Vitamin B6 suppresses apoptosis of NM-1 bovine endothelial cells induced by homocysteine and copper
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- 作者:Naoko Endo ; Kazuo Nishiyama ; Masaaki Okabe ; Mitsuharu Matsumoto ; Hiroaki Kanouchi ; Tatsuzo Oka
- 关键词:Vitamin B6 ; Homocysteine ; Copper ; Antioxidant ; Apoptosis ; NM-1 cells
- 刊名:Biochimica et Biophysica Acta (BBA)/General Subjects
- 出版年:2007
- 出版时间:April 2007
- 年:2007
- 卷:1770
- 期:4
- 页码:571-577
- 全文大小:488 K
文摘
Hyperhomocysteinemia is an important risk factor for atherosclerosis. We previously reported that formation of early atherosclerosis in the rat aorta was associated with hyperhomocysteinemia and reduction of antioxidant activity caused by low concentration of vitamin B6 in vivo. In the present study, we examined effects of vitamin B6 on apoptosis of bovine endothelial cells (NM-1 cells) treated with homocysteine and copper. Homocysteine and copper induced extracellular hydrogen peroxide, intracellular ROS and cellular lipid peroxide levels. Cell viability was reduced to 30 % compared to that of control cells. On the other hand, pyridoxal treatment as well as EDTA treatment increased viability of NM-1 cells treated with homocysteine and copper to about 60 % , and significantly decreased extracellular hydrogen peroxide, intracellular ROS and cellular lipid peroxide levels. The treatment of catalase recovered cell viability and reduced the level of extracellular hydrogen peroxide and intracellular ROS. Cell death by homocysteine and copper was confirmed to be due to apoptosis by evaluation of DNA fragmentation and by TUNEL assay. However, apoptosis of NM-1 cells induced by homocysteine and copper was due to a caspase-independent pathway as it was not inhibited by the caspase inhibitor, Z-VAD-fmk. Apoptosis of NM-1 cells induced by homocysteine and copper accompanied with mitochondrial permeability but not cytochrome c release. These results suggest that pyridoxal treatment suppresses apoptosis of NM-1 cells induced by homocysteine and copper, most likely through antioxidant effects.