Skip to Content
Merck
  • Elastin degradation and calcification in an abdominal aorta injury model: role of matrix metalloproteinases.

Elastin degradation and calcification in an abdominal aorta injury model: role of matrix metalloproteinases.

Circulation (2004-11-17)
Dina M Basalyga, Dan T Simionescu, Wanfen Xiong, B Timothy Baxter, Barry C Starcher, Narendra R Vyavahare
ABSTRACT

Elastin calcification is a widespread feature of vascular pathology, and circumstantial evidence exists for a correlation between elastin degradation and calcification. We hypothesized that matrix metalloproteinase (MMP)-mediated vascular remodeling plays a significant role in elastin calcification. In the present studies, we determined that short-term periadventitial treatment of the rat abdominal aorta with low concentrations of calcium chloride (CaCl2) induced chronic degeneration and calcification of vascular elastic fibers in the absence of aneurysm formation and inflammatory reactions. Furthermore, the rate of progression of calcification depended on the application method and concentration of CaCl2 applied periarterially. Initial calcium deposits, associated mainly with elastic fibers, were persistently accompanied by elastin degradation, disorganization of aortic extracellular matrix, and moderate levels of vascular cell apoptosis. Application of aluminum ions (known inhibitors of elastin degradation) before the CaCl2-mediated injury significantly reduced elastin calcification and abolished both extracellular matrix degradation and apoptosis. We also found that MMP-knockout mice were resistant to CaCl2-mediated aortic injury and did not develop elastin degeneration and calcification. Collectively, these data strongly indicate a correlation between MMP-mediated elastin degradation and vascular calcification.

MATERIALS
Product Number
Brand
Product Description

Sigma-Aldrich
Anti-Macrophages/Monocytes Antibody, clone ED-1, clone ED-1, Chemicon®, from mouse