Volume 15, Issue 1 pp. 52-62

Stem cell-mediated natural tissue engineering

H. Möllmann

Corresponding Author

H. Möllmann

Kerckhoff Heart Center, Dept. of Cardiology, Bad Nauheim, Germany

Franz Groedel Institute of the Kerckhoff Heart Center, Experimental Cardiology, Bad Nauheim, Germany

These authors contributed equally.

Correspondence to: Dr. Helge MÖLLMANN,
Kerckhoff Heart Center, Benekestrasse 2–8, 61231 Bad Nauheim, Germany.
Tel.: +149 6032 996 0
Fax: +149 6032 996 2827
E-mail: [email protected]Search for more papers by this author
H.M. Nef

H.M. Nef

Kerckhoff Heart Center, Dept. of Cardiology, Bad Nauheim, Germany

Franz Groedel Institute of the Kerckhoff Heart Center, Experimental Cardiology, Bad Nauheim, Germany

These authors contributed equally.

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S. Voss

S. Voss

Franz Groedel Institute of the Kerckhoff Heart Center, Experimental Cardiology, Bad Nauheim, Germany

These authors contributed equally.

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C. Troidl

C. Troidl

Franz Groedel Institute of the Kerckhoff Heart Center, Experimental Cardiology, Bad Nauheim, Germany

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M. Willmer

M. Willmer

Franz Groedel Institute of the Kerckhoff Heart Center, Experimental Cardiology, Bad Nauheim, Germany

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S. Szardien

S. Szardien

Kerckhoff Heart Center, Dept. of Cardiology, Bad Nauheim, Germany

Franz Groedel Institute of the Kerckhoff Heart Center, Experimental Cardiology, Bad Nauheim, Germany

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A. Rolf

A. Rolf

Kerckhoff Heart Center, Dept. of Cardiology, Bad Nauheim, Germany

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M. Klement

M. Klement

Franz Groedel Institute of the Kerckhoff Heart Center, Experimental Cardiology, Bad Nauheim, Germany

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R. Voswinckel

R. Voswinckel

Kerckhoff Heart Center, Dept. of Pulmology, Bad Nauheim, Germany

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S. Kostin

S. Kostin

Max-Planck-Institute for Heart and Lung Research, Bad Nauheim, Germany

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H.A. Ghofrani

H.A. Ghofrani

Kerckhoff Heart Center, Dept. of Pulmology, Bad Nauheim, Germany

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C.W. Hamm

C.W. Hamm

Kerckhoff Heart Center, Dept. of Cardiology, Bad Nauheim, Germany

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A. Elsässer

A. Elsässer

Franz Groedel Institute of the Kerckhoff Heart Center, Experimental Cardiology, Bad Nauheim, Germany

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First published: 24 January 2011
Citations: 7

Abstract

Recently, we demonstrated that a fully differentiated tissue developed on a ventricular septal occluder that had been implanted due to infarct-related septum rupture. We suggested that this tissue originated from circulating stem cells. The aim of the present study was to evaluate this hypothesis and to investigate the physiological differentiation and transdifferentiation potential of circulating stem cells. We developed an animal model in which a freely floating membrane was inserted into each the left ventricle and the descending aorta. Membranes were removed after pre-specified intervals of 3 days, and 2, 6 and 12 weeks; the newly developed tissue was evaluated using quantitative RT-PCR, immunohistochemistry and in situ hybridization. The contribution of stem cells was directly evaluated in another group of animals that were by treated with granulocyte macrophage colony-stimulating factor (GM-CSF) early after implantation. We demonstrated the time-dependent generation of a fully differentiated tissue composed of fibroblasts, myofibroblasts, smooth muscle cells, endothelial cells and new blood vessels. Cells differentiated into early cardiomyocytes on membranes implanted in the left ventricles but not on those implanted in the aortas. Stem cell mobilization with GM-CSF led to more rapid tissue growth and differentiation. The GM-CSF effect on cell proliferation outlasted the treat ment period by several weeks. Circulating stem cells contributed to the development of a fully differentiated tissue on membranes placed within the left ventricle or descending aorta under physiological conditions. Early cardiomyocyte generation was identified only on membranes positioned within the left ventricle.

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