Recombinant adeno-associated virus vectors induce functionally impaired transgene product–specific CD8+ T cells in mice
Shih-Wen Lin, … , Marcio O. Lasaro, Hildegund C.J. Ertl
Shih-Wen Lin, … , Marcio O. Lasaro, Hildegund C.J. Ertl
Published November 15, 2007
Citation Information: J Clin Invest. 2007;117(12):3958-3970. https://doi.org/10.1172/JCI33138.
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Research Article

Recombinant adeno-associated virus vectors induce functionally impaired transgene product–specific CD8+ T cells in mice

Abstract

Recombinant adeno-associated virus (rAAV) vectors were used in human trials as carriers of vaccines for HIV-1 after encouraging preclinical results. However, the clinical trials yielded disappointing results. Here we demonstrated that in mice, rAAV vectors expressing the gene encoding HIV-1 gag stimulated gag-specific CD8+ T cells, but these T cells failed to expand after a booster immunization with a replication-defective adenoviral (Ad) vector also expressing gag. We tested rAAV vectors of different serotypes expressing HIV-1 gag for induction of transgene product–specific CD8+ T cells and found that the immunoinhibitory effect of rAAV priming observed with different AAV serotypes was transgene product specific, was independent of the interval between prime and boost, and extended to boosts with vaccine modalities other than Ad vectors. rAAV vector–induced CD8+ T cells proliferated poorly, produced low levels of IFN-γ in response to gag stimulation, and upregulated immunoinhibitory molecules. These T cells did not protect efficiently against challenge with a surrogate pathogen. Finally, we showed that the impaired proliferative capacity of the T cells was caused by persistence of the antigen-encoding rAAV vectors and could be reversed by placing the CD8+ T cells in an antigen-free environment. Our data suggest that rAAV vectors induce functionally impaired T cells and could dampen the immune response to a natural infection.

Authors

Shih-Wen Lin, Scott E. Hensley, Nia Tatsis, Marcio O. Lasaro, Hildegund C.J. Ertl

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Figure 10

Blockage of PD-1 does not rescue the proliferative capability of rAAV-induced transgene product–specific CD8+ T cells.

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Blockage of PD-1 does not rescue the proliferative capability of rAAV-in...
Groups of mice were immunized with 1011 gc rAAV2/7gag and then treated with 200 μg anti-PD-1 antibody, twice prior to boost and 3 times after boost, 3 days apart, as described previously (36, 50, 51). Control mice were treated with 200 μg IgG2a. Mice were then immunized with 1010 vp AdC68gag, and 2 and 5 weeks later, lymphocytes were harvested from blood. Shown are density plots of live cells stained with an antibody to CD8 (x axis) and the tet (y axis). Numbers within plots denote tet+CD8+ cells as a percentage of CD8+ cells.