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Am J Physiol Regul Integr Comp Physiol 294: R1491-R1497, 2008. First published April 2, 2008; doi:10.1152/ajpregu.00031.2008
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TRANSLATIONAL PHYSIOLOGY

Neonatal stem cells exhibit specific characteristics in function, proliferation, and cellular signaling that distinguish them from their adult counterparts

Troy A. Markel,1 Meijing Wang,1 Paul R. Crisostomo,1 Maiuxi C. Manukyan,1 Jeffrey A. Poynter,1 and Daniel R. Meldrum1,2,3

Departments of 1Surgery, 2Cellular and Integrative Physiology, and the 3Center for Immunobiology, Indiana University School of Medicine, Indianapolis, Indiana

Submitted 16 January 2008 ; accepted in final form 18 March 2008

ABSTRACT

Stem cells may be a novel treatment modality for organ ischemia, possibly through beneficial paracrine mechanisms. Stem cells from older hosts have been shown to exhibit decreased function during stress. We therefore hypothesized that 1) neonatal bone marrow mesenchymal stem cells (nBMSCs) would produce different levels of IL-6, VEGF, and IGF-1 compared with adults (aBMSCs) when stimulated with TNF or LPS; 2) differences in cytokines would be due to distinct cellular characteristics, such as proliferation or pluripotent potential; and 3) differences in cytokines would be associated with differences in p38 MAPK and ERK signaling within nBMSCs. BMSCs were isolated from adult and neonatal mice. Cells were exposed to TNF or LPS with or without p38 or ERK inhibition. Growth factors were measured via ELISA, proliferation via daily cell counts, cell surface markers via flow cytometry, and pluripotent potential via alkaline phosphatase activity. nBMSCs produced lower levels of IL-6 and VEGF, but higher levels of IGF-1 under basal conditions, as well as after stimulation with TNF, but not LPS. Neonatal and adult BMSCs had similar pluripotent potentials and cell surface markers, but nBMSCs proliferated faster. Furthermore, p38 and ERK appeared to play a more substantial role in nBMSC cytokine and growth factor production. Neonatal stem cells may aid in decreasing the local inflammatory response during ischemia, and could possibly be expanded more rapidly than adult cells prior to therapeutic use.

interleukin-6; insulin-like growth factor-1; vascular endothelial growth factor; fetal; ischemia; stem cell therapy


Address for reprint requests and other correspondence: D. R. Meldrum, 635 Barnhill Dr., 2017 Van Nuys Medical Science Bldg., Indianapolis, IN 46202 (e-mail: dmeldrum{at}iupui.edu)






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