一个钙化的慢性完全闭塞的临床前模型。

A calcified chronic total occlusion preclinical model.

机构信息

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.

出版信息

Catheter Cardiovasc Interv. 2021 Feb 15;97(3):437-442. doi: 10.1002/ccd.28870. Epub 2020 Apr 3.

DOI:10.1002/ccd.28870

PMID:32243080

Abstract

OBJECTIVE

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]).

BACKGROUND

Percutaneous revascularization of CTOs frequently fails in heavily calcified occlusions. Development of novel approaches requires a reproducible preclinical model of calcified CTO.

METHODS

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).

RESULTS

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.

CONCLUSIONS

Complex mineralization occurs in preclinical CTO models with dietary supplementation of cholesterol with vitamin D and calcium.

摘要

目的

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。

背景

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。

方法

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。

结果

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。