比较病理学:人与动物放射引起的冠状动脉疾病。

R Virmani, A Farb, A J Carter, R M Jones
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引用次数: 0

摘要

恶性肿瘤纵隔放射治疗后冠状动脉疾病的发生一直存在争议。然而,缺乏动脉粥样硬化危险因素的年轻人在放疗后冠状动脉病理的发展高度提示了因果关系。到目前为止,最令人信服的病理改变是外膜瘢痕和内侧萎缩,并伴有严重的内膜动脉粥样硬化疾病,包括核心坏死、纤维组织和钙化。冠状动脉粥样硬化患者支架植入术后腔内放射治疗的初步临床研究在治疗和预防再狭窄方面有很大的希望。然而,关于冠状动脉内放射治疗对人类的长期影响的数据很少或没有。因此,在动物模型中研究辐射的慢性影响,以预测可能发生在人类身上的情况,可能是很重要的。我们评估了1个月和6个月时猪冠状动脉中不同剂量(0.15-23.0微克/ 32P) β粒子放射支架的效果。1个月时,内膜和中膜形态发生剂量依赖性变化。高活性(>3微ci)引起中间坏死,纤维蛋白沉积在中膜和内膜,在支架支架周围区域弥散红细胞最为明显。在支架支架外仅见少见的平滑肌细胞(SMCs)和炎症细胞。在中等(1微ci)支架活性组中,新内膜被SMCs和富含蛋白多糖的基质扩张,管腔表面发生局灶性内皮化。支架支架附近有新生血管毛细血管和血管外红细胞。低活性(3.0微ci)放射性支架诱导明显的内膜增厚,变化类似于动脉粥样硬化,包括含有胆固醇的坏死碎片,周围有巨噬细胞聚集,纤维化和局灶性钙化。放射动脉与未放射动脉相比,动脉外膜增厚增加。中等支架活性(1.0微ci)也显示出更大的内膜增厚(与对照支架相比),并且主要由富含蛋白聚糖基质中的SMCs组成。在
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Comparative pathology: radiation-induced coronary artery disease in man and animals.

The occurrence of coronary artery disease following mediastinal radiation for malignancies has long been debated. However, the development of coronary pathology in young individuals following radiation who lack risk factors for atherosclerosis is highly suggestive of a cause-and-effect relationship. By far the most convincing pathologic changes are adventitial scarring and medial atrophy with severe intimal atherosclerotic disease consisting of necrotic core, fibrous tissue, and calcification. Initial clinical studies in patients with coronary atherosclerosis treated with intraluminal radiation following stenting hold great promise in the treatment and prevention of restenosis. There are little or no data, however, on long-term effects of intra-coronary radiation therapy in man. Therefore, it may be important to study the chronic effects of radiation in animal models in order to predict what is likely to occur in humans. We evaluated the effects of varying doses (0.15-23.0 microCi of 32P) of beta-particle-emitting radioactive stents in pig coronary arteries at 1 and 6 months. At 1 month, there were dose-dependent changes in the morphology of the intima and media. High activities (>3 microCi) caused medial necrosis with fibrin deposition in the media and intima, with interspersed red cells most marked in regions surrounding the stent struts. Only rare smooth muscle cells (SMCs) and inflammatory cells were seen away from the stent struts. In the intermediate (1 microCi) stent activity group, the neointima was expanded by SMCs and a proteoglycan-rich matrix with focal endothelialization of the luminal surface. Neovascular capillaries and extravascular red cells were present adjacent to stent struts. At low activities (<0.5 microCi), the neointima was significantly smaller than control stents and consisted of SMCs and matrix with complete endothelialization of the luminal surface. The neointimal cell density of the media and intima decreased with increasing doses of radiation. In pigs 6 months after radioactive stenting (activities ranging from 0.5-12 microCi 32P), >3.0 microCi radioactive stents induced marked neointimal thickening, with changes similar to atherosclerosis, consisting of necrotic debris containing cholesterol clefts surrounded by macrophage collections, fibrosis, and focal calcification. There was increased adventitial thickening in the radiated vs non-radiated arteries. The intermediate stent activity (1.0 microCi) also showed greater neointimal thickening (vs control stents) and consisted mostly of SMCs in a proteoglycan-rich matrix. At <1.0 microCi, there were minimal differences seen between radiated and control non-radiated stented arteries. The media was unevenly injured in all stent activities and varied from less than to significantly greater than controls. These data suggest that radiation-induced coronary atherosclerosis seen in man is partially simulated in normal porcine coronary arteries 6 months following high-dose beta-particle-emitting radioactive stent placement. There is greater fibrosis and thickness of the adventitia and focal attenuation of the media in man and severe luminal narrowing in pig coronary arteries treated with high doses of radiation. Only long-term clinical follow up and careful autopsy studies will determine if endoluminal or intra-arterial radiation is a viable means of reducing restenosis in man.

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