小鼠动脉粥样硬化模型的建立

Yiquan Dai, Xiaoxiao Yan, Xiao‐Ru Liu, Yichen Lin, Hongyu Chen
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引用次数: 0

摘要

目的建立稳定可靠的小鼠动脉粥样硬化(AS)模型,规范AS模型鉴定的主要过程。方法采用高脂饲料(hfd)喂养载脂蛋白E (ApoE)基因敲除小鼠(ApoE-/-)建立小鼠AS模型。16周后测定体重、血糖、血压、血脂,并对主动脉进行油红O和苏木精染色,评价AS斑块。结果与C57BL/6J正常饮食(和)组相比,ApoE-/- hfd小鼠的胆固醇[(20.09±1.02)mmol/L]和低密度脂蛋白胆固醇[(6.84±0.65)mmol/L]显著升高[总胆固醇(TC):(2.04±0.07)mmol/L, LDL-C:(0.25±0.01)mmol/L, F=190.543, 82.795, P<0.01]。全主动脉油红O染色显示,ApoE-/-+ hfd小鼠AS病变大小[(22.09±3.49)%]较ApoE-/-+小鼠[(1.46±0.96)%,F=118.558, P<0.01]显著增加。主动脉根部横切面分析也得到了类似的结果。苏木精和伊红(HE)染色显示主动脉根横断面典型的As斑块。结论hfd有效促进了ApoE-/-小鼠AS的发展。建立基因鉴定-概况分析-血脂分析-形态学分析的流程对AS模型进行验证。小鼠AS模型的建立为体内AS相关疾病的研究提供了有价值的工具。关键词:动脉粥样硬化;基因敲除小鼠;低密度脂蛋白;胆固醇;Lorta
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Establishment of mouse atherosclerotic model
Objective To establish a stable and reliable mouse atherosclerotic (AS) model, and standardize principal process of AS model identification. Methods The mouse AS model was developed by feeding apolipoprotein E (ApoE) gene knockout mice (ApoE-/-) on high-fat diet (hfd). Sixteen weeks later, the body weight, blood sugar, blood pressure and blood lipid were determined, and aortas were stained with oil red O and hematoxylin to evaluate the AS plaque. Results Cholesterol [(20.09±1.02) mmol/L] and low density lipoprotein cholesterol [(6.84±0.65) mmol/L] of ApoE-/- mice with hfd were significantly increased as compared with that in C57BL/6J normal diet (nd) group [total cholesterol (TC): (2.04±0.07) mmol/L, LDL-C: (0.25±0.01) mmol/L, F=190.543, 82.795, P<0.01]. Oil Red O staining of entire aorta showed that AS lesion size in ApoE-/-+ hfd mice [(22.09±3.49)%] was dramatically increased as compared with that in ApoE-/-+ nd mice [(1.46±0.96)%, F=118.558, P<0.01]. Similar result was obtained from cross-sections of aortic root analysis. Hematoxylin and eosin (HE) staining of cross-sections of aorta root showed typical As plaques. Conclusion The hfd treatment successfully promoted AS development in ApoE-/- mice. The process of gene identification-general situation analysis-blood lipid analysis-morphologic analysis was established to verify AS model. The establishment of mouse AS model provides a valuable tool for the study of AS-related diseases in vivo. Key words: Atherosclerosis; Gene knock out mice; Low density lipoprotein; Cholesterol; Lorta
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