Cell-to-cell Connection of Endothelial Progenitor Cells With Cardiac Myocytes by Nanotubes: A Novel Mechanism for Cell Fate Changes?

doi:10.1161/01.RES.0000168650.23479.0c

Circulation Research. 2005
Published online before print May 5, 2005, doi: 10.1161/01.RES.0000168650.23479.0c

A more recent version of this article appeared on May 27, 2005

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Submitted on November 16, 2004
Revised on March 24, 2005
Accepted on April 25, 2005

Cell-to-cell Connection of Endothelial Progenitor Cells With Cardiac Myocytes by Nanotubes: A Novel Mechanism for Cell Fate Changes?

Masamichi Koyanagi ; Ralf P. Brandes ; Judith Haendeler ; Andreas M. Zeiher ; and Stefanie Dimmeler ^*

From the Molecular Cardiology (M.K., J.H., A.M.Z, S.D.), Department of Internal Medicine III, University of Frankfurt, Germany; Institute of Cardiovascular Physiology (R.P.B.), University of Frankfurt, Germany

^* To whom correspondence should be addressed. E-mail: Dimmeler{at}em.uni-frankfurt.de.

The regeneration of new myocardium by stem or progenitor cellsis an important therapeutic option. Cellular or nuclear fusionis considered as an alternative to cell reprogramming by transdifferentiation.However, the generation of hybrid cells may also be a consequenceof a transient transmembrane exchange of proteins and organellesbetween cells. Therefore, we investigated the formation of intercellularconnections, which may allow the transport of macromolecularstructures between Dil-ac-LDL labeled adult human endothelialprogenitor cells (EPC) and GFP-expressing neonatal rat cardiomyocytes(CM) in a coculture system. FACS analysis revealed that, 6 daysafter initiation of coculture, 2.1±0.4% of the cells stainedpositive for GFP and Dil-ac-LDL. 6 hours after initiation ofthe coculture, ultrafine intercellular structures between Dil-ac-LDL-labeledEPC and GFP-expressing CM were observed. The number of EPC,which established nanotubular connections with CM increasedfrom 0.5±0.2% after 6 hours to 2.6±0.3% after 24 hoursof coculture. The intercellular connections had a diameter from50 to 800 nm, a length of 5 to 120 µm, and were only transientlyestablished. To determine whether the nanotubular structuresallowed the transport of organelles, we labeled CM with a mitochondriallive tracker (MitoTracker). Using time-lapse video microscopy,we observed the transport of stained complexes between CM andEPC resulting in up-take of MitoTracker-positive structuresin EPC. Thus, the present study shows a novel type of cell-to-cellcommunication between progenitor cells and CM in vitro, whichmay contribute to the acquisition of a cardiomyogenic phenotypeindependent of permanent cellular or nuclear fusion.

Key words: progenitor cells • fusion • cardiac myocytes

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