Antigen-specific humoral tolerance or immune augmentation induced by intramuscular delivery of adeno-associated viruses encoding CTLA4-Ig-antigen fusion molecules

被引:9
作者
Logan, G. J. [1 ]
Wang, L. [2 ]
Zheng, M. [1 ]
Ginn, S. L. [1 ]
Copper, R. L. [2 ]
Alexander, I. E. [1 ,3 ]
机构
[1] Childrens Hosp Westmead, Childrens Med Res Inst, Gene Therapy Res Unit, Wentworthville, NSW 2145, Australia
[2] Monash Univ, Dept Microbiol, Victoria Bioinformat Consortium, Clayton, Vic 3168, Australia
[3] Univ Sydney, Discipline Paediat & Child Hlth, Westmead, NSW 2145, Australia
基金
英国医学研究理事会;
关键词
adeno-associated virus; humoral tolerance; genetic vaccines; CTLA4-Ig; fusion molecules; RECOMBINANT ADENOASSOCIATED VIRUS; COAGULATION-FACTOR-IX; SEVERE COMBINED IMMUNODEFICIENCY; ERYTHROPOIETIN GENE-THERAPY; IG-FUSION PROTEINS; DENDRITIC CELLS; HEMOPHILIA-B; AUTOIMMUNE-DISEASES; SKELETAL-MUSCLE; BINDING DOMAIN;
D O I
10.1038/gt.2008.168
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
This study initially sought to investigate the immunostimulatory properties of recombinant adeno-associated virus (rAAV) with a view to developing a genetic vaccine for malaria using muscle as a target tissue. To augment humoral immunity, the AAV-encoded antigen was genetically fused with CTLA4-Ig, a recombinant molecule that binds B7 costimulatory molecules. At 10(9) vg, CTLA4-Ig fusion promoted the humoral immune response 100-fold and was dependent on CTLA4-Ig binding with B7 costimulatory molecules, confirming plasmid DNA models using this strategy. In distinct contrast, 10(12)-10(13) vg of rAAV1 specifically induced long-lived humoral tolerance through a mechanism that is independent of CTLA4-Ig binding with B7. This finding was unexpected, as rAAV delivery to muscle, unlike liver, has shown that this tissue provides a highly immunogenic environment for induction of humoral immunity against rAAV transgene products. An additional unpredicted consequence of antigen fusion with CTLA4-Ig was the enhancement of antigen expression by approximately one log, an effect mapped to the hinge and Fc domain of IgG(1), but not involving antigen dimerization or the neonatal Fc receptor. Collectively, these findings significantly advance the potential of rAAV both as a vaccine or immunotherapeutic platform for the induction of antigen-specific humoral immunity or tolerance and as a gene therapeutic delivery system.
引用
收藏
页码:200 / 210
页数:11
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