In the present work, we evaluated the neutralizing capacity of the antibodies induced by dengue virus type 1 and 2 envelope domain III recombinant proteins in monkeys against strains of different dengue virus type 1 and 2 genotypes. Here we demonstrated that dengue virus type 1 and 2 recombinant proteins induced high titers of neutralizing antibodies against different genotype strains.An effective humoral immune response is critical for protecting against dengue viruses (DEN) (12)(13)(14) and is the essential goal of recombinant subunit vaccines based on envelope (E) domain III. Domain III is thought to mediate interactions between the virus and cellular receptors involved in virus attachment (6,21). In addition, many of the most potent anti-DEN neutralizing monoclonal antibodies characterized to date recognize this domain (8, 9,24).There is some evidence that the antibody response to a DEN genotype does not necessarily neutralize homogenotypic DEN strains. In fact, sera from patients infected with DEN type 2 (DEN 2) or DEN 3 show variations in the neutralizing antibody responses against strains isolated early and late during the same epidemic (1, 26). Preclinical studies have exposed that the primary immune responses induced after infection of mice and monkeys with DEN 2 strains belonging to both Asian and American genotypes show differences in the responses of neutralizing antibodies against the same and different strains of infection (4, 5). Based on monoclonal antibody data, changes of specific amino acids in domain III result in the loss of binding of neutralizing monoclonal antibodies (11,19,24). A recent study has also demonstrated that monoclonal antibodies show differentiated neutralizing activities depending on the virulence of the strain (7). Based on the previously reported evidence (1, 4, 5, 7, 11,19,24,26), the humoral immune response induced by a vaccine candidate should be evaluated against strains of different genotypes of each serotype.Previously, we have reported that recombinant proteins containing domain III of DEN 1 or DEN 2 E proteins fused to the P64k protein from Neisseria meningitidis (PD10 and PD5, respectively) induce neutralizing antibodies and partial protection in immunized monkeys (3, 10). In the context of P64k, amino acid changes in E domain III included in the fusion protein have been involved in the antigenicity and immunogenicity of the resultant molecules in the mouse model (28). In the present work, we evaluate the neutralizing antibody activity in sera collected from Macaca fascicularis monkeys immunized with such recombinant proteins against strains of different genotypes.Sera from Macaca fascicularis monkeys previously immunized with DEN 1 or DEN 2 recombinant fusion proteins were evaluated by a plaque reduction neutralization test (PRNT) against DEN 1 or DEN 2 strains belonging to different genotypes of the corresponding serotype (Table 1) (17,23). The E domain III used for the PD10 or PD5 genetic construction belongs to strain DEN 1 Jamaica or DEN 2 Jamaica, respective...
