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重组溶瘤新城疫病毒的产生及来自两个转基因的完整IgG抗体的表达。

Generation of a recombinant oncolytic Newcastle disease virus and expression of a full IgG antibody from two transgenes.

作者信息

Pühler F, Willuda J, Puhlmann J, Mumberg D, Römer-Oberdörfer A, Beier R

机构信息

Therapeutic Research Group Oncology, Bayer Schering Pharma AG, Berlin, Germany.

出版信息

Gene Ther. 2008 Mar;15(5):371-83. doi: 10.1038/sj.gt.3303095. Epub 2008 Jan 17.

DOI:10.1038/sj.gt.3303095
PMID:18200068
Abstract

The most advanced oncolytic Newcastle disease virus (NDV) strains that are used in clinical trials for the treatment of cancer are wild-type mesogenic strains. These virus strains have an inherent, nongenetically engineered, oncolytic activity and selectively replicate in tumor cells but not in normal human cells. To date no investigations have been performed with genetically engineered mesogenic NDV regarding the oncolytic activity. We describe here the generation of recombinant viruses of the mesogenic naturally oncolytic NDV strain MTH68. We show that not only one, but also two additional transgenes coding for amino-acid chains with a molecular weight of 25 and 50 kDa can be inserted into the viral genome without affecting viral growth, oncolytic potency or tumor-selective replication of the virus. Transgenic expression of the heavy and light chains of a monoclonal antibody, as separate additional transcriptional cassettes, leads to the expression of full immunoglobulin G (IgG) monoclonal antibody by recombinant NDV. Infection of tumor cells with antibody-transgenic viruses results in the efficient production and secretion of a functional full size IgG antibody by the tumor cells, that specifically binds to its target-antigen in tumor tissue. This approach will allow to combine the advantages of oncolytic RNA viruses and monoclonal antibodies in a single powerful anticancer agent with improved or even new therapeutic properties.

摘要

用于癌症治疗临床试验的最先进的溶瘤新城疫病毒(NDV)毒株是野生型中等毒力毒株。这些病毒毒株具有固有的、未经基因工程改造的溶瘤活性,可在肿瘤细胞中选择性复制,但不在正常人类细胞中复制。迄今为止,尚未对基因工程改造的中等毒力NDV的溶瘤活性进行研究。我们在此描述了中等毒力天然溶瘤NDV毒株MTH68重组病毒的产生。我们表明,编码分子量为25和50 kDa氨基酸链的两个额外转基因不仅可以插入病毒基因组,而且不会影响病毒的生长、溶瘤效力或肿瘤选择性复制。作为单独的额外转录盒,单克隆抗体重链和轻链的转基因表达导致重组NDV表达完整的免疫球蛋白G(IgG)单克隆抗体。用抗体转基因病毒感染肿瘤细胞会导致肿瘤细胞高效产生和分泌功能性全尺寸IgG抗体,该抗体可特异性结合肿瘤组织中的靶抗原。这种方法将使溶瘤RNA病毒和单克隆抗体的优势在一种具有改进甚至新治疗特性的强大抗癌药物中结合起来。

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