs were isolated using AMD3100 and DWBI and tested for EC markers, acetylated LDL uptake, growth kinetics, metabolic activity, flow-mediated nitric oxide production and seeded onto titanium tubes implanted into vessels of pigs. DWBI increased the yield of porcine pBD-ECs 6.6-fold, and AMD3100 increased the yield 4.5-fold. AMD3100-mobilized ECs were phenotypically indistinguishable from nonmobilized ECs. In porcine implants, the cells expressed endothelial nitric oxide synthase, reduced thrombin-antithrombin complex systemically and prevented thrombosis. Administration of AMD3100 and the DWBI method both increase pBD-EC yield.
ISSN:1746-0751
1746-076X
DOI:10.2217/rme.15.2