© 2002 by European Society of Cardiology
Copyright © 2001, European Society of Cardiology
Mechanisms underlying maintenance of smooth muscle cell quiescence in rat aorta: role of the cyclin dependent kinases and their inhibitors
Bristol Heart Institute, Bristol Royal Infirmary, Bristol BS2 8HW, UK
* Corresponding author. Bristol Heart Institute, Level 7, Bristol Royal Infirmary, Bristol BS2 8HW, UK. Tel.: +44-117-9283-587; fax: +44-117-9283-581
Objective: We sought to understand why smooth muscle cell proliferation is effectively repressed in intact rat aortic tissue. Methods: Quiescent isolated rat aortic smooth muscle cells and segments of intact rat aorta were stimulated with 10% serum and the time course of expression and activity of proteins involved in cell cycle control were determined. Results: After serum stimulation, smooth muscle cells in intact aortic tissue exhibit no proliferation, whereas isolated cells entered S phase 14–16 h later. Activation of ERKs 1 and 2, and induction of cyclin D1 occurred both in isolated cells and aortic tissue. Regulation of Cdk4, cyclin E and Cdk2 protein levels was also not different. Levels of the cyclin-dependent kinase inhibitors (CKIs), p16 and p27, were initially high in quiescent isolated cells and tissue; levels were downregulated by serum in isolated cells but not in aortic tissue. Cyclin D1/Cdk4, and cyclin E/Cdk2 kinases were active before S phase entry in isolated cells, but remained inactive in aortic tissue. Conclusions: Cell cycle entry is prevented in aortic tissue, and this is associated with an inability to downregulate p16 and p27 CKIs, and therefore to activate cyclin D1 and cyclin E associated kinase activities.
KEYWORDS Cell culture/isolation; Extracellular matrix; Protein kinases; Signal transduction; Smooth muscle