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五聚体 CRP 通过抑制 mmLDL-单核细胞相互作用来减弱 mmLDL 的炎症作用。

Pentameric CRP attenuates inflammatory effects of mmLDL by inhibiting mmLDL--monocyte interactions.

机构信息

Baker IDI Heart & Diabetes Institute, Melbourne, Victoria 8008, Australia.

出版信息

Atherosclerosis. 2012 Oct;224(2):384-93. doi: 10.1016/j.atherosclerosis.2012.07.039. Epub 2012 Aug 10.

Abstract

Previous studies have reported that C-reactive protein (CRP) interacting with low-density lipoproteins (LDL) affects macrophage activation and LDL uptake. However, the physiological relevance of CRP-LDL interaction with circulating monocytes remains elusive. Moreover, recent studies have shown that CRP exists in two isoforms with partly opposing characteristics pentameric (pCRP) and monomeric CRP (mCRP). Here we investigated the effects of CRP interacting with minimally modified low-density lipoprotein (mmLDL) interaction in regard to events involved in formation of atherosclerotic plaque. We analyzed the effect of mmLDL on human monocytes and found a substantial increase in monocyte activation as evaluated by CD11b/CD18 expression and increased monocyte adhesion under static and under shear flow conditions to human endothelial cells. Monocyte adhesion and activation was attenuated by pCRP via the prevention of mmLDL binding to monocytes. These anti-inflammatory properties of pCRP were lost when it dissociates to the monomeric form. Our results elucidate the physiological relevance of the CRP-mmLDL interaction and furthermore confirm the importance of the previously described pCRP dissociation to mCRP as a localized inflammatory "activation" mechanism.

摘要

先前的研究报告指出,C 反应蛋白(CRP)与低密度脂蛋白(LDL)相互作用会影响巨噬细胞的激活和 LDL 的摄取。然而,CRP-LDL 与循环单核细胞相互作用的生理相关性仍不清楚。此外,最近的研究表明,CRP 存在两种具有部分相反特征的同工型:五聚体(pCRP)和单体 CRP(mCRP)。在这里,我们研究了 CRP 与最小修饰的低密度脂蛋白(mmLDL)相互作用对动脉粥样硬化斑块形成相关事件的影响。我们分析了 mmLDL 对人单核细胞的影响,发现单核细胞的激活明显增加,其评估指标为 CD11b/CD18 的表达,以及在静态和剪切流条件下人内皮细胞的单核细胞黏附增加。pCRP 通过阻止 mmLDL 与单核细胞结合,减轻了单核细胞的黏附和激活。当 pCRP 解离为单体形式时,其抗炎特性丧失。我们的研究结果阐明了 CRP-mmLDL 相互作用的生理相关性,并进一步证实了先前描述的 pCRP 向 mCRP 解离作为局部炎症“激活”机制的重要性。

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