Effect of Metallothionein and Rosuvastatin on Atherosclerosis and SM22α Expression in ApoE-deficient Mice

doi:10.3969/j.issn.1674-5817.2014.06.004

Abstract

Abstract: Objective To research the effect of metallothionein(MT) and rosuvastatin on atherosclerosis and smooth muscle 22 alpha (SM22α) expression in ApoE-deficient mice. Methods Thirty 6-week-old ApoE- deficient male mice were divided into hyperlipidemia model group, rosuvastatin group, and MT group randomly, fed with fatty diet for 13 weeks. Ten background strain C57BL/6J (wild type) male mice were selected as normal control group,and fed with normal diet for 13 weeks. After 13 weeks, eyeballs were extracted and blood was taken from ApoE-deficient mice for detecting lipid profile, then the mice were executed and the aortas were dissociated, 5 mm vessel in aorta arch were taken and fixed in 10% formalin, then treated with paraffin imbedding, slicing, HE staining and SM22α immunohistochemistry staining; some specimen was preserved in -80 ℃ refrigerator, total protein and RNA were extracted, West Blot and RT-PCR were taken.To observe morphology changes of aortic wall, to analyse SM22α expression intensity of aorta tissue qualitatively and quantitively. Results The blood lipid level in rosuvastation group was lower than that in hyperlipidemia model group (P<0.05). There is no difference in the blood lipid level between MT group and hyperlipidemia model group (P>0.05). Compared with normal control group, intimal thickness, plaque volume increased and SM22α protein and mRNA expression decreased in hyperlipidemia model group. Compared with hyperlipidemia model group, intimal thickness, plaque volume decreased and SM22α protein and mRNA expression increased in MT and rovustatin group. Conclusion The MT has no effect on lipid profile, rovustatin can lower blood lipid obviously. MT and rovustatin can alleviate atherosclerosis lesions and increase SM22α protein and mRNA expression in aorta of ApoE-deficient mice. Their anti-athrosclerosis effect is related to up regulating SM22α expression.

Key words: Metallothionein, Rosavastation, ApoE-deficient mice, Atherosclerosis, SM22α

CLC Number:

Q95-33

ZHU Zhong-sheng,LU Ya-li. Effect of Metallothionein and Rosuvastatin on Atherosclerosis and SM22α Expression in ApoE-deficient Mice[J]. Laboratory Animal and Comparative Medicine, 2014, 34(6): 449-453. DOI: 10.3969/j.issn.1674-5817.2014.06.004.

References

[1] Diaz-Ruiz A, Vacio-Adame P, Monroy-Noyola A, et al.Metallothionein-II inhibits lipid peroxidation and improves functional recovery after transient brain ischemia and reperfusion in rats[J]. Oxid Med Cell Longev, 2014, 436429. doi: 10.1155/2014/436429. Epub 2014 Feb 25.
[2] Arai H.Oxidative modification of lipoproteins[J]. Subcell Biochem, 2014, 77:103-114.
[3] Lv P, Miao SB, Shu YN, et al.Phosphorylation of smooth muscle 22α facilitates angiotensin II-induced ROS production via activation of the PKCδ-P47phox axis through release of PKCδ and actin dynamics and is associated with hypertrophy and hyperplasia of vascular smooth muscle cells in vitro and in vivo[J]. Circ Res, 2012, 111(6):697-707.
[4] Desjardins F, Sekkali B, Verreth W, et al.Rosuvastatin increases vascular endothelial PPARgamma expression and corrects blood pressure variability in obese dyslipidaemic mice[J]. Eur Heart J, 2008, 29(1):128-137.
[5] Tanaka T, Sato H, Doi H, et al. Runx2 represses myocardin-mediated differentiation and facilitates osteogenic conversion of vascular smooth muscle cells [J]. Mol Cell Biol, 2008, 28(3):1147-1160.
[6] Won KJ, Lee HM, Lee CK, et al.Protein tyrosine phosphatase SHP-2 is positively involved in platelet-derived growth factor-signaling in vascular neointima formation via the reactive oxygen species-related pathway[J]. J Pharmacol Sci, 2011, 115(2):164-175.
[7] Cherian MG.Metabolism of orally administered cadmium-metallothionein in mice[J]. Environ Health Perspect, 1979, 28:127-130.
[8] Wamhoff BR, Hoofnagle MH, Burns A, et al.A G/C element mediates repression of the SM22alpha promoter within phenotypically modulated smooth muscle cells in experimental atherosclerosis[J]. Circ Res, 2004, 95(10): 981-988.
[9] 程云会, 韩梅, 温进坤, 等. 收缩蛋白在血管新生内膜形成过程中的表达变化及其对血管收缩力的影响[J].中国病理生理杂志, 2005, 21(11):21l1-2l15.
[10] Chen R, Zhang F, Song L, et al.Transcriptome profiling reveals that the SM22α-regulated molecular pathways contribute to vascular pathology[J]. J Mol Cell Cardiol, 2014, 72: 263-272.

[1]	WENG Jiayi, MA Xuexing, LI Yuan, SUN Kangyun. CD137 Signaling Promotes Cardio-cerebral Angiogenesis in Mice Through Regulating Endothelial-mesenchymal Transition [J]. Laboratory Animal and Comparative Medicine, 2021, 41(5): 418-425.
[2]	XU Zhenkun, REN Liwei, YUAN Tao. Establishment of Atherosclerosis Model Induced by Feeding High-fat Diet Plus Carotid Artery Balloon Injury in Rabbits with Insulin Resistance [J]. Laboratory Animal and Comparative Medicine, 2020, 40(1): 28-32.
[3]	SUN Li-hua, ZHANG Ying, CAO Gui-qiu, LI Peng, HU Qiang, ZHANG Ya-ling, XING Shi-feng. Mechanism of Circulating Endothelial MicroRNA Related to Atherosclerosis Induced by Inflammatory Response of Macrophages in Mouse [J]. Laboratory Animal and Comparative Medicine, 2019, 39(3): 201-207.
[4]	WANG Cong, CHEN Xiao-xue, YANG Shao-ling, WANG Feng-ling, FAN Lin-yan, HE Qian-qian. Comparative Analysis of Rabbit Carotid Atherosclerosis Models Established by Collar And Air-drying Method [J]. Laboratory Animal and Comparative Medicine, 2019, 39(3): 208-212.
[5]	ZHANG Mei-ying, YANG Wei, WU Hong-lian, DONG Wan-wei, ZHOU Sheng-lai,YU Yang, WANG Wei, GUO Xiao-chong, ZHENG Zhi-hong. A Preliminary Study on Phenotype of 5-Lipoxygenase Transgenic Mice [J]. Laboratory Animal and Comparative Medicine, 2015, 35(4): 265-270.
[6]	SI Xu-wei, XI Sai-fei, XU Xiao-ping, ZHUGE Fu-yuan, CHEN Xiao-zhen, CAI Yue-qin, CHEN Min-li. Comparative Study on Formation of Atherosclerosis and Phospholipase A2 Expression in ZDF and SD Rats [J]. Laboratory Animal and Comparative Medicine, 2015, 35(1): 10-16.
[7]	CHEN Fang-ming, PAN Yong-ming, CHEN Liang, SHI Yuan, ZHU Ke-yan, YU Xu-ping, CHEN Min-li. Expression of Inflammatory Factors in Atherosclerosis Model of Bama Mini-pig [J]. Laboratory Animal and Comparative Medicine, 2014, 34(3): 193-198.
[8]	ZHANG Yi, ZHAN Wei-wei, WU Yong-ji, ZHOU Wu-gang, CHEN Dong-rui, JIANG Wei-min, ZHENG Lin. Effects of High Fat Diet on Arterial Ring's Tension in SD Rats [J]. Laboratory Animal and Comparative Medicine, 2014, 34(2): 126-130.
[9]	ZHANG Xiao-feng, WANG Guo-hua, GUAN Yu, XIA Jing. Effects of Hyperhomocysteinemia (HHcy) on Depression in Rats [J]. Laboratory Animal and Comparative Medicine, 2011, 31(4): 276-279.
[10]	CHEN Jia-wei，ZHOU Shi-bei，TAN Zhi-ming. Preliminary Study on Correlation between Plasma Titers of Ox-LDL Auto-antibody and Extent of Atherosclerosis in Mice Auto-antibody and Extent of Atherosclerosis in Mice [J]. Laboratory Animal and Comparative Medicine, 2010, 30(4): 261-264.
[11]	HUANG Cheng-lei1,LI Tian-qi1,QIAO Wei-wei2,LUO Xin-ping1,LI Jian1,NI Huan-chun1,SHEN Wei1,LI Hong-zhi3,JIN Bo1,SHI Hai-ming1. Establishment and Evaluation on Modified Athesclerotic plaque Model in Rabbit [J]. Laboratory Animal and Comparative Medicine, 2007, 27(1): 6-10.
[12]	CAI Bao-Xiang, XIE Mei-Lin, GU Zhen-Lun. Experimental Study on Rabbit Atherosclerotic Plaque Rupture Model [J]. Laboratory Animal and Comparative Medicine, 2004, 24(4): 200-203.
[13]	LI Dong-Bao, CHEN Hui, SHEN Lu-Hua. The Serial Experimental Research of Atherosclerosis Model in Rabbit Iliac Artery [J]. Laboratory Animal and Comparative Medicine, 2000, 20(4): 213-216.
[14]	LU Jing-Fen-1, MAO You-Xia-1, YANG Yun-2, WANG Yi-Cheng-1, SHI Yi-Xu-2, ZHOU Qiu-Hua-2. Influence of Magnetized Water on the Experimental Hyperlipemia and Atherosclerosis in Rabbits [J]. Laboratory Animal and Comparative Medicine, 2000, 20(4): 227-229.
[15]	SUN Jing-Fang. Establishment of NJS Inbred Strain from KM Mouse Ⅰ. Breeding Method and History [J]. Laboratory Animal and Comparative Medicine, 1996, 16(3,4): 131-133.