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衰老对小鼠静脉循环的影响。

Effect of ageing on the murine venous circulation.

机构信息

Center for Molecular and Vascular Biology, KU Leuven, Campus Gasthuisberg, Leuven, Belgium.

出版信息

Histochem Cell Biol. 2012 Apr;137(4):537-46. doi: 10.1007/s00418-012-0913-8. Epub 2012 Jan 18.

DOI:10.1007/s00418-012-0913-8
PMID:22252159
Abstract

The effect of ageing on the morphology of veins, venous valves and arteries was investigated in male wild-type mice using an adapted procedure with injection of a silicone polymer Microfil(®) that preserves morphology of the vasculature. Throughout the hind limb the arterial, but not the venous, lumen area and wall thickness were significantly greater in 24-month as compared to 10-week-old C57BL/6 mice. Venous valves were most frequently located at the sapheno-femoral vein junction in the lower extremities, and appeared thicker at the base supported by structurally intact collagen fibers, and thinner towards the proximal end of the valve leaflet, with less organized collagen. Overall, valves were less supported by structurally intact collagen at 24 months as compared to 10 weeks. Endothelial expression of CD31, endothelial protein C receptor or von Willebrand factor (VWF) was not affected by age, while thrombomodulin expression was lower in aged versus young arteries. At both ages, expression of VWF was lower at venous valves versus veins. Evaluation of the blood coagulation profile revealed that aged mice had shortened prothrombin time, elevated plasma levels of factor (F)VII, FVIII and VWF and increased neutrophil and platelet counts. Thus, our data indicate that in mice with ageing, venous valves become more fragile, in association with a procoagulant and inflammatory blood phenotype. Taken together, we found that the procoagulant state in ageing, is accompanied by mild vascular changes.

摘要

本研究采用改良的硅酮聚合物 Microfil®注射方法,研究了衰老对雄性野生型小鼠静脉、静脉瓣和动脉形态的影响。在整个后肢中,与 10 周龄 C57BL/6 小鼠相比,24 月龄小鼠的动脉管腔面积和壁厚显著增大,但静脉管腔面积和壁厚没有显著变化。静脉瓣最常位于下肢的股隐静脉交界处,其基部由结构完整的胶原纤维支撑,显得较厚,而瓣叶的近端较薄,胶原排列较不规则。总的来说,与 10 周龄相比,24 月龄时静脉瓣的结构完整性胶原支撑较少。内皮细胞 CD31、内皮蛋白 C 受体或血管性血友病因子(VWF)的表达不受年龄影响,而年龄较大的动脉中血栓调节蛋白的表达较低。在两个年龄段,与静脉相比,静脉瓣的 VWF 表达均较低。凝血状态评估显示,老年小鼠的凝血酶原时间缩短,血浆因子(F)VII、FVIII 和 VWF 水平升高,中性粒细胞和血小板计数增加。因此,我们的数据表明,在衰老的小鼠中,静脉瓣变得更加脆弱,同时伴有促凝和炎症的血液表型。综上所述,我们发现衰老时的促凝状态伴随着轻微的血管变化。

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本文引用的文献

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Genes regulating lymphangiogenesis control venous valve formation and maintenance in mice.调控淋巴管生成的基因控制小鼠静脉瓣膜的形成和维持。
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Diameter and compliance of the greater saphenous vein - effect of age and nitroglycerine.大隐静脉的直径和顺应性——年龄及硝酸甘油的影响
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