Expression of chimeric envelope proteins in helper cell lines and integration into Moloney murine leukemia virus particles

被引:0
|
作者
Schnierle, BS [1 ]
Moritz, D [1 ]
Jeschke, M [1 ]
Groner, B [1 ]
机构
[1] INST EXPTL CANC RES, TUMOR BIOL CTR, D-79106 FREIBURG, GERMANY
关键词
recombinant retroviral structural proteins; erbB-2; erbB-3 and erbB-4 receptors; retroviral docking sites; envelope protein processing;
D O I
暂无
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
New retroviral constructs with a grafted specificity of infection could become useful gene delivery vehicles with applications in systemic gene therapy. We have constructed retroviral vectors to target gene transfer to human tumor cells. Chimeric envelope proteins have been expressed to obtain viral particles with a defined specificity of infection. Two tumor cell-specific recognition domains were cloned and fused with the viral envelope gene. A recognition domain specific for ErbB-2 expressing tumor cells was derived from a monoclonal antibody directed against the ErbB-2 receptor in the form of a single chain antibody domain (scFv-erbB-2). The receptor binding domain was derived from the heregulin gene (HRG70). This domain provides recognition specificity for ErbB-3 and ErbB-4 receptor expressing tumor cells. The recognition domains were inserted at the amino terminal end into the MoMLV envelope gene. Helper cell lines were established which express the recombinant envelope protein genes, the gag and pol genes and packageable retroviral RNA. The analysis of the helper cell line revealed that the recombinant ErbB-2 scFv-envelope protein was expressed, but not incorporated into viral particles. ThescFv-erbB-2-envelope protein was not inserted into the cell membrane and the assembly of retroviral particles was not completed. In contrast, the HRG-70-envelope protein was expressed on the surface of the helper cells and incorporated into retroviral particles. The HRG70-envelope protein, however, did not alter the host range of infection. Only cells expressing the ecotropic viral receptor could be infected.
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页码:334 / 342
页数:9
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