TY - JOUR
T1 - Sox2 Transduction enhances cardiovascular repair capacity of blood-derived mesoangioblasts
AU - Koyanagi, Masamichi
AU - Iwasaki, Masayoshi
AU - Rupp, Stefan
AU - Tedesco, Francesco Saverio
AU - Yoon, Chang Hwan
AU - Boeckel, Jes Niels
AU - Trauth, Janina
AU - Schütz, Corina
AU - Ohtani, Kisho
AU - Goetz, Rebekka
AU - Iekushi, Kazuma
AU - Bushoven, Philipp
AU - Momma, Stefan
AU - Mummery, Christine
AU - Passier, Robert
AU - Henschler, Reinhard
AU - Akintuerk, Hakan
AU - Schranz, Dietmar
AU - Urbich, Carmen
AU - Galvez, Beatriz G.
AU - Cossu, Giulio
AU - Zeiher, Andreas M.
AU - Dimmeler, Stefanie
PY - 2010/4
Y1 - 2010/4
N2 - RATIONALE: Complementation of pluripotency genes may improve adult stem cell functions. OBJECTIVES: Here we show that clonally expandable, telomerase expressing progenitor cells can be isolated from peripheral blood of children. The surface marker profile of the clonally expanded cells is distinct from hematopoietic or mesenchymal stromal cells, and resembles that of embryonic multipotent mesoangioblasts. Cell numbers and proliferative capacity correlated with donor age. Isolated circulating mesoangioblasts (cMABs) express the pluripotency markers Klf4, c-Myc, as well as low levels of Oct3/4, but lack Sox2. Therefore, we tested whether overexpression of Sox2 enhances pluripotency and facilitates differentiation of cMABs in cardiovascular lineages. METHODS AND RESULTS: Lentiviral transduction of Sox2 (Sox-MABs) enhanced the capacity of cMABs to differentiate into endothelial cells and cardiomyocytes in vitro. Furthermore, the number of smooth muscle actin positive cells was higher in Sox-MABs. In addition, pluripotency of Sox-MABs was shown by demonstrating the generation of endodermal and ectodermal progenies. To test whether Sox-MABs may exhibit improved therapeutic potential, we injected Sox-MABs into nude mice after acute myocardial infarction. Four weeks after cell therapy with Sox-MABs, cardiac function was significantly improved compared to mice treated with control cMABs. Furthermore, cell therapy with Sox-MABs resulted in increased number of differentiated cardiomyocytes, endothelial cells, and smooth muscle cells in vivo. CONCLUSIONS: The complementation of Sox2 in Oct3/4-, Klf4-, and c-Myc-expressing cMABs enhanced the differentiation into all 3 cardiovascular lineages and improved the functional recovery after acute myocardial infarction. © 2010 American Heart Association. All rights reserved.
AB - RATIONALE: Complementation of pluripotency genes may improve adult stem cell functions. OBJECTIVES: Here we show that clonally expandable, telomerase expressing progenitor cells can be isolated from peripheral blood of children. The surface marker profile of the clonally expanded cells is distinct from hematopoietic or mesenchymal stromal cells, and resembles that of embryonic multipotent mesoangioblasts. Cell numbers and proliferative capacity correlated with donor age. Isolated circulating mesoangioblasts (cMABs) express the pluripotency markers Klf4, c-Myc, as well as low levels of Oct3/4, but lack Sox2. Therefore, we tested whether overexpression of Sox2 enhances pluripotency and facilitates differentiation of cMABs in cardiovascular lineages. METHODS AND RESULTS: Lentiviral transduction of Sox2 (Sox-MABs) enhanced the capacity of cMABs to differentiate into endothelial cells and cardiomyocytes in vitro. Furthermore, the number of smooth muscle actin positive cells was higher in Sox-MABs. In addition, pluripotency of Sox-MABs was shown by demonstrating the generation of endodermal and ectodermal progenies. To test whether Sox-MABs may exhibit improved therapeutic potential, we injected Sox-MABs into nude mice after acute myocardial infarction. Four weeks after cell therapy with Sox-MABs, cardiac function was significantly improved compared to mice treated with control cMABs. Furthermore, cell therapy with Sox-MABs resulted in increased number of differentiated cardiomyocytes, endothelial cells, and smooth muscle cells in vivo. CONCLUSIONS: The complementation of Sox2 in Oct3/4-, Klf4-, and c-Myc-expressing cMABs enhanced the differentiation into all 3 cardiovascular lineages and improved the functional recovery after acute myocardial infarction. © 2010 American Heart Association. All rights reserved.
KW - Circulating progenitors
KW - Differentiation
KW - Reprogramming
KW - Sox2
U2 - 10.1161/CIRCRESAHA.109.206045
DO - 10.1161/CIRCRESAHA.109.206045
M3 - Article
C2 - 20185800
SN - 1524-4571
VL - 106
SP - 1290
EP - 1302
JO - Circulation research
JF - Circulation research
IS - 7
ER -