3-Deazaadenosine Inhibits Vasa Vasorum Neovascularization in Aortas of ApoE-/-/LDL-/- Double Knockout Mice

A. C. Langheinrich; D. Sedding; M. Kampschulte; J. Wilhelm; W. Haberbosch; W. S. Rau; E. L. Ritman; R. M. Bohle

doi:10.1055/s-2008-1073684

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Rofo 2008; 180 - VO_313_1
DOI: 10.1055/s-2008-1073684

3-Deazaadenosine Inhibits Vasa Vasorum Neovascularization in Aortas of ApoE-/-/LDL-/- Double Knockout Mice

AC Langheinrich ¹, D Sedding ¹, M Kampschulte ¹, J Wilhelm ¹, W Haberbosch ², WS Rau ¹, EL Ritman ³, RM Bohle ⁴

¹Universitätsklinikum Giessen, Diagnostische Radiologie, Giessen
²Suhl
³Rochester
⁴Homburg (Saar)

Congress Abstract

Ziele: Atherosclerosis and inflammation/angiogenesis are strongly associated including growth of vasa vasorum (VV) and plaque neovascularization, but a causative role for neovascularization has still not been established. Hence, we investigated the effect of 3-Deazaadenosine (c³Ado), an anti-inflammatory and anti-proliferative drug, on plaque progression and VV neovascularization in apoE-/-/LDL-/- double knockout mice. Methode: The arterial trees from apoE-/-/LDL-/- mice with, or without c³Ado at the age of 16 (n=10), 18 (n=8) and 20 weeks (n=7) were infused in situ with Microfil, and the aortas harvested and scanned with micro-CT (12µm cubic voxel). We characterized plaque volume and VV luminal volume along the descending aorta using Analyze 6.0 software. Cellular effects of c³Ado on human endothelial and vascular smooth muscle cells were investigated in cell cultures and on nylon cDNA expression arrays. Ergebnis: Lesions spatially connected to VV increased from 16 to 20 weeks significantly (p<0.001). The volume of atherosclerotic lesions was significantly reduced in animals treated with c3Ado (p<0.01). This was accompanied by a significant decrease of vasa vasorum neovascularization along the descending aorta (p<0.01). Using nylon cDNA expression arrays, we identified the regulation of anti-proliferative, anti-inflammatory genes in human smooth muscle cells which might be involved in the anti-angiogenetic effects of c³Ado. Moreover, c³Ado dose-dependently prevented the proliferation and migration of human coronary artery endothelial cells in vitro. Schlussfolgerung: The smaller lesion volume in animals treated with c³Ado was closely associated with a reduced VV neovascularization, suggesting a direct relationship between lesion growth and VV development.

Korrespondierender Autor: Langheinrich AC

Universitätsklinikum Giessen, Diagnostische Radiologie, Klinikstrasse 36, 35390 Giessen

E-Mail: Alexander.Langheinrich@radiol.med.uni-giessen.de

Imaging - Atherosclerosis - Angiogenesis - micro-CT - Vasa Vasorum