Protective effects of Astragaloside and Quercetin on rat myocardial cells after hypoxia.

Jiong-yu HU; Yue-sheng Huang; Hua-pei Song; Dong-xia Zhang; Fei Xiang; Zhi-gang Zhu; Miao Teng; Qiong Zhang

Return

Protective effects of Astragaloside and Quercetin on rat myocardial cells after hypoxia.

Author: Jiong-Yu HU ¹ ; Yue-Sheng HUANG ; Hua-Pei SONG ; Dong-Xia ZHANG ; Fei XIANG ; Zhi-Gang ZHU ; Miao TENG ; Qiong ZHANG
Author Information

1. Institute of Burn Research, Southwest Hospital, State Key Laboratory of Trauma, Burns and Combined Injury, Third Military Medical University, Chongqing 400038, PR China.
Publication Type:Journal Article
MeSH: Animals; Cell Hypoxia; Myocytes, Cardiac; drug effects; metabolism; Quercetin; pharmacology; Rats; Rats, Sprague-Dawley; Saponins; pharmacology; Triterpenes; pharmacology
From: Chinese Journal of Burns 2007;23(3):175-178
CountryChina
Language:Chinese
Abstract:
OBJECTIVETo investigate and compare the protective effects of Astragaloside IV (AST) and Quercetin (QUE) on rat myocardial cells after their exposure to hypoxia, and to determine their dose-effect relationship.
METHODSMyocardial cells from fetal SD rat were cultured in vitro and divided into 7 groups: i.e. A (hypoxia), B (hypoxia and 100 mg/L of QUE), C (hypoxia and 50 mg/L of QUE), D (hypoxia and 25 mg/L of QUE), E (hypoxia and 50.0 mg/L of AST), F (hypoxia and 25.0 mg/L of AST), G (hypoxia and 12.5 mg/L AST) H(hypoxia and 10 mg/L of VitE) groups. Different doses of AST and QUE were added into the culture media cells in each group before the myocardial cells receiving hypoxia for 12 hrs. The number of viable cells (CCK-8) and the content of lactate dehydrogenase (LDH), superoxide dismutase (SOD), malondialdehyde (MDA), active oxygen (ROS, with detection only in A, C, F and H groups) were determined after hypoxia.
RESULTSThe amount of LDH, MDA, ROS (C, F groups) in group B - G decreased significantly compared with those of group A, while the number of viable cells and the SOD content increased significantly. The protective effects were better in group B - G than that of the group H. With the same dosage, levels of LDH, CCK-8 in AST-treated groups were significantly lower than those in QUE-treated group (the number of viable cells in group C, F was 0.454 +/- 0.018, 0.471 +/- 0.017, and the content of lactate dehydrogenase was 2800 +/- 9,2312 +/- 52). There were no significant differences in MDA, SOD and ROS levels between AST and QUE treated groups (ROS in C and F groups were 16.0 +/- 5.3 vs 22.4 +/- 8.7, P > 0.05).
CONCLUSIONAST and QUE might be beneficial in the protection of myocardial cells against hypoxia because of attenuation of oxidative damage. The protective effects of both AST and QUE are better than that of VitE, and that of AST is better than QUE as shown by a decrease in the amount of LDH and increase in the number of viable cells with the same dosage, but no obvious difference is shown between them in attenuating oxidative damage.