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(Circulation Research. 2001;88:e1.)
© 2001 American Heart Association, Inc.

Letter to the Editor

Contribution of Endothelial Cells of Hematopoietic Origin to Blood Vessel Formation

Eberhard Gunsilius, Hans-Christoph Duba, Andreas L. Petzer, Christian M. Kähler, Günther A. Gastl

University of Innsbruck, Anichstrasse 35, 6020 Innsbruck, Austria

eberhard.gunsilius@uibk.ac.at

	Introduction

 
To the Editor:

Crosby et al¹ noted in their report that the recruitment of bone marrow–derived endothelial progenitor cells to newly forming blood vessels might have been hitherto overlooked. Postulated already a century ago,² there is now ample evidence for a close association between blood progenitor cells and angiogenesis³ and the existence of a hemangioblastic progenitor capable of generating blood cells as well as endothelial cells.^{4 5 6} Also, the integration of bone marrow–derived endothelial cells or their progenitors into sites of neoangiogenesis is well-known.^{7 8 9} Their view that bone marrow–derived endothelial cells do not contribute substantially to the endothelium of blood vessels in stable adult tissue is equivocal. Endothelial cells are among those exhibiting the lowest replication level in the body with only 0.01% cells engaged in cell division at any time.¹⁰ Nevertheless, vascular endothelial cells that are lost from the vessel intima through necrosis or apoptosis must be replaced (maintenance angiogenesis). We are not aware of data showing that maintenance angiogenesis occurs through proliferation of adjacent endothelial cells. Thus, most likely, bone marrow–derived endothelial cells contribute to this maintenance angiogenesis.¹¹

Vascular endothelial growth factor (VEGF) can mobilize endothelial cells or their progenitors from the bone marrow,⁹ and the delivery of VEGF to subjects may be deleterious.^{12 13} Hypoxia can also launch mobilization of endothelial precursor cells from the bone marrow, as hematopoietic cytokines (granulocyte/macrophage colony-stimulating factor) can do.¹⁴ Malignant tumor growth results in hypoxia within the neoplastic tissue, potentially mobilizing bone marrow–derived endothelial cells as well in a paracrine fashion, thus contributing . . . [Full Text of this Article]