首页> 外文会议>IEEE Engineering in Medicine and Biology Annual Conference >Rolling and adhesion of monocytes to early atherosclerotic lesions of apolipoprotein E-/-(apoE-/-) mice requires P-selectin, PSGL-1, α{sub}4 integrin and VCAM-1
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Rolling and adhesion of monocytes to early atherosclerotic lesions of apolipoprotein E-/-(apoE-/-) mice requires P-selectin, PSGL-1, α{sub}4 integrin and VCAM-1

机译:单核细胞对早期动脉粥样硬化病变的滚动和粘附性载脂蛋白E - / - / - / - / - )小鼠需要p-selectin,psgl-1,α{sub} 4整合蛋白和vcam-1

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To investigate the molecular basis of mononuclear cell rolling and adhesions to vascular endothelium prone to develop atherosclerotic lesion, isolated carotid arteries from ApoE-/- and other relevant mice were perfused under physiological shearstress conditions. Carotid arteries from 10-12 weeks old ApoE-/- and C57BL/6 wide-type mice fed a Western diet for 4-5 weeks, representing early atherosclerotic lesions according to vessel histology, supported mononuclear cell (U937) attachment, rollingand adhesion, while carotid arteries from an atherosclerosis-resistant strain (BALB/C) showed no adhesion. Antibody blocking assays showed that mononuclear rolling and adhesion were significantly inhibited by treating the vessel with P-selectin antibodyor treating U937 with anti-PSGL-1. Treating the vessel with VCAM-1 antibody or treating U937 with α{sub}4β{sub}1 integrin antibody caused rolling velocities to increase (from 86±4 to 167±7 um/s). This suggests that mononuclear cell can attach, rolland adhere on early atherosclerotic endothelium via the P-selectin--PSGL-1 and VCAM-1--α{sub}4β{sub}1 pathways.
机译:为了研究单核细胞轧制的分子基础和粘连的血管内皮,易于发育动脉粥样硬化病变,在物理鞘乳病条件下灌注来自ApoE的颈动脉 - 和其他相关小鼠的分离的颈动脉。来自10-12周的颈动脉 - / - 和C57BL / 6宽型小鼠喂养西方饮食4-5周,根据血管组织学,支持单核细胞(U937)附着,轧制和粘附,而动脉粥样硬化菌株(BALB / C)的颈动脉显示出没有粘附。抗体阻断测定显示通过用抗PSGL-1处理U937的P型选择蛋白抗体仪来显着抑制单核轧制和粘附。用VCAM-1抗体治疗血管或用α{Sub}4β{sub} 1整联蛋白抗体治疗U937,导致滚动速度增加(从86±4到167±7 um / s)。这表明单核细胞可以通过p-SELETIN - PSGL-1和VCAM-1 - α}4β{u} 1途径将单核细胞连接在早期的动脉粥样硬化内皮上。

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