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携带不同密度碳水化合物配体的聚合物颗粒的细胞分布。

Cellular distribution of polymer particles bearing various densities of carbohydrate ligands.

作者信息

Adachi N, Maruyama A, Ishihara T, Akaike T

机构信息

Department of Biomolecular Engineering, Faculty of Bioscience and Biotechnology, Tokyo Institute of Technology, Yokohama, Japan.

出版信息

J Biomater Sci Polym Ed. 1994;6(5):463-79. doi: 10.1163/156856294x00446.

Abstract

The density effect of carbohydrate-ligands on nanometer-order particles (nanoparticles) upon cellular binding and internalization was investigated. Poly(vinylbenzyl-beta-D-lactonamide) (PVLA), a beta-galactose-carrying styrene homopolymer, was employed as a model ligand for the asialoglycoprotein receptors on hepatocytes. In order to control the surface ligand densities on the particles, PVLA was mixed with poly(vinylbenzyl-D-gluconamide) (PVGA), a PVLA analog without beta-galactose, and their mixtures were used as surface coatings. The particles with low ligand densities associated more with hepatocytes than high ligand density particles. The surface density of the ligand considerably influenced the cellular distribution. Most of the particles bearing high densities of ligands were found inside the cells, whereas particles with low ligand densities were found on the plasma membrane surface of the hepatocytes. These results were indicative of high densities of ligands on the surface requiring hepatocytes to internalize the particles promptly by receptor-mediated endocytosis, while low densities of ligands on the surface was not sufficient to internalize, but allowed particles to bind on the cell surface. These findings enabled us to regulate cellular distributions of particles by controlling ligand density on the surface.

摘要

研究了碳水化合物配体对纳米级颗粒(纳米粒子)细胞结合和内化的密度效应。聚(乙烯基苄基-β-D-内酰胺)(PVLA),一种携带β-半乳糖的苯乙烯均聚物,被用作肝细胞上脱唾液酸糖蛋白受体的模型配体。为了控制颗粒表面的配体密度,将PVLA与聚(乙烯基苄基-D-葡糖酰胺)(PVGA)(一种不含β-半乳糖的PVLA类似物)混合,并将它们的混合物用作表面涂层。低配体密度的颗粒比高配体密度的颗粒与肝细胞的结合更多。配体的表面密度对细胞分布有很大影响。大多数携带高配体密度的颗粒位于细胞内,而低配体密度的颗粒则位于肝细胞的质膜表面。这些结果表明,表面高配体密度需要肝细胞通过受体介导的内吞作用迅速内化颗粒,而表面低配体密度不足以内化,但允许颗粒结合在细胞表面。这些发现使我们能够通过控制表面配体密度来调节颗粒的细胞分布。

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