Cortical and retinal defects caused by dosage-dependent reductions in VEGF-A paracrine signaling

To determine the function of VEGF-A in nervous system development, we have utilized the Nestin promoter-driven Cre recombinase transgene, in conjunction with a conditional and hypomorphic VEGF-A allele, to lower VEGF-A activity in neural progenitor cells. Mice with intermediate levels of VEGF-A acti...

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Bibliographic Details
Published in:Developmental biology 2003-10, Vol.262 (2), p.225-241
Main Authors: Haigh, Jody J, Morelli, Paula I, Gerhardt, Holger, Haigh, Katharina, Tsien, John, Damert, Annette, Miquerol, Lucile, Muhlner, Ulrich, Klein, Rudiger, Ferrara, Napoleone, Wagner, Erwin F, Betsholtz, Christer, Nagy, Andras
Format: Article
Language:English
Subjects:
Animals
Blood vessel
Cerebral Cortex - abnormalities
Conditional gene inactivation
Cortex
Cre recombinase
Endothelium
Integrases - genetics
Integrases - metabolism
Intermediate Filament Proteins - genetics
Intermediate Filament Proteins - metabolism
Medicin och hälsovetenskap
Mice
Mice, Transgenic
Neovascularization, Physiologic - physiology
Nerve Tissue Proteins
Nervous system
Nestin
Paracrine Communication - physiology
Retina
Retina - abnormalities
Vascular Endothelial Growth Factor A - metabolism
VEGF-A
Viral Proteins - genetics
Viral Proteins - metabolism
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Summary:To determine the function of VEGF-A in nervous system development, we have utilized the Nestin promoter-driven Cre recombinase transgene, in conjunction with a conditional and hypomorphic VEGF-A allele, to lower VEGF-A activity in neural progenitor cells. Mice with intermediate levels of VEGF-A activity showed decreased blood vessel branching and density in the cortex and retina, resulting in a thinner retina and aberrant structural organization of the cortex. Severe reductions in VEGF-A led to decreases in vascularity and subsequent hypoxia, resulting in the specific degeneration of the cerebral cortex and neonatal lethality. Decreased neuronal proliferation and hypoxia was evident at E11.5, leading to increased neuronal apoptosis in the cortex by E15.5. In order to address whether the observed changes in the structural organization of the nervous system were due to a direct and autocrine role of VEGF-A on the neural population, we conditionally inactivated the main VEGF-A receptor, Flk1, specifically in neuronal lineages, by using the Nestin Cre transgene. The normality of these mice ruled out the possibility that VEGF-A/Flk1 signaling has a significant autocrine role in CNS development. VEGF-A dosage is therefore a critical parameter regulating the density of the vascular plexus in the developing CNS that is in turn a key determinant in the development and architectural organization of the nervous system.
ISSN:0012-1606
1095-564X
DOI:10.1016/S0012-1606(03)00356-7