Differential Healing Activities of CD34+ and CD14+ Endothelial Cell Progenitors

doi:10.1161/01.ATV.0000203513.29227.6f

Published Online
on January 12, 2006

Arteriosclerosis, Thrombosis, and Vascular Biology. 2006
Published online before print January 12, 2006, doi: 10.1161/01.ATV.0000203513.29227.6f

A more recent version of this article appeared on April 1, 2006

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Submitted on June 21, 2005
Accepted on January 4, 2006

Differential Healing Activities of CD34⁺ and CD14⁺ Endothelial Cell Progenitors

Ola Awad ; Eduard Dedkov ; Chunhua Jiao ; Steven Bloomer ; Robert J. Tomanek ; and Gina C. Schatteman ^*

From the Departments of Anatomy and Cell Biology (O.A., E.D., R.J.T.) and Exercise Science (C.J., S.B., G.C.S.), University of Iowa, Iowa City, Iowa.

^* To whom correspondence should be addressed. E-mail: gina-schatteman{at}uiowa.edu.

Objective--Peripheral blood contains primitive (stem cell-like)and monocytic-like endothelial cell progenitors. Diabetes apparentlyconverts these primitive progenitors, from a pro-angiogenicto anti-angiogenic phenotype. Monocytic progenitors seem tobe less affected by diabetes, but potential pro-angiogenic activitiesof freshly isolated monocytic progenitors remain unexplored.We compared the ability of primitive and monocytic endothelialcell progenitors to stimulate vascular growth and healing indiabetes and investigated potential molecular mechanisms throughwhich the cells mediate their in vivo effects.

Methods and Results--HumanCD34⁺ primitive progenitors and CD14⁺ monocytic progenitorswere injected locally into the ischemic limbs of diabetic mice.CD14⁺ cell therapy improved healing and vessel growth, althoughnot as rapidly or effectively as CD34⁺ cell treatment. Westernblot analysis revealed that cell therapy modulated expressionof molecules in the VEGF, MCP-1, and angiopoietin pathways.

Conclusions--Injectionof freshly isolated circulating CD14⁺ cells improves healingand vascular growth indicating their potential for use in acuteclinical settings. Importantly, CD14⁺ cells could provide atherapeutic option for people with diabetes, the function ofwhose CD34⁺ cells may be compromised. At least some progenitor-inducedhealing probably is mediated through increased sensitivity toVEGF and increases in MCP-1, and possibly modulation of angiopoietins.

Key words: angiogenesis • CD34 • diabetes • endothelial progenitor cells • monocytes

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