PDGF-BB regulates splitting angiogenesis in skeletal muscle by limiting VEGF-induced endothelial proliferation

PDGF-BB regulates splitting angiogenesis in skeletal muscle by limiting VEGF-induced endothelial proliferation

VEGF induces normal or aberrant angiogenesis depending on its dose in the microenvironment around each producing cell in vivo. This transition depends on the balance between VEGF-induced endothelial stimulation and PDGF-BB-mediated pericyte recruitment, and co-expression of PDGF-BB normalizes aberra...

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Veröffentlicht in:Angiogenesis (London) 2018-11, Vol.21 (4), p.883-900
Hauptverfasser: Gianni-Barrera, R., Butschkau, A., Uccelli, A., Certelli, A., Valente, P., Bartolomeo, M., Groppa, E., Burger, M. G., Hlushchuk, R., Heberer, M., Schaefer, D. J., Gürke, L., Djonov, V., Vollmar, B., Banfi, A.
Format: Artikel
Sprache:eng
Schlagworte:
Aberration
Angiogenesis
Animals
Becaplermin - metabolism
Biomedical and Life Sciences
Biomedicine
Cancer Research
Cardiology
Cell Biology
Cell Proliferation
Constraining
Endothelial Cells - cytology
Endothelial Cells - metabolism
Enlargement
Expansion
Gene expression
Kinases
Mechanical stimuli
Mice
Mice, SCID
Muscle, Skeletal - blood supply
Muscle, Skeletal - cytology
Muscle, Skeletal - metabolism
Muscles
Musculoskeletal system
Myoblasts
Neovascularization, Physiologic
Oncology
Ophthalmology
Original Paper
Overexpression
Pericytes
Platelet-derived growth factor
Platelet-derived growth factor BB
Reduction
Shear stress
Signaling
Skeletal muscle
Splitting
Surgical implants
Vascular endothelial growth factor
Vascular Endothelial Growth Factor A - metabolism
Vascular Endothelial Growth Factor Receptor-2 - metabolism
Vascular endothelial growth factor receptors
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Zusammenfassung:VEGF induces normal or aberrant angiogenesis depending on its dose in the microenvironment around each producing cell in vivo. This transition depends on the balance between VEGF-induced endothelial stimulation and PDGF-BB-mediated pericyte recruitment, and co-expression of PDGF-BB normalizes aberrant angiogenesis despite high VEGF doses. We recently found that VEGF over-expression induces angiogenesis in skeletal muscle through an initial circumferential vascular enlargement followed by longitudinal splitting, rather than sprouting. Here we investigated the cellular mechanism by which PDGF-BB co-expression normalizes VEGF-induced aberrant angiogenesis. Monoclonal populations of transduced myoblasts, expressing similarly high levels of VEGF alone or with PDGF-BB, were implanted in mouse skeletal muscles. PDGF-BB co-expression did not promote sprouting and angiogenesis that occurred through vascular enlargement and splitting. However, enlargements were significantly smaller in diameter, due to a significant reduction in endothelial proliferation, and retained pericytes, which were otherwise lost with high VEGF alone. A time-course of histological analyses and repetitive intravital imaging showed that PDGF-BB co-expression anticipated the initiation of vascular enlargement and markedly accelerated the splitting process. Interestingly, quantification during in vivo imaging suggested that a global reduction in shear stress favored the initiation of transluminal pillar formation during VEGF-induced splitting angiogenesis. Quantification of target gene expression showed that VEGF-R2 signaling output was significantly reduced by PDGF-BB co-expression compared to VEGF alone. In conclusion, PDGF-BB co-expression prevents VEGF-induced aberrant angiogenesis by modulating VEGF-R2 signaling and endothelial proliferation, thereby limiting the degree of circumferential enlargement and enabling efficient completion of vascular splitting into normal capillary networks despite high VEGF doses.
ISSN:0969-6970
1573-7209
1573-7209
DOI:10.1007/s10456-018-9634-5