Effects of benzo(a)pyrene on the contractile function of the thoracic aorta of Sprague-Dawley rats

To evaluate the possible vascular effects of an environment carcinogen benzo(a)pyrene (BaP). The cytotoxicit of BaP and rat liver S9 (0.25 mg/mL)-activated BaP were examined by MTT assay. Thoracic aortic rings were dissected from Sprague-Dawley rats. Contraction of aortic rings was induced by 60 mmo...

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Published in:Biomedical and environmental sciences Vol. 25; no. 5; p. 549
Main Authors: Gan, Tie Er, Xiao, Su Ping, Jiang, Ying, Hu, Hu, Wu, Yi Hua, Duerksen-Hughes, Penelope J, Sheng, Jian Zhong, Yang, Jun
Format: Journal Article
Language:English
Published: China 01-10-2012
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Summary:To evaluate the possible vascular effects of an environment carcinogen benzo(a)pyrene (BaP). The cytotoxicit of BaP and rat liver S9 (0.25 mg/mL)-activated BaP were examined by MTT assay. Thoracic aortic rings were dissected from Sprague-Dawley rats. Contraction of aortic rings was induced by 60 mmol/L KCl or 10(-6) mol/L phenylephrine (PE) in an ex-vivo perfusion system after BaP (100 μmol/L) incubation for 6 h. [Ca(2+)](i) was measured using Fluo-4/AM. For in-vivo treatment, rats were injected with BaP for 4 weeks (10 mg/kg, weekly, i.p.). BaP (1-500 μm) did not significantly affect cell viability; S9-activated BaP stimulated cell proliferation. BaP did not affect the contractile function of endothelium-intact or -denuded aortic rings. BaP did not affect ATP-induced ([Ca(2+)](i)) increases in human umbilical vein endothelial cells. In BaP-treated rats, heart rate and the number of circulating inflammatory cells were not affected. Body weight decreased while blood pressure increased significantly. The maximum aortic contractile responses to PE and KCl and the maximum aortic relaxation response to acetylcholine were significantly decreased by 25.0%, 34.2%, and 10.4%, respectively. These results suggest, in accordance with its DNA-damaging properties, that metabolic activation is a prerequisite for BaP-induced cardiovascular toxicity.
ISSN:0895-3988
DOI:10.3967/0895-3988.2012.05.008