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在重组烟草花叶病毒表面表达的疟疾抗原表位。

Malarial epitopes expressed on the surface of recombinant tobacco mosaic virus.

作者信息

Turpen T H, Reinl S J, Charoenvit Y, Hoffman S L, Fallarme V, Grill L K

机构信息

Biosource Technologies, Inc., Vacaville, CA 95688.

出版信息

Biotechnology (N Y). 1995 Jan;13(1):53-7. doi: 10.1038/nbt0195-53.

Abstract

Using malaria as a model disease, we engineered the surface of tobacco mosaic tobamovirus (TMV) for presentation of selected epitopes to the mammalian immune system. The TMV coat protein is a well-characterized and abundant self-assembling polymer previously shown to be a highly immunogenic carrier. Selected B-cell epitopes were either inserted into the surface loop region of the TMV coat protein or fused to the C terminus using the leaky stop signal derived from the replicase protein reading frame. Tobacco plants systemically infected with each of these constructs contained high titers of genetically stable recombinant virus, enabling purification of the chimeric particles in high yield. Symptoms induced in tobacco ranged from a normal mosaic pattern similar to that induced by the parental U1 strain to a unique bright yellow mosaic. As measured by quantitative ELISA against synthetic peptide standards, wild type TMV coat protein and fusion protein synthesized by the leaky stop mechanism coassembled into virus particles at the predicted ratio of approximately 20:1. Recombinant plant viruses have the potential to meet the need for scalable and cost effective production of subunit vaccines that can be easily stored and administered.

摘要

以疟疾作为模型疾病,我们对烟草花叶烟草花叶病毒(TMV)的表面进行了改造,以便向哺乳动物免疫系统呈递选定的表位。TMV外壳蛋白是一种特征明确且丰富的自组装聚合物,先前已证明它是一种高度免疫原性的载体。选定的B细胞表位要么插入TMV外壳蛋白的表面环区,要么利用源自复制酶蛋白阅读框的渗漏终止信号与C末端融合。用这些构建体中的每一个进行系统感染的烟草植株都含有高滴度的遗传稳定重组病毒,从而能够高产率地纯化嵌合颗粒。烟草中诱导产生的症状从类似于亲本U1株系诱导产生的正常花叶图案到独特的亮黄色花叶图案不等。通过针对合成肽标准品的定量ELISA测定,野生型TMV外壳蛋白和通过渗漏终止机制合成的融合蛋白以大约20:1的预测比例共同组装成病毒颗粒。重组植物病毒有潜力满足对可扩展且经济高效生产的亚单位疫苗的需求,这种疫苗易于储存和施用。

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