用冠状动脉和主动脉参考组织验证动脉粥样硬化研究中常用的人类和小鼠组织:在疾病发生和斑块稳定性方面有相似之处,但有显著差异。

Q3 Medicine
Rogier A. van Dijk MD, PhD , Robert Kleemann PhD , Alexander F. Schaapherder MD, PhD , Antoon van den Bogaerdt PhD , Ulf Hedin MD, PhD , Ljubica Matic PhD , Jan H.N. Lindeman MD, PhD
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引用次数: 0

摘要

目的:动脉粥样硬化过程的特征完全依赖于通过一致分级系统进行的组织学评估和分期。到目前为止,还没有将动脉粥样硬化研究中常用的实验模型和组织资源中的动脉粥样硬化过程与实际人类动脉粥样硬化过程进行正面比较。材料和方法:使用改良的美国心脏协会组织学分类法(Virmani分类法)对已建立的小鼠动脉粥样硬化模型和人类颈动脉内膜切除术标本中存在的动脉粥样硬化过程进行系统分级。各方面与在人类冠状动脉和主动脉动脉粥样硬化参考组织中观察到的动脉粥样硬化过程一致,这些参考组织可通过基于人类组织/器官供体材料的生物库获得。结果:除了主动脉病变中没有斑块内出血外,人类冠状动脉粥样硬化和主动脉动脉粥样硬化不同阶段的组织学特征相似。颈动脉内膜切除术样本均代表终末期“纤维钙化斑块”病变,尽管原发性病变偶尔会出现具有与冠状动脉/主动脉病变相似的大体形态的继发性、进行性和易损性病变。对于小鼠病变,观察到中间病变类型(“病理性内膜增厚”和“早期纤维动脉粥样硬化瘤”)的明显组织学相似性。然而,所研究的小鼠病变都没有进展到相当于晚期纤维动脉粥样硬化瘤或更严重的程度。在疾病发生方面观察到了显著的对比:尽管人类的疾病发生的特征是内膜中的间充质细胞流入,但最早的小鼠病变仅为内膜,具有内皮下积聚的泡沫细胞。缺乏间充质(和中间)反应。事实上,我们得出的结论是,在本研究中包括的所有小鼠模型中都没有“适应性内膜增厚”阶段。结论:Virmani冠状动脉粥样硬化分类法可用于实验性和临床性动脉粥样硬化的系统分级。这种组织学分级工具的应用显示出人类和小鼠动脉粥样硬化中期病变的明显相似性。然而,在疾病开始和晚期动脉粥样硬化病变方面观察到明显的对比。颈动脉内膜切除术都代表晚期纤维钙化斑块病变,尽管继发性早期病变可能存在于样本的子集中。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Validating human and mouse tissues commonly used in atherosclerosis research with coronary and aortic reference tissue: similarities but profound differences in disease initiation and plaque stability

Validating human and mouse tissues commonly used in atherosclerosis research with coronary and aortic reference tissue: similarities but profound differences in disease initiation and plaque stability

Validating human and mouse tissues commonly used in atherosclerosis research with coronary and aortic reference tissue: similarities but profound differences in disease initiation and plaque stability

Validating human and mouse tissues commonly used in atherosclerosis research with coronary and aortic reference tissue: similarities but profound differences in disease initiation and plaque stability

Objective

Characterization of the atherosclerotic process fully relies on histological evaluation and staging through a consensus grading system. So far, a head-to-head comparison of atherosclerotic process in experimental models and tissue resources commonly applied in atherosclerosis research with the actual human atherosclerotic process is missing.

Material and Methods

Aspects of the atherosclerotic process present in established murine atherosclerosis models and human carotid endarterectomy specimen were systematically graded using the modified American Heart Association histological classification (Virmani classification). Aspects were aligned with the atherosclerotic process observed in human coronary artery and aortic atherosclerosis reference tissues that were available through biobanks based on human tissue/organ donor material.

Results

Apart from absent intraplaque hemorrhages in aortic lesions, the histological characteristics of the different stages of human coronary and aortic atherosclerosis are similar. Carotid endarterectomy samples all represent end-stage “fibrous calcified plaque” lesions, although secondary, progressive, and vulnerable lesions with gross morphologies similar to coronary/aortic lesions occasionally present along the primary lesions. For the murine lesions, clear histological parallels were observed for the intermediate lesion types (“pathological intimal thickening,” and “early fibroatheroma”). However, none of the murine lesions studied progressed to an equivalent of late fibroatheroma or beyond. Notable contrasts were observed for disease initiation: whereas disease initiation in humans is characterized by a mesenchymal cell influx in the intima, the earliest murine lesions are exclusively intimal, with subendothelial accumulation foam cells. A mesenchymal (and medial) response are absent. In fact, it is concluded that the stage of “adaptive intimal thickening” is absent in all mouse models included in this study.

Conclusions

The Virmani classification for coronary atherosclerosis can be applied for systematically grading experimental and clinical atherosclerosis. Application of this histological grading tool shows clear parallels for intermediate human and murine atherosclerotic lesions. However, clear contrasts are observed for disease initiation, and late stage atherosclerotic lesions. Carotid endarterectomy all represent end-stage fibrous calcified plaque lesions, although secondary earlier lesions may present in a subset of samples.

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