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Age-related decline in prostacyclin synthesis by human aortic endothelial cells. Qualitative and quantitative analysis.

机译:人主动脉内皮细胞前列环素合成的年龄相关性下降。定性和定量分析。

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摘要

To investigate the functional alteration of human aortic endothelial cells with aging, prostacyclin synthesis was qualitatively and quantitatively examined. The endothelial cells of human aortas and umbilical veins or inferior vena cavae were immunohistochemically examined and found positive for prostacyclin, but the intensity of aortic endothelial cells from older subjects was low. In addition to the endothelial cells, smooth muscle cells in the thickened intima, not the media, of the aorta were also immunoreactive. Endothelial cells were successfully cultured from human aortas obtained from infants through aged subjects and were subdivided into three groups: young, middle, and old. Prostacyclin synthesis by endothelial cells from all types of blood vessels was extremely great at the primary culture, but decreased abruptly in the following subcultures. Among the aortic endothelial cells, the young group synthesized the largest amount of prostacyclin in a conventional culture condition, with synthesis progressively decreasing in the older groups. The in vitro prostacyclin biosynthesis was supported by the qualitative analysis on the tissue sections. These results indicate that prostacyclin synthesis of the aortic endothelial cells decreases with age, but intimal smooth muscle cells potentially have a back-up mechanism and substitute this synthesis to some extent. The decreased synthesis of prostacyclin with age may play an important role in the development and advancement of thrombosis and atherosclerosis.
机译:为了研究人类主动脉内皮细胞随着年龄的增长而发生的功能改变,对前列环素的合成进行了定性和定量研究。对人主动脉和脐静脉或下腔静脉的内皮细胞进行了免疫组织化学检查,发现前列环素呈阳性,但老年受试者的主动脉内皮细胞强度较低。除内皮细胞外,在主动脉增厚的内膜而不是中层的平滑肌细胞也具有免疫反应性。血管内皮细胞成功地从年龄较大的婴儿中获得的人主动脉中培养,并分为三组:年轻人,中年人和老人。在初次培养中,来自各种类型血管的内皮细胞的前列环素合成极高,但在随后的继代培养中急剧下降。在主动脉内皮细胞中,年轻组在常规培养条件下合成了最大量的前列环素,而老组则逐渐减少。对组织切片的定性分析支持体外前列环素的生物合成。这些结果表明,主动脉内皮细胞的前列环素合成随着年龄的增长而降低,但是内膜平滑肌细胞可能具有备用机制,并在某种程度上替代了该合成。随着年龄的增长,前列环素的合成减少可能在血栓形成和动脉粥样硬化的发生和发展中起重要作用。

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