Rotavirus genotypes and the indigenous children of Brazilian midwest in the vaccine era, 2008-2012: footprints of animal genome

World group A rotavirus (RVA) surveillance data provides useful estimates of the disease burden, however, indigenous population might require special consideration. The aim of this study was to describe the results of G­ and P­types from Brazilian native children ≤3 years. Furthermore, selected strains have been analyzed for the VP7, VP6, VP4, and NSP4 encoding genes in order to gain insight into genetic variability of Brazilian strains. A total of 149 samples, collected during 2008­2012, were tested for RVA using ELISA and PAGE, following by RT­PCR and sequencing. RVA infection was detected in 8.7% of samples (13/149). Genotype G2P[4] was detected in 2008 and 2010, G8P[6] in 2009, and G3P[8] in 2011. The phylogenetic analysis of the VP7 and VP4 genes grouped the Brazilian G2P[4] and G3P[8] strains within the lineages currently circulating in humans worldwide. However, the phylogenetic analysis of the VP6 and NSP4 from the Brazilian G2P[4] strains, and the VP7 and NSP4 from the Brazilian G3P[8] strains suggest a distant common ancestor with different animal strains (bovine, caprine, and porcine). The epidemiological and genetic information obtained in the present study is expected to provide an updated understanding of RVA genotypes circulating in the native infant population, and to formulate policies for the use of RVA vaccines in indigenous Brazilian people. Moreover, these results highlight the great diversity of human RVA strains circulating in Brazil, and an in­depth surveillance of human and animal RVA will lead to a better understanding of the complex dynamics of RVA evolution

[Vaccine potential of rotavirus outer capsid protein [VP4] cloned into the plasmid]

Rotaviruses are associated with endemic diarrhea in children under the age of 5, leading to approximately 800,000 deaths every year. Introduction of rotavirus vaccines into childhood immunization programs can contribute to substantial reduction in mortality from rotavirus gastroenteritis in developing countries. VP4 is outer capsid spike protein of rotavirus by which virus can bind to its receptor. VP4 protein can induce production of neutralizing antibodies. Regarding these concepts we cloned VP4 gene of rotavirus in plasmid vector for future expression. BSC-1 cells were cultured as a monolayer. Rotavirus CPE positive cell cultures were freeze-thawed three times. Rotavirus was partially purified by ultracentrifuge. Oligonucleotide primers, specific for gene segment 4 which encodes VP4, were synthesized. Rotavirus RNA extracted and used as a template for synthesis of cDNA by reverse transcriptase. Then they proliferated by PCR and PCR products were cloned into plasmid vector which was analyzed by restriction enzymes and sequencing. Sequencing result was analyzed with BLAST software that had a 100% homology with SA11 rotavirus genome segment 4 in NCBI Gene Bank. Sequencing result confirms highly that the nucleotide sequences of VP4 gene after long and continuous passage of SA11 rotavirus is conserved in our laboratory

Prevalence of antibodies to dengue virus, hepadnavirus and rotavirus in non-human primates

The aim of this study was to determine the prevalence of several viral antibodies in non-human primates from two zoological gardens from Venezuela. Only two out of 66 sera were positive for antibodies to dengue virus by hemagglutination inhibition. Six out of 62 sera exhibited antibodies against Hepatitis B virus (HBV) core antigen. Viral DNA was detected by nested PCR in one positive serum and in three negative without serological evidence of HBV infection. Sequence analysis showed the circulation of HBV genotype F, predominant in Venezuela. Antibodies against rotavirus antigens were found in 87 percent (20/23) of Old World primates and in 50 percent (13/26) of New World primates. Both the prevalence of antibodies and the mean O.D. value by ELISA were significantly lower in New World primate sera. These results suggest that non-human primates do not seem to represent an important reservoir for dengue virus infection, highly endemic in Venezuela. Anthropozoonotic infection of HBV seems to occur among primates not only from the Old but also from the New World, reinforcing the importance of vaccination of species at risk. This study also suggests a lower frequency of infection by rotavirus of non-human primates from the New World, compared to primates from the Old World.

En este estudio se determinó la prevalencia de anticuerpos contra varios virus en primates no humanos de dos parques zoológicos de Venezuela. Sólo dos de 66 sueros fueron positivos, por inhibición de la hemaglutinación, para anticuerpos contra virus dengue. Seis de 62 sueros presentaron anticuerpos contra la cápside del virus de la hepatitis B virus (VHB). Se detectó el ADN viral, mediante PCR en dos rondas, en uno de éstos y en tres sueros sin evidencia serológica de infección por VHB. El análisis de la secuencia mostró la circulación del VHB genotipo F, predominante en Venezuela. Un 87 por ciento (20/23) de los sueros de primates del Viejo Mundo y un 50 (13/26) de los del Nuevo Mundo mostraron anticuerpos contra antígenos de rotavirus. Tanto la prevalencia de anticuerpos como los valores promedio de D.O. por ELISA fueron significativamente menores en sueros de primates del Nuevo Mundo. Los primates no humanos no parecen jugar un papel importante como reservorio de la infección por virus dengue, altamente prevalente en el país. La infección por cepas humanas del VHB en primates sugiere infección antroponótica y la importancia de vacunar las especies a riesgo. Los resultados sugieren igualmente una menor frecuencia de infección por rotavirus en primates del Nuevo Mundo.