AI Article Synopsis
- Cell proliferation in vascular cells plays a crucial role in processes like wound healing and diseases such as atherosclerosis.
- Proliferating endothelial and smooth muscle cells produce higher levels of reactive oxygen species (ROS) and oxidized LDL compared to non-proliferating cells, with ROS generation linked to specific signaling pathways.
- The study identifies a connection between cell proliferation and oxidative stress in vascular diseases, suggesting that while ROS generation is associated with proliferation, it is not necessary for cell division itself.
Article Abstract
Cell proliferation of vascular cells is a key feature in vascular biology, wound healing, and pathophysiological processes such as atherosclerosis and restenosis. In atherosclerotic intima, cell proliferation colocalizes with oxidized LDL that indicate a local oxidative stress. This study aims to investigate whether cell proliferation is causally related with extracellular ROS generation and subsequent LDL oxidation. Sparse proliferating endothelial and smooth muscle cells generate higher levels of extracellular ROS (O2*- and H2O2) and LDL oxidation than confluent contact-inhibited cells. During wound healing of confluent cell layer, cell proliferation associated with healing also induced enhanced extracellular ROS generation and LDL oxidation. Proliferation-associated extracellular ROS generation is mediated through mitogenic signaling pathways, involving ERK1/2 and PKC, but is independent of de novo DNA synthesis, gene expression and protein synthesis. Data obtained with inhibitors of oxidases suggest that proliferation-associated extracellular ROS are not generated by a single ROS-generating system and are not essential for cell proliferation. In conclusion, our data show that proliferating vascular cells (in sparse culture or during wound healing) generate high levels of extracellular ROS and LDL oxidation through regulation of ROS-generating systems by mitogenic signaling. This constitutes a link between proliferative events and oxidative stress/LDL oxidation in atherosclerotic lesions and restenosis.
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| http://dx.doi.org/10.1016/j.freeradbiomed.2003.09.008 | DOI Listing |
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