Schulich Heart Centre, Sunnybrook Health Sciences Centre, University of Toronto, Toronto, Ontario, Canada.
Faculty of Health Sciences, Ben Gurion University of the Negev, Beer-Sheva, Israel.
Catheter Cardiovasc Interv. 2021 Feb 15;97(3):437-442. doi: 10.1002/ccd.28870. Epub 2020 Apr 3.
To create an experimental chronic total occlusion (CTO) model with calcification by dietary modification (cholesterol, calcium carbonate, vitamin D) and local injection of pro-calcification factors (dipotassium phosphate, calcium chloride, and bone morphogenetic protein-2 [BMP-2]).
Percutaneous revascularization of CTOs frequently fails in heavily calcified occlusions. Development of novel approaches requires a reproducible preclinical model of calcified CTO.
CTOs were created in 18 femoral arteries of 9 New Zealand White rabbits using the thrombin injection model. Dietary interventions included a high cholesterol diet (0.5% or 0.25%), calcium carbonate (150 mg × 3-5 days/week), and vitamin D (50,000 U × 3-5 days/week). In selected animals, BMP-2 (1-4 μg), dipotassium phosphate, and calcium chloride were injected locally at the time of CTO creation. Animals were sacrificed at 2 weeks (n = 4 arteries), 6 weeks (n = 4 arteries), and 10-12 weeks (n = 14 arteries).
CTOs showed evidence of chronic lipid feeding (foam cells) and chronic inflammation (intimal/medial fibrosis and microvessels, inflammatory cells, internal elastic lamina disruption). In calcium/vitamin D supplemented rabbits, mineralization (calcification and/or ossification) was evident as early as 2 weeks post CTO creation, and in 78% of the overall arteries. Mineralization changes were not present in the absence of calcium/vitamin D dietary supplements. Mineralization occurred in 85% of BMP-treated arteries and 60% of arteries without BMP.
Complex mineralization occurs in preclinical CTO models with dietary supplementation of cholesterol with vitamin D and calcium.
通过饮食调整(胆固醇、碳酸钙、维生素 D)和局部注射促钙化因子(磷酸二氢钾、氯化钙和骨形态发生蛋白-2[BMP-2])来创建具有钙化的实验性慢性完全闭塞(CTO)模型。
在严重钙化闭塞的情况下,经皮血运重建治疗 CTO 经常失败。开发新方法需要可重复的钙化 CTO 临床前模型。
使用凝血酶注射模型在 9 只新西兰白兔的 18 条股动脉中创建 CTO。饮食干预包括高胆固醇饮食(0.5%或 0.25%)、碳酸钙(150mg×3-5 天/周)和维生素 D(50000U×3-5 天/周)。在选定的动物中,在创建 CTO 时局部注射 BMP-2(1-4μg)、磷酸二氢钾和氯化钙。在 2 周(n=4 条动脉)、6 周(n=4 条动脉)和 10-12 周(n=14 条动脉)处死动物。
CTO 显示出慢性脂质喂养(泡沫细胞)和慢性炎症(内膜/中膜纤维化和微血管、炎症细胞、内弹性膜破坏)的证据。在补充钙/维生素 D 的兔子中,早在 CTO 创建后 2 周就出现了矿物质化(钙化和/或骨化),并且在 78%的总体动脉中。在没有钙/维生素 D 饮食补充的情况下,没有出现矿物质化变化。在接受 BMP 治疗的动脉中,85%出现了矿物质化,而在没有 BMP 的动脉中,60%出现了矿物质化。
在饮食补充胆固醇、维生素 D 和钙的 CTO 模型中,会发生复杂的钙化。
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