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The combined role of P- and E-selectins in atherosclerosis.

机译:P-选择素和E-选择素在动脉粥样硬化中的联合作用。

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摘要

P- and E-selectins are adhesion molecules mediating the first step in leukocyte extravasation. Because their function in leukocyte adhesion is overlapping, we hypothesized that there might be a combined effect of these selectins on the development of atherosclerotic lesions. We bred P- and E-selectin-double-deficient mice onto the low-density lipoprotein receptor (LDLR)-deficient background (LDLR-/- P/E-/-) and compared lesion development in these mice to that in mice wild type for both selectins (LDLR-/- P/E+/+). After 8 wk on atherogenic diet, the LDLR-/- P/E-/- mice developed fatty streaks in the aortic sinus that were five times smaller than those in LDLR-/- P/E+/+ mice. The density of macrophages in the fatty streaks was comparable between LDLR-/- P/E+/+ and LDLR-/- P/E-/- mice. After 22 wk on the diet, the lesions spread throughout the aorta but this process was delayed in LDLR-/- P/E-/- mice. At 37 wk on diet, the lesions progressed to the fibrous plaque stage in both genotypes. However, the lesions in the aortic sinus in LDLR-/- P/E-/- mice were 40% smaller and less calcified than those of LDLR-/- P/E +/+ mice. Our results suggest that P- and E-selectins together play an important role in both early and advanced stages of atherosclerotic lesion development.
机译:P-选择素和E-选择素是介导白细胞外渗第一步的粘附分子。因为它们在白细胞粘附中的功能是重叠的,所以我们假设这些选择素可能对动脉粥样硬化病变的发展有综合作用。我们将P-和E-选择素双缺陷小鼠繁殖到低密度脂蛋白受体(LDLR)缺陷背景(LDLR-/-P / E-/-)上,并将这些小鼠的病变发展与野生小鼠的病变发展进行了比较两个选择素的类型(LDLR-/-P / E + / +)。致动脉粥样化饮食8周后,LDLR-/-P / E-/-小鼠的主动脉窦出现脂肪条纹,是LDLR-/-P / E + / +小鼠的脂肪条纹的五倍。脂肪条纹中巨噬细胞的密度在LDLR-/-P / E + / +和LDLR-/-P / E-/-小鼠之间相当。饮食22周后,病变扩散到整个主动脉,但在LDLR-/-P / E-/-小鼠中该过程被延迟。在饮食的第37周,两种基因型的病灶都进展到纤维斑阶段。但是,与LDLR-/-P / E + / +小鼠相比,LDLR-/-P / E-/-小鼠的主动脉窦病变小40%,钙化程度低。我们的结果表明,P-选择素和E-选择素在动脉粥样硬化病变发展的早期和晚期均起着重要作用。

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