From September 2005 to March 2007, 238 individuals being vaccinated for the first time with the yellow fever (YF) -17DD vaccine were enrolled in a cohort established in Recife, Brazil. A prospective study indicated that, after immunization, anti-YF immunoglobulin M (IgM) and anti-YF IgG were present in 70.6% (IgM) and 98.3% (IgG) of the vaccinated subjects. All vaccinees developed protective immunity, which was detected by the plaque reduction neutralization test (PRNT) with a geometric mean titer of 892. Of the 238 individuals, 86.6% had IgG antibodies to dengue virus; however, the presence of anti-dengue IgG did not interfere significantly with the development of anti-YF neutralizing antibodies. In a separate retrospective study of individuals immunized with the 17DD vaccine, the PRNT values at 5 and 10 years post-vaccination remained positive but showed a significant decrease in neutralization titer (25% with PRNT titers < 100 after 5 years and 35% after 10 years).
Dengue virulence and fitness are important factors that determine disease outcome.
However, dengue virus (DENV) molecular biology and pathogenesis are not completely
elucidated. New insights on those mechanisms have been facilitated by the development
of reverse genetic systems in the past decades. Unfortunately, instability of
flavivirus genomes cloned in Escherichia coli has been a major
problem in these systems. Here, we describe the development of a complete reverse
genetics system, based on the construction of an infectious clone and replicon for a
low passage DENV-3 genotype III of a clinical isolate. Both constructs were assembled
into a newly designed yeast- E. coli shuttle vector by homologous
recombination technique and propagated in yeast to prevent any possible genome
instability in E. coli . RNA transcripts derived from the infectious
clone are infectious upon transfection into BHK-21 cells even after repeated passages
of the plasmid in yeast. Transcript-derived DENV-3 exhibited growth kinetics,
focus formation size comparable to original DENV-3 in mosquito
C6/36 cell culture. In vitro characterisation of DENV-3 replicon confirmed its
identity and ability to replicate transiently in BHK-21 cells. The reverse genetics
system reported here is a valuable tool that will facilitate further molecular
studies in DENV replication, virus attenuation and pathogenesis.
Anti-HEV antibodies were detected in animals from abattoir and in farms from northeast Brazil. Our results suggest that HEV is highly disseminated in the swine population and might present a great risk to animal handlers and for consumption of raw or undercooked meat and meat products in northeast Brazil.
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