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肝脏和巨噬细胞的去唾液酸糖蛋白受体在识别和结合的结构特异性上的差异。

The differences in structural specificity for recognition and binding between asialoglycoprotein receptors of liver and macrophages.

作者信息

Ozaki K, Lee R T, Lee Y C, Kawasaki T

机构信息

Department of Biological Chemistry, Faculty of Pharmaceutical Sciences, Kyoto University, Japan.

出版信息

Glycoconj J. 1995 Jun;12(3):268-74. doi: 10.1007/BF00731329.

DOI:10.1007/BF00731329
PMID:7496141
Abstract

The Gal/GalNAc-specific lectin on the surface of rat peritoneal macrophages (macrophage asialoglycoprotein binding protein, M-ASGP-BP), which consists of a single polypeptide chain of 42 kDa, can form a homo-oligomeric receptor exhibiting high affinity for asialoorosomucoid (ASOR) [Ozaki K., Ii M., Itoh N., Kawasaki T. (1992) J Biol Chem 267: 9229-35]. In this study, the binding affinity of M-ASGP-BP was studied by using a series of synthetic or natural glycosides as inhibitors of 125I-ASOR binding to recombinant M-ASGP-BP expressed on COS-1 cells (rM-ASGP-BP), and the results were compared with those of human hepatic lectin (HHL) on Hep G2 cells. Clustering of multiple Gal (or GalNAc) residues increased the binding affinity to M-ASGP-BP as well as to HHL. In contrast to HHL and other mammalian hepatic lectins, rM-ASGP-BP bound Gal residues tighter than GalNAc residues. A galactose-terminated triantennary N-glycoside, having one N-acetyl-lactosamine unit on the 6 branch and two N-acetyl-lactosamine units on the 3 branch of the trimannosyl core structure, showed affinity enhancement of approximately 10(5) over a monovalent ligand for HHL, while the same glycopeptide showed enhancement of about 2000-fold for rM-ASGP-BP. These results suggest that spatial arrangements of sugar combining sites and subunit organization of macrophage and hepatic lectins are different.

摘要

大鼠腹膜巨噬细胞表面的半乳糖/ N - 乙酰半乳糖胺特异性凝集素(巨噬细胞去唾液酸糖蛋白结合蛋白,M - ASGP - BP)由一条42 kDa的单多肽链组成,可形成对去唾液酸血清类黏蛋白(ASOR)具有高亲和力的同型寡聚受体[小崎K.,饭井M.,伊藤N.,川崎T.(1992年)《生物化学杂志》267: 9229 - 35]。在本研究中,通过使用一系列合成或天然糖苷作为125I - ASOR与COS - 1细胞上表达的重组M - ASGP - BP(rM - ASGP - BP)结合的抑制剂,研究了M - ASGP - BP的结合亲和力,并将结果与Hep G2细胞上的人肝凝集素(HHL)进行比较。多个半乳糖(或N - 乙酰半乳糖胺)残基的聚集增加了对M - ASGP - BP以及HHL的结合亲和力。与HHL和其他哺乳动物肝凝集素不同,rM - ASGP - BP与半乳糖残基的结合比与N - 乙酰半乳糖胺残基的结合更紧密。一种在三甘露糖核心结构的6分支上有一个N - 乙酰乳糖胺单元且在3分支上有两个N - 乙酰乳糖胺单元的半乳糖末端三天线N - 糖苷,对HHL而言,其对单价配体的亲和力增强了约10^5倍,而对rM - ASGP - BP而言,相同的糖肽显示出约2000倍的增强。这些结果表明巨噬细胞和肝凝集素的糖结合位点的空间排列和亚基组织是不同的。

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