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β2-糖蛋白I在脂质体与肝细胞相互作用中的作用。

The role of beta2-glycoprotein I in liposome-hepatocyte interaction.

作者信息

Yan X, Morselt H W M, Scherphof G L, Poelstra K, Kamps J A A M

机构信息

Groningen University Institute for Drug Exploration, Department of Cell Biology, University of Groningen, The Netherlands.

出版信息

Biochim Biophys Acta. 2004 Dec 15;1667(2):208-14. doi: 10.1016/j.bbamem.2004.10.008.

Abstract

Adsorption of serum proteins to the liposomal surface plays a critical role in liposome clearance from the blood. The aim of this study was to investigate the role of liposome-adsorbed serum proteins in the interaction of liposomes with hepatocytes. We analyzed the serum proteins adsorbing to the surface of differently composed small unilamellar liposomes during incubation with human or rat serum, and found that one protein, with a molecular weight of around 55 kDa, adsorbed in a large amount to negatively charged liposomes containing phosphatidylserine (PS) or phosphatidylglycerol (PG). The binding was dependent on the liposomal charge density. The approximately 55-kDa protein was identified as beta2-glycoprotein I (beta2GPI) by Western blotting. Despite the high affinity of beta2GPI for strongly negatively charged liposomes, in vitro uptake and binding experiments with isolated rat hepatocytes, Kupffer cells or liver endothelial cells, and with HepG2 cells showed no enhancing effect of this protein on the association of negatively charged liposomes with any of these cells. On the contrary, an inhibitory effect was observed. We conclude that despite abundant adsorption to negatively charged liposomes, beta2GP1 inhibits, rather than enhances, liposome uptake by liver cells.

摘要

血清蛋白在脂质体表面的吸附在脂质体从血液中的清除过程中起着关键作用。本研究的目的是探讨脂质体吸附的血清蛋白在脂质体与肝细胞相互作用中的作用。我们分析了在与人或大鼠血清孵育期间吸附到不同组成的小单层脂质体表面的血清蛋白,发现一种分子量约为55 kDa的蛋白大量吸附到含有磷脂酰丝氨酸(PS)或磷脂酰甘油(PG)的带负电荷的脂质体上。这种结合取决于脂质体的电荷密度。通过蛋白质印迹法将约55 kDa的蛋白鉴定为β2-糖蛋白I(β2GPI)。尽管β2GPI对强负电荷脂质体具有高亲和力,但在与分离的大鼠肝细胞、库普弗细胞或肝内皮细胞以及HepG2细胞进行的体外摄取和结合实验中,该蛋白对带负电荷脂质体与这些细胞中任何一种的结合均未显示增强作用。相反,观察到了抑制作用。我们得出结论,尽管β2GP1大量吸附到带负电荷的脂质体上,但它抑制而非增强肝细胞对脂质体的摄取。

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