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HDL in innate and adaptive immunity

机译:HDL具有先天性和适应性免疫

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During infections or acute conditions high-density lipoproteins cholesterol (HDL-C) levels decrease very rapidly and HDL particles undergo profound changes in their composition and function. These changes are associated with poor prognosis following endotoxemia or sepsis and data from genetically modified animal models support a protective role for HDL. The same is true for some parasitic infections, where the key player appears to be a specific and minor component of HDL, namely apoL-1. The ability of HDL to influence cholesterol availability in lipid rafts in immune cells results in the modulation of toll-like receptors, MHC-II complex, as well as B- and T-cell receptors, while specific molecules shuttled by HDL such as sphingosine-1-phosphate (S1P) contribute to immune cells trafficking. Animal models with defects associated with HDL metabolism and/or influencing cell cholesterol efflux present features related to immune disorders. All these functions point to HDL as a platform integrating innate and adaptive immunity. The aim of this review is to provide an overview of the connection between HDL and immunity in atherosclerosis and beyond.
机译:在感染或急性疾病期间,高密度脂蛋白胆固醇(HDL-C)的含量会迅速下降,并且HDL颗粒的成分和功能会发生深刻变化。这些变化与内毒素血症或败血症后的不良预后有关,转基因动物模型的数据支持HDL的保护作用。对于某些寄生虫感染也是如此,其中关键因素似乎是HDL的特定和次要成分,即apoL-1。 HDL影响免疫细胞脂质筏中胆固醇利用率的能力导致调节toll样受体,MHC-II复合物以及B细胞和T细胞受体,而HDL穿梭的特定分子(如鞘氨醇- 1-磷酸(S1P)有助于免疫细胞运输。具有与HDL代谢有关和/或影响细胞胆固醇外排的缺陷的动物模型具有与免疫疾病有关的特征。所有这些功能都将HDL视为集成了先天免疫和自适应免疫的平台。这篇综述的目的是概述HDL与动脉粥样硬化及其他疾病中免疫力之间的联系。

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