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乙型肝炎病毒包膜 L 蛋白衍生的生物纳米胶囊:进入人肝细胞的细胞附着和进入机制。

Hepatitis B virus envelope L protein-derived bio-nanocapsules: mechanisms of cellular attachment and entry into human hepatic cells.

机构信息

Graduate School of Bioagricultural Sciences, Nagoya University, Furo-cho, Chikusa-ku, Nagoya 464-8601, Japan.

出版信息

J Control Release. 2012 Jun 10;160(2):322-9. doi: 10.1016/j.jconrel.2011.11.004. Epub 2011 Nov 10.

DOI:10.1016/j.jconrel.2011.11.004
PMID:22100387
Abstract

A bio-nanocapsule (BNC) is a hollow nanoparticle consisting of an approximately 100-nm-diameter liposome with about 110 molecules of hepatitis B virus (HBV) surface antigen L protein embedded as a transmembrane protein. BNC can encapsulate various drugs and genes and deliver them specifically to human hepatic cells based on the ability of HBV to recognize human hepatocyte, which is integrated in the N-terminal region of L protein. However, it is elusive whether the cellular attachment and entry into hepatic cells of BNC utilize the early infection mechanism of HBV. In this study, we have found that while all human hepatic cells show distinct affinities for BNC compared to non-hepatic cells, primary hepatocytes shows the highest efficiency for cellular binding and incorporation of BNC. Amounts of BNCs bound weakly and strongly to cell membranes and those entered into the cells varied significantly depending on the types of human hepatic cells. The weak and strong binding modes of BNC are likely mediated through binding to two distinct HBV receptors (heparin-mediated low-affinity and unidentified high-affinity receptors), which play major roles in the early infection mechanism of HBV. The rates of cellular uptake of BNC are similar to those reported for HBV. The BNCs incorporated into the cells are swiftly sorted to either early endosomes or macropinosomes and then to late endosomes and/or lysosomes. These findings strongly suggest that BNC is bound to and incorporated into human hepatic cells according to the early infection mechanism of HBV.

摘要

一种生物纳米胶囊(BNC)是一种中空的纳米颗粒,由一个大约 100nm 直径的脂质体组成,其中大约有 110 个乙型肝炎病毒(HBV)表面抗原 L 蛋白分子作为跨膜蛋白嵌入其中。BNC 可以封装各种药物和基因,并根据 HBV 识别人肝细胞的能力,将其特异性递送到人肝细胞中,这种能力整合在 L 蛋白的 N 端区域。然而,BNC 进入肝细胞的细胞附着和进入是否利用 HBV 的早期感染机制仍然难以捉摸。在这项研究中,我们发现,虽然所有的人肝细胞与非肝细胞相比,对 BNC 表现出明显的亲和力,但原代肝细胞对 BNC 的细胞结合和内化效率最高。BNC 与细胞膜的弱结合和强结合的数量以及进入细胞的数量因人类肝细胞的类型而异。BNC 的弱结合和强结合模式可能是通过与两种不同的 HBV 受体(肝素介导的低亲和力和未鉴定的高亲和力受体)结合介导的,这两种受体在 HBV 的早期感染机制中起主要作用。BNC 的细胞摄取率与 HBV 的报道相似。进入细胞的 BNC 迅速被分拣到早期内体或巨胞饮体,然后进入晚期内体和/或溶酶体。这些发现强烈表明,BNC 根据 HBV 的早期感染机制与人类肝细胞结合并被其内化。

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