关于大脂质体肝内跨内皮转运的机制

On the mechanism of hepatic transendothelial passage of large liposomes.

作者信息

Romero E L, Morilla M J, Regts J, Koning G A, Scherphof G L

机构信息

Groningen University Institute for Drug Exploration, Faculty of Medical Sciences, Department of Physiological Chemistry, University of Groningen, The Netherlands.

出版信息

FEBS Lett. 1999 Apr 1;448(1):193-6. doi: 10.1016/s0014-5793(99)00364-6.

DOI:10.1016/s0014-5793(99)00364-6

PMID:10217439

Abstract

Liposomes of 400 nm in diameter can cross the 100-nm fenestrations in the endothelium of the hepatic sinusoid, provided they contain phosphatidylserine (PS) but not phosphatidylglycerol (PG) [Daemen et al. (1997) Hepatology 26, 416]. We present evidence indicating that (i) the PS effect does not involve a pharmacological action of this lipid on the size of the fenestrations, (ii) fluid-type but not solid-type PS liposomes have access to the hepatocytes and (iii) the lack of uptake of PG liposomes by hepatocytes is not due to a lack of affinity of the hepatocytes for PG surfaces. We conclude that the mechanism responsible for the uptake of large PS-containing liposomes by hepatocytes in vivo involves a mechanical deformation of these liposomes during their passage across the endothelial fenestrations.

摘要

直径为400纳米的脂质体能够穿过肝血窦内皮细胞上100纳米的窗孔，前提是它们含有磷脂酰丝氨酸（PS）而非磷脂酰甘油（PG）[Daemen等人（1997年），《肝脏病学》26卷，416页]。我们提供的证据表明：（i）PS的作用并不涉及这种脂质对窗孔大小的药理作用；（ii）流体型而非固体型的PS脂质体能够进入肝细胞；（iii）肝细胞不摄取PG脂质体并非由于肝细胞对PG表面缺乏亲和力。我们得出结论，体内肝细胞摄取含大量PS脂质体的机制涉及这些脂质体在穿过内皮窗孔过程中的机械变形。

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关于大脂质体肝内跨内皮转运的机制

On the mechanism of hepatic transendothelial passage of large liposomes.

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