Author:
Lindblom Per,Gerhardt Holger,Liebner Stefan,Abramsson Alexandra,Enge Maria,Hellström Mats,Bäckström Gudrun,Fredriksson Simon,Landegren Ulf,Nyström Henrik C.,Bergström Göran,Dejana Elisabetta,Östman Arne,Lindahl Per,Betsholtz Christer
Abstract
Several platelet-derived growth factor (PDGF) and vascular endothelial growth factor (VEGF) family members display C-terminal protein motifs that confer retention of the secreted factors within the pericellular space. To address the role of PDGF-B retention in vivo, we deleted the retention motif by gene targeting in mice. This resulted in defective investment of pericytes in the microvessel wall and delayed formation of the renal glomerulus mesangium. Long-term effects of lack of PDGF-B retention included severe retinal deterioration, glomerulosclerosis, and proteinuria. We conclude that retention of PDGF-B in microvessels is essential for proper recruitment and organization of pericytes and for renal and retinal function in adult mice.
Publisher
Cold Spring Harbor Laboratory
Subject
Developmental Biology,Genetics
Reference38 articles.
1. Allavena P ., Dejana, E., Bussolino, F., Vecchi, A., and Mantovani, A. 1995. Cytokine regulation of endothelial cells. In Cytokines: A practical approach (ed. F.R. Balkwill), pp. 225-245. IRL Press, Oxford.
2. Pericytes: Cell Biology and Pathology
3. Characterization of the retention motif in the C-terminal part of the long splice form of platelet-derived growth factor A-chain.
4. Functional binding of secreted molecules to heparan sulfate proteoglycans in Drosophila
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