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Matrix vesicles in the fibrous cap of atherosclerotic plaque: possible contribution to plaque rupture

机译:动脉粥样硬化斑块的纤维帽中的基质囊泡:可能导致斑块破裂

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摘要

Plaque rupture is the most common type of plaque complication and leads to acute ischaemic events such as myocardial infarction and stroke. Calcification has been suggested as a possible indicator of plaque instability. Although the role of matrix vesicles in the initial stages of arterial calcification has been recognized, no studies have yet been carried out to examine a possible role of matrix vesicles in plaque destabilization. Tissue specimens selected for the present study represented carotid specimens obtained from patients undergoing carotid endarterectomy. Serial frozen cross-sections of the tissue specimens were cut and mounted on glass slides. The thickness of the fibrous cap (FCT) in each advanced atherosclerotic lesion, containing a well developed lipidecrotic core, was measured at its narrowest sites in sets of serial sections. According to established criteria, atherosclerotic plaque specimens were histologically subdivided into two groups: vulnerable plaques with thin fibrous caps (FCT <100 μm) and presumably stable plaques, in which fibrous caps were thicker than 100 μm. Twenty-four carotid plaques (12 vulnerable and 12 presumably stable plaques) were collected for the present analysis of matrix vesicles in fibrous caps. In order to provide a sufficient number of representative areas from each plaque, laser capture microdissection (LCM) was carried out. The quantification of matrix vesicles in ultrathin sections of vulnerable and stable plaques revealed that the numbers of matrix vesicles were significantly higher in fibrous caps of vulnerable plaques than those in stable plaques (8.908±0.544 versus 6.208±0.467 matrix vesicles per 1.92 μm2 standard area; P= 0.0002). Electron microscopy combined with X-ray elemental microanalysis showed that some matrix vesicles in atherosclerotic plaques were undergoing calcification and were characterized by a high content of calcium and phosphorus. The percentage of calcified matrix vesicles/microcalcifications was significantly higher in fibrous caps in vulnerable plaques compared with that in stable plaques (6.705±0.436 versus 5.322±0A94; P= 0.0474). The findings reinforce a view that the texture of the extracellular matrix in the thinning fibrous cap of atherosclerotic plaque is altered and this might contribute to plaque destabilization.
机译:斑块破裂是斑块并发症的最常见类型,并导致急性缺血性事件,例如心肌梗塞和中风。已建议钙化可作为斑块不稳定性的可能指标。尽管已经认识到基质小泡在动脉钙化的初始阶段中的作用,但是尚未进行研究以研究基质小泡在斑块失稳中的可能作用。选择用于本研究的组织标本代表从接受颈动脉内膜切除术的患者获得的颈动脉标本。切下组织样本的连续冷冻横截面并将其安装在载玻片上。在一系列连续切片的最狭窄部位测量每个晚期动脉粥样硬化病变中纤维帽(FCT)的厚度,该病变包含发达的脂质/坏死核心。根据既定标准,将动脉粥样硬化斑块标本在组织学上分为两组:脆弱的斑块和薄的纤维帽(FCT <100μm)和大概稳定的斑块,其中纤维帽的厚度大于100μm。收集二十四个颈动脉斑块(12个易损斑块和12个大概稳定的斑块),用于目前在纤维帽中的基质囊泡的分析。为了从每个斑块中提供足够数量的代表性区域,进行了激光捕获显微切割(LCM)。对易损和稳定斑块的超薄切片中的基质囊泡进行定量分析显示,易损斑块的纤维盖中基质囊泡的数量显着高于稳定斑块中的囊泡(8.908±0.544对6.208±0.467基质囊泡,每1.92μm 2 标准面积; P = 0.0002)。电子显微镜结合X射线元素显微分析表明,动脉粥样硬化斑块中的一些基质囊泡正在钙化,钙和磷含量高。与易损斑块相比,易损斑块中纤维帽的钙化基质囊泡/微钙化百分比显着更高(6.705±0.436对5.322±0A94; P = 0.0474)。这些发现强化了这样一种观点,即动脉粥样硬化斑块变薄的纤维帽中细胞外基质的质地发生了改变,这可能会导致斑块不稳定。

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