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全长无RNA乙肝核心颗粒的表达、纯化及特性分析

Expression, purification and characterization of full-length RNA-free hepatitis B core particles.

作者信息

Broos Katleen, Vanlandschoot Peter, Maras Marleen, Robbens Johan, Leroux-Roels Geert, Guisez Yves

机构信息

Laboratory of Plant Physiology, Department of Biology, 171 Groenenborgerlaan, Building U, 6th Floor, CGB University of Antwerp, 2020 Antwerpen, Belgium.

出版信息

Protein Expr Purif. 2007 Jul;54(1):30-7. doi: 10.1016/j.pep.2007.02.006. Epub 2007 Feb 20.

Abstract

The nucleocapsid or core particle of the hepatitis B virus has become one of the favourite recombinant vaccine carriers for foreign peptides, proteins and stimulatory oligonucleotides. The core protein consists of three regions: an N-terminal, a central and a C-terminal region that can accommodate the addition or insertion of the foreign sequences. The protamine-like C-terminal region that binds host RNA randomly during recombinant particle formation is often truncated. It is commonly thought that these truncations do not affect particle assembly. Recent studies have demonstrated that the C-terminal domains mediate a glycosaminoglycan-dependent attachment of nucleocapsids to the plasma membranes of host cells. This interaction might well contribute to the immunogenicity of nucleocapsids. Testing the hypothesis that full-length particles might be safer and superior for the induction of an immune response against the nucleocapsids and inserted sequences, requires the availability of purified particles. In this report, we detail a novel method for the synthesis and purification of full-length core particles essentially free of RNA from Escherichia coli.

摘要

乙肝病毒的核衣壳或核心颗粒已成为用于外源肽、蛋白质和刺激性寡核苷酸的最受欢迎的重组疫苗载体之一。核心蛋白由三个区域组成:一个N端区域、一个中央区域和一个C端区域,后者能够容纳外源序列的添加或插入。在重组颗粒形成过程中随机结合宿主RNA的类鱼精蛋白C端区域常常被截短。人们普遍认为这些截短不会影响颗粒组装。最近的研究表明,C端结构域介导核衣壳通过糖胺聚糖依赖的方式附着于宿主细胞的质膜。这种相互作用很可能有助于核衣壳的免疫原性。要验证全长颗粒在诱导针对核衣壳和插入序列的免疫反应方面可能更安全且更具优势这一假设,需要获得纯化的颗粒。在本报告中,我们详细介绍了一种从大肠杆菌中合成和纯化基本不含RNA的全长核心颗粒的新方法。

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