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1 s vaccine candidates in mice and compared to DNA vaccination.
2 ce to ErbB-2 which was partially overcome by DNA vaccination.
3 ctionality to plasmids for gene delivery and DNA vaccination.
4 ral immune responses to this glycoprotein by DNA vaccination.
5 istribution of isotypes than that seen after DNA vaccination.
6 ween innate and adaptive immunity in mucosal DNA vaccination.
7 and Ag-specific immune responses elicited by DNA vaccination.
8 role in the induction of immune responses by DNA vaccination.
9 de ligands, inhibition of Th1 cytokines, and DNA vaccination.
10 lts have important clinical implications for DNA vaccination.
11 noregulatory role for CD8+ T cells following DNA vaccination.
12  cross-priming method of immune induction by DNA vaccination.
13 lethal LCMV infections is achieved following DNA vaccination.
14 ffector phase of the Th1 response after LACK DNA vaccination.
15 or generating immune responses in mice after DNA vaccination.
16 n an IL-1beta/IL-18-independent manner after DNA vaccination.
17 fic antibody and CTL responses in mice after DNA vaccination.
18 as a particularly potent adjuvant for the gD DNA vaccination.
19 rt the use of IL-6 as a cytokine adjuvant in DNA vaccination.
20 hat systemic protection was achieved by LACK DNA vaccination.
21 ion of protective immune responses following DNA vaccination.
22 e potential to tailor the immune response to DNA vaccination.
23 tion of AIDS virus-specific CTL responses by DNA vaccination.
24 n be delivered in vitro and in vivo by using DNA vaccination.
25 the potential of this strategy for enhancing DNA vaccination.
26  not be easily detectable directly after the DNA vaccination.
27 with either CD25 mAb to deplete Tregs and/or DNA vaccination.
28 fically for applications in gene therapy and DNA vaccination.
29 iral transmission when injected 5 days after DNA vaccination.
30 ll, CD4(+) T-cell, and antibody responses to DNA vaccination.
31 HIV-1 envelope (Env) glycoprotein induced by DNA vaccination.
32 ralizing antibodies, peptide antagonists and DNA vaccination.
33 anti-gp120 Abs under identical conditions of DNA vaccination.
34          Only Treg depletion followed by neu DNA vaccination abrogated tolerance to neu, resulting in
35 tramer staining of in vitro stimulated PBMC, DNA vaccinations administered to the skin with the gene
36                   Furthermore, TA99 enhances DNA vaccination against a distinct melanoma antigen, gp1
37                 In conclusion, TA99 enhances DNA vaccination against both the target antigen Tyrp1 an
38  very little data describes the potential of DNA vaccination against CDAD.
39 emory CD8(+) T-cell response generated by gB-DNA vaccination against HSV.
40 with EGFP and the first report of successful DNA vaccination against M. avium.
41                 Recent reports of successful DNA vaccination against Mycobacterium tuberculosis in sm
42                                   To improve DNA vaccination against Mycobacterium tuberculosis, we e
43 uction of anti-Tyrp1 CD8+T-cell responses to DNA vaccination against Tyrp1 as assessed by IFN-gamma E
44 from lethal HSV-2 challenge compared with gD DNA vaccination alone in both inbred and outbred mice.
45  before papilloma onset was lengthened by E6 DNA vaccination alone or to some extent by GM-CSF DNA in
46 ymphocytes compared to infiltrates following DNA vaccination alone.
47 pigs in which BCG vaccination was boosted by DNA vaccination, although this increase was not statisti
48 he immunogenicity and protective efficacy of DNA vaccination and allows for significant reduction of
49                                         When DNA vaccination and conventional ATRA therapy are combin
50 yer's patch as a promising target tissue for DNA vaccination and demonstrates the efficacy of gene gu
51  was no GVHD in HSCT recipients treated with DNA vaccination and donor leukocyte infusion.
52  on the innate immune mechanisms involved in DNA vaccination and further enrich our understanding on
53 sults support use of these growth factors in DNA vaccination and specifically indicate their applicab
54 egy combines the antigen-specific effects of DNA vaccination and the beneficial effects of local gene
55                                    After the DNA vaccinations and the first protein boost, a greater
56 ic strategies such as myoblast implantation, DNA vaccination, and gene therapy for various disease co
57 es support the importance of investigating a DNA vaccination approach for the immunologic control of
58          As a result, we turned instead to a DNA vaccination approach using a plasmid encoding the hs
59  whether cytotoxic T cell (CTL) responses to DNA vaccination are dependent upon MHC class II-restrict
60 an disease have shown that SCTs expressed by DNA vaccination are potent stimulators of cytotoxic T ly
61             This method can be combined with DNA vaccination as a novel strategy to provide both shor
62     Protective immunity is induced by CFP-10 DNA vaccination as measured by a CFU reduction in the lu
63                            Here we show that DNA vaccination at birth results in the rapid induction
64                                              DNA vaccination based immunotargeting of xCT in mice cha
65 ine MCP-1 during the early phases of plasmid DNA vaccination because injecting the type II NKT cell-a
66                                   The fourth DNA vaccination boosted the immune responses.
67                                              DNA vaccination by Biojector(R) was well-tolerated and c
68                               In conclusion, DNA vaccination by electroporation primed for TCR clonot
69 uggests that the tumor-protective effects of DNA vaccination can be largely attributed to idiotype-sp
70              These findings demonstrate that DNA vaccination can elicit protection against lentivirus
71                                              DNA vaccination can elicit the production of anti-tumor
72 mor regression induced by Treg depletion and DNA vaccination can exacerbate autoimmunity, which warra
73                                              DNA vaccination can induce both humoral and cellular imm
74 mediated immunity against malaria parasites; DNA vaccination can induce both types of effector respon
75   These results show for the first time that DNA vaccination can result in potent transmission-blocki
76                    In heavily infected mice, DNA vaccinations can switch the immune response from one
77 w that TA99 improves therapeutic efficacy of DNA vaccination combined with adoptive T-cell transfer i
78                                              DNA vaccination combined with Mycobacterium bovis bacill
79 s was more frequent and was skewed following DNA vaccination compared to that of protein immunization
80            These data not only indicate that DNA vaccination could be a successful approach to protec
81             In addition, we assessed whether DNA vaccination could retard the growth of a secondary a
82       However, unlike BCG vaccination, MPB83 DNA vaccination did not protect challenged guinea pigs f
83 tide, implying that the responses induced by DNA vaccination differ quantitatively but not qualitativ
84 he type of memory T-cell response induced by DNA vaccination does not determine the type of response
85 infection with P. berghei ANKA 6 weeks after DNA vaccination elicited comparable anti-Pbs48/45 antibo
86   As in patients with chronic HBV infection, DNA vaccination failed to generate T cells that cleared
87                       In addition, HER-2/neu DNA vaccination followed by CTL analysis further showed
88 culated with four vaccinations of DNA or two DNA vaccinations, followed by two boosts of affinity-pur
89 t study we have evaluated the feasibility of DNA vaccination for the induction of CTL reactivity to f
90 experiment, rabbit groups were treated by E6 DNA vaccination, GM-CSF DNA inoculation, or a combinatio
91                                     Although DNA vaccination has been emerged as a potential immunoth
92               In other animal model systems, DNA vaccination has been used to protect animals against
93                                              DNA vaccination has been widely studied in several model
94                                              DNA vaccination has emerged as a powerful approach in th
95               These results demonstrate that DNA vaccination has potential as a new approach for cont
96                                              DNA vaccination has proved to be a generally applicable
97  that under conditions of natural challenge, DNA vaccination has the capacity to confer complete prot
98      Tumor-bearing mice treated with KGF and DNA vaccination have improved long-term survival and dec
99 ine, moxifloxacin, and, perhaps, therapeutic DNA vaccination have the potential to improve on the cur
100 g antibody responses to WNV were elicited by DNA vaccination in humans, including in older individual
101  to generate CTL responses following plasmid DNA vaccination in mice lacking both B7-1 and B7-2 could
102 ifficult to translate promising results from DNA vaccination in mice to larger animals and humans.
103               These results demonstrate that DNA vaccination in the absence of any heterologous boost
104 ted to Tyrp1 peptide in mice receiving gp100 DNA vaccination in the presence of TA99.
105      We report here that TA99 enhances Tyrp1 DNA vaccination in the treatment of B16 lung metastases,
106 ther, we show that concurrent multiple-route DNA vaccinations induce strong cellular immunity, in add
107                                              DNA vaccination induced antibody to and T cell responses
108                                        p24CE DNA vaccination induced humoral immune responses similar
109                                              DNA vaccination-induced immune responses significantly d
110         Here, we show that a single neonatal DNA vaccination induces cellular and humoral immune resp
111  While recent studies have demonstrated that DNA vaccination induces potent CD8+ T cell memory in viv
112  we investigate whether the site and mode of DNA vaccination influences the quality of the cellular i
113                                              DNA vaccination is a novel immunization strategy that ha
114                                              DNA vaccination is a promising strategy to induce effect
115                                              DNA vaccination is a rapidly developing technology that
116                                              DNA vaccination is an attractive alternative for deliver
117                                              DNA vaccination is an effective means of eliciting both
118                                              DNA vaccination is an effective means of eliciting stron
119                              We describe how DNA vaccination is being developed for use in commercial
120 sponse to both intramuscular and intradermal DNA vaccination is highly dependent upon the generation
121    Moreover, the induction of memory CTLp by DNA vaccination is independent of MHC class II molecules
122  demonstrate that for the parameters tested, DNA vaccination is indistinguishable from live virus inf
123                  However, a major problem of DNA vaccination is its limited potency, because only a v
124                                              DNA vaccination is particularly useful for the induction
125 pparent that the immune response achieved by DNA vaccination is quite malleable, and can be manipulat
126                             Epitope-specific DNA vaccination leads to powerful antitumor attack and c
127         Interestingly, we found that plasmid DNA vaccination led to high-frequency CTL responses spec
128                                              DNA vaccination lends itself well to increasing the amou
129        In contrast to strong responses after DNA vaccination, M84-specific CD8(+)-T-cell responses we
130 that transfected muscle cells at the site of DNA vaccination may contribute to the magnitude and/or d
131                                      Because DNA vaccination may directly transfect dendritic cells,
132                                              DNA vaccination may offer a new approach to Ag-specific
133 l grade products for use in gene therapy and DNA vaccination may require >90% of the plasmid to be in
134 hanism by which CD8+ T cells induced by LACK DNA vaccination mediate both short- and long-term protec
135                      These data suggest that DNA vaccination merits further investigation as a potent
136                   These results suggest that DNA vaccination might yield improved vaccines to replace
137                      In contrast, by using a DNA vaccination model, to separate the events of vaccina
138                                      Using a DNA vaccination model, we determined that immunization w
139 ion, during the first days following plasmid DNA vaccination, NKT cells release IL-5 and MCP-1, leadi
140                                              DNA vaccination of hamsters with the HTNV M gene conferr
141                                              DNA vaccination of LMP2- and LMP7-deficient mice induced
142 d to a plasmid for Gag antigen alone (pGag), DNA vaccination of mice with pSPD-Gag-CD40L induced an i
143 oduced arenavirus neutralizing antibodies by DNA vaccination of rabbits with plasmids encoding the fu
144                                              DNA vaccination of rhesus monkeys with either the SEOV o
145 cination represents an approach for enabling DNA vaccination of the mucosa.
146 l TMEV infection to determine the effects of DNA vaccination on the course of TMEV-induced central ne
147                            T cells primed by DNA vaccination or by infection exhibited similar cytoki
148 treatment of established AHR, we developed a DNA vaccination plasmid containing OVA cDNA fused to IL-
149 elin microarrays demonstrate that tolerizing DNA vaccination plus GpG-ODN further decreased anti-myel
150 tivated cells measured directly ex vivo, the DNA vaccination primes for both CD4(+) and CD8(+) T cell
151    Finally, pulmonary, but not i.m., plasmid DNA vaccination protected mice from a lethal recombinant
152 scale, low-cost vaccine production, moreover DNA vaccination, proteomics, adjuvant design and oral va
153 rategy for safe, reproducible, and pain-free DNA vaccination remains elusive.
154                                              DNA vaccination represents a novel strategy for inducing
155 Thus, expression of IRBP in the periphery by DNA vaccination results in tolerance that acts at least
156                                              DNA vaccination showed protective and therapeutic effica
157 f DNA-encoding Flt3L and GM-CSF before MSP1a DNA vaccination significantly increased the population o
158                            Gene gun-mediated DNA vaccination stimulates an immune response characteri
159 p by DCS: In this study, we describe a novel DNA vaccination strategy to enhance uptake and presentat
160 and B-cell responses can be achieved by this DNA vaccination strategy.
161  to carbohydrate Ags, we describe results of DNA vaccination studies in mice using plasmids encoding
162 shed the protective response induced by LACK DNA vaccination, suggesting a role for CD8(+) T cells in
163                 Antiidiotypic Abs induced by DNA vaccination supported in vitro complement-mediated c
164                                              DNA vaccination that can induce both cellular and humora
165 eover, the addition of GpG-ODN to tolerizing DNA vaccination therapy effectively reduced overall mean
166 nst a second antigen beyond that afforded by DNA vaccination through CpG motifs.
167    This technology promises to be useful for DNA vaccination to elicit CD8 T cells, in vivo study of
168 unt for this may be the selective ability of DNA vaccination to induce CD8+ IFN-gamma-producing T cel
169                                    Following DNA vaccination, transfected cells secreted vaccine prot
170 ted the influence of antigen targeting after DNA vaccination upon the induction of cellular immune re
171                                              DNA vaccination using cationic polymers as carriers has
172 s and P. falciparum, and delivered by either DNA vaccination, viral vector vaccines or as protein-in-
173                         Importantly, Bla g 1 DNA vaccination was able to induce IL-10-secreting regul
174                          The insulin B-chain DNA vaccination was effective through induction of regul
175                                              DNA vaccination was employed to study immune responses t
176                                              DNA vaccination was evaluated with the experimental muri
177 nerate CTL responses following plasmid gp120 DNA vaccination was fully reconstituted by coadministeri
178 N mice showed that the immunity conferred by DNA vaccination was haplotype dependent.
179 e protective immune response induced by LACK DNA vaccination was IL-12 dependent.
180 nation of local gene delivery and tolerizing DNA vaccination, we demonstrate that codelivery of the i
181                    To explore the utility of DNA vaccination, we have constructed eukaryotic expressi
182 MV infections was conferred within 1 week of DNA vaccination, well before the peak of the CD8(+) T-ce
183 minantly IgG2a); no serological responses to DNA vaccination were observed in the absence of Salmonel
184 ytotoxic T-cell responses induced by plasmid DNA vaccination were reduced in Sting-deficient animals.
185                          Three intramuscular DNA vaccinations were delivered biweekly via in vivo ele
186 reduces regulatory T-cell populations during DNA vaccination, whereas IL-12 increases this cellular s
187 esponses of the greatest magnitude after the DNA vaccinations, while the i.d. group exhibited the res
188                   Here, we show that plasmid DNA vaccination with a cassette encoding antigen (OVA) a
189             Previously, we demonstrated that DNA vaccination with a plasmid expressing the SEOV M gen
190              We previously demonstrated that DNA vaccination with a pp89-expressing plasmid effective
191 ove on this strategy by combining xenogeneic DNA vaccination with an agonist anti-glucocorticoid-indu
192                   In this study, we employed DNA vaccination with an immunologically optimized mouse
193 Our investigators have previously shown that DNA vaccination with antigen linked to calreticulin (CRT
194 the unfavorable response of male NOD mice to DNA vaccination with InsB chain.
195                      We show here that after DNA vaccination with M84, a higher percentage of M84-spe
196                                         (ii) DNA vaccination with monomeric gp120-based antigens can
197                   These results suggest that DNA vaccination with selected CMV genes may provide a sa
198               Consistent with this activity, DNA vaccination with Sendai virus NP induced a substanti
199                                              DNA vaccination with SmCT-SOD induced a mean of 39% prot
200  multiclade consensus HIV Gag plasmid during DNA vaccination with that of IL-12.
201  We compared the protective efficacy of LACK DNA vaccination with that of recombinant LACK protein in
202                    We previously showed that DNA vaccination with the cottontail rabbit papillomaviru
203                                              DNA vaccination with the LAWD and IL-12 genes significan
204                                              DNA vaccination with the M3 gene, encoding an immune eva
205 l antibody responses were detected following DNA vaccination with the N-terminal domain of SERA, sugg
206 ave addressed the question of whether "naked DNA" vaccination with a eukaryotic expression vector (pc
207 llectively, these results show that a single DNA vaccination within hours or days of birth can induce

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