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甲醛处理的白蛋白含有单体和聚合物形式,它们被肝脏的内皮细胞和库普弗细胞以不同方式清除:清除剂受体异质性的证据。

Formaldehyde treated albumin contains monomeric and polymeric forms that are differently cleared by endothelial and Kupffer cells of the liver: evidence for scavenger receptor heterogeneity.

作者信息

Jansen R W, Molema G, Harms G, Kruijt J K, van Berkel T J, Hardonk M J, Meijer D K

机构信息

Department of Pharmacology and Therapeutics, University Centre for Pharmacy, Groningen, The Netherlands.

出版信息

Biochem Biophys Res Commun. 1991 Oct 15;180(1):23-32. doi: 10.1016/s0006-291x(05)81249-5.

Abstract

Formaldehyde treated albumin (F-HSA) was found to consist of a monomeric and a polymeric fraction. Both fractions were primarily endocytosed by rat liver sinusoidal cells. However, immunohistochemical staining of endocytosed material showed that the relative contribution of the endothelial and Kupffer cells in uptake of the monomer and the polymer differed significantly, with the monomer mainly having an endothelial cell- and the polymer predominantly having a Kupffer cell pattern of distribution. To directly confirm these heterogeneous patterns, we injected in vivo the 125I-labeled F-HSA fractions and isolated the endothelial and Kupffer cells by centrifugal elutriation. 73.7% of the monomeric F-HSA was found in endothelial cells and only 14.9% was found in Kupffer cells. In contrast, the polymeric F-HSA (1500 kD) was mainly endocytosed by Kupffer cells (71%), whereas the endothelial cells contributed only for 24% in hepatic uptake. In vivo studies and isolated perfused rat liver experiments showed that endocytosis of both monomer and polymer was inhibited by co-administration of polyinosinic acid, a well known inhibitor for scavenger receptors, indicating that these receptors on endothelial and Kupffer cells are mainly involved in this uptake process.

摘要

经甲醛处理的白蛋白(F-HSA)被发现由单体和聚合物部分组成。这两个部分主要由大鼠肝窦状细胞进行内吞作用。然而,对内吞物质的免疫组织化学染色显示,内皮细胞和库普弗细胞在摄取单体和聚合物中的相对贡献存在显著差异,单体主要以内皮细胞分布模式为主,而聚合物则主要以库普弗细胞分布模式为主。为了直接证实这些异质性模式,我们在体内注射了125I标记的F-HSA部分,并通过离心淘洗分离出内皮细胞和库普弗细胞。发现73.7%的单体F-HSA存在于内皮细胞中,仅14.9%存在于库普弗细胞中。相比之下,聚合物F-HSA(1500 kD)主要被库普弗细胞内吞(71%),而内皮细胞在肝脏摄取中的贡献仅为24%。体内研究和离体灌注大鼠肝脏实验表明,同时给予多聚肌苷酸(一种众所周知的清道夫受体抑制剂)可抑制单体和聚合物的内吞作用,这表明内皮细胞和库普弗细胞上的这些受体主要参与了这一摄取过程。

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