Recombinant adeno-associated virus vectors induce functionally impaired transgene product–specific CD8+ T cells in mice
J. Clin. Invest. Shih-Wen Lin, et al. 117:3958 doi:10.1172/JCI33138 [
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Figure 7rAAV vectors increase regulatory cells, which do not cause impairment of the proliferative capacity of rAAV-induced CD8
+ T cells.
(
A and
B) BALB/c mice were immunized with 10
11 gc rAAV2/7gag and 1 month later boosted with 10
10 vp AdC68gag; control mice received rAAV2/7gag or AdC68gag. At 10 days after the boost, splenocytes were analyzed for percentage of CD4
+CD25
+FoxP3
+ cells (
A) and CD4
+CD25
+GITR
+ cells (
B). (
C) Mice immunized with 10
11 gc rAAV2/7gag were treated 3 days before the 10
10 vp AdC68gag boost with 200 μg antibody to CD25 i.p.; control mice were treated with 200 mg of control antibody. (
D) For adoptive transfer, 2 × 10
6 CD4
+, CD8
+, B220
+, or other cells were sorted from splenocytes of BALB/c mice immunized with 10
11 gc rAAV2/7gag 1 month earlier and injected through the tail vein into naive mice. Recipient mice were immunized 1 day later with 10
10 vp AdC68gag; control mice did not receive cells but did receive the 10
11 gc rAAV2/7gag prime and 10
10 vp AdC68gag boost. (
E) Serum (200 μl) from naive mice or mice receiving an immunization of 10
11 gc rAAV2/7gag was transferred i.v. into naive mice, and then 1 day later recipient mice were immunized with 10
10 vp AdC68gag vector; control mice received no serum but were immunized with 10
11 gc rAAV2/7gag followed by a 10
10 vp AdC68gag boost. At 10 days after the boost, splenocytes were analyzed by ICS. In
C–
E, frequency of gag-specific IFN-γ–secreting CD8
+ T cells is shown. Background values (less than 0.1%) were subtracted prior to plotting. Error bars represent SD for 5 mice.