Perlecan Maintains microvessel integrity in vivo and modulates their formation in vitro

6533b85dfe1ef96bd12bda18

RESEARCH PRODUCT

Perlecan Maintains microvessel integrity in vivo and modulates their formation in vitro

Erika Gustafsson Maylin Almonte-becerril Wilhelm Bloch Mercedes Costell

subject

Integrins Anatomy and Physiology Glycobiology lcsh:Medicine Cardiovascular urologic and male genital diseases Cardiovascular System Biochemistry Biotecnologia Basement Membrane Mice Pregnancy Molecular Cell Biology Morphogenesis Histochemistry lcsh:Science Skin Mice Knockout Peripheral Vascular Diseases Extracellular Matrix Proteins Neovascularization Pathologic Teratoma Proteïnes de membrana Brain Cell Differentiation Extracellular Matrix Connective Tissue Cytochemistry Medicine Female Fibroblast Growth Factor 2 Proteoglycans Research Article endocrine system Mice 129 Strain Cèl·lules Neovascularization Physiologic Cell Migration Growth Factors Cell Adhesion Animals Birth Defects Biology Extracellular Matrix Adhesions Embryoid Bodies Embryonic Stem Cells lcsh:R fungi Proteins Extracellular Matrix Composition Mice Inbred C57BL carbohydrates (lipids)Cancer and Oncology Microvessels Cardiovascular Anatomy lcsh:Q Heparan Sulfate Proteoglycans Developmental Biology

description

Perlecan is a heparan sulfate proteoglycan assembled into the vascular basement membranes (BMs) during vasculogenesis. In the present study we have investigated vessel formation in mice, teratomas and embryoid bodies (EBs) in the absence of perlecan. We found that perlecan was dispensable for blood vessel formation and maturation until embryonic day (E) 12.5. At later stages of development 40% of mutant embryos showed dilated microvessels in brain and skin, which ruptured and led to severe bleedings. Surprisingly, teratomas derived from perlecan-null ES cells showed efficient contribution of perlecan-deficient endothelial cells to an apparently normal tumor vasculature. However, in perlecan-deficient EBs the area occupied by an endothelial network and the number of vessel branches were significantly diminished. Addition of FGF-2 but not VEGF(165) rescued the in vitro deficiency of the mutant ES cells. Furthermore, in the absence of perlecan in the EB matrix lower levels of FGFs are bound, stored and available for cell surface presentation. Altogether these findings suggest that perlecan supports the maintenance of brain and skin subendothelial BMs and promotes vasculo- and angiogenesis by modulating FGF-2 function.

year	journal	country	edition	language
2012-08-07

10.1371/journal.pone.0053715 http://hdl.handle.net/10550/53992