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Session 91
Poster Abstracts Vaccine Trials in Human Subjects Friday, 1:30 - 3:30 pm Hall A |
Background: Studies in animals have demonstrated that immunization
with recombinant adenovirus vectors is an efficient way to elicit HIV-specific
cell mediated immune (CMI) responses.
Two prototype recombinant Ad5 vaccines expressing a human codon optimized
consensus clade B HIV-1 gag gene were tested in clinical trials.
Methods: The
first vaccine, Ad5 HIV-1 gag, was tested in a multi-center,
placebo controlled, randomized double blind trial in 160 healthy volunteers
18-50 years of age at low risk of HIV infection using a 3 dose regimen (Day 1,
Week 4, Week 26) escalating doses from 108 to 1011 viral
particles/dose (vp/dose). After the
study had been initiated, genetic instability in the vector was noted in later
passages; therefore the vector was modified to improve stability. The resulting vector, MRKAd5 HIV-1 gag, was
tested in a multi-center, placebo controlled, randomized double blind trial in
92 healthy volunteers 18-50 years of age at low risk of HIV infection using
escalating doses from 109 to 1011 vp/dose. In both studies subjects were followed for
safety and immunogenicity.
Results: Both vaccines were generally safe and well
tolerated. CMI responses, as measured by
ELISPOT, were elicited at all dose levels studied, though the vaccines were less
immunogenic in subjects with high titers (>200) of pre-existing neutralizing
antibodies to Ad5. The dose-response
relationship to immunogenicity was similar for each vaccine; therefore the data
from both vaccines are combined in the table below.
Pooled
Ad5 and MRKAd5 gag vaccine ELISPOT summaries at Wk 8 by Baseline Ad5 Titer
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Baseline Ad5 Titer |
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Dose Level (vp/d) |
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<200 |
> 200 |
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10^8 |
% Resp. |
60% |
0% |
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G. Mean (Resp.) |
276 |
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N |
15 |
7 |
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10^9 |
% Resp. |
69% |
20% |
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G. Mean (Resp.) |
213 |
187 |
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N |
32 |
15 |
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10^10 |
% Resp. |
69% |
33% |
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G. Mean (Resp.) |
263 |
309 |
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N |
36 |
24 |
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10^11 |
% Resp. |
75% |
53% |
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G. Mean (Resp.) |
286 |
168 |
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N |
44 |
17 |
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Pooled |
% Resp. |
70% |
32% |
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G. Mean (Resp.) |
259 |
218 |
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N |
127 |
63 |
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ELISPOT responder: ³ 55 SFCs/10^6 PBMCs and ³ 4-fold over media control |
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Conclusions: In these 2 studies, both adenovirus type 5 vectors
were generally safe and well tolerated and were immunogenic in humans. Pre-existing immunity to Ad5 dampens
immunogenicity.
Keywords: Vaccines; Cell mediated immunity; Adenovirus
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