Hepatites Virais Frequência do antígeno de superfície da hepatite viral tipo B nos portadores do HIV e grávidas atendidos no Laboratório Elisa-Blot do Hospital Agostinho Neto Praia em 2006 e 2007

Com a finalidade de fazer uma avaliação da frequência do antígeno de superfície da hepatite viral do tipo B (AgHBs) nos portadores HIV e grávidas atendidos no Laboratório Elisa-Blot do Hospital Agostinho Neto em 2006 e 2007, foi feito um estudo descritivo retrospectivo, com base na recolha de dados entre 1 de Janeiro de 2006 a 31 de Dezembro de 2007. Os dados foram recolhidos com base em fichas e no banco de dados informático, existentes no Laboratório Elisa-Blot do Hospital Agostinho Neto. Os dados foram colectados segundo as variáveis de tempo, pessoa e lugar. Os resultados demonstraram uma frequência do AgHBs durante o período de estudo de 4,96% (25/504). Esse valor corresponde a 11% (15/135) dos portadores do HIV e 3% em grávidas com sorologia positiva para HBsAg. Em relação ao perfil dos portadores do HIV, estes tinham uma idade média de 40,6 anos, a maioria do sexo feminino e residentes no concelho da Praia. As grávidas tinham uma idade média de 28,4 anos, a maioria residente também no concelho da Praia. As análises também demonstraram que o perfil dos casos com sorologia positiva para o AgHBs nos portadores do HIV era na sua maioria do sexo masculino com uma proporção de 60% durante o período de estudo. A maior ocorrência ocorreu na faixa etária 30 a 49 anos com uma proporção de 67% e 50% relativamente ao período de estudo. O concelho da Praia foi o que apresentou maior proporção com 67% e 58% em 2006 e 2007 respectivamente. Em relação as grávidas a maior proporção de positividade do AgHBs ocorreu também na faixa etária 30 a 49 anos com 75% e 67% e no concelho da Praia com uma proporção de 50% e 67% referentes aos anos 2006 e 2007 respectivamente.

Molecular epidemiology and evolution of HIV-1 in Portugal and portuguese speaking african countries

The aims of this thesis were to better characterize HIV-1 diversity in Portugal, Angola, Mozambique and Cape Verde and to investigate the origin and epidemiological history of HIV-1 in these countries. The impact of these issues in diagnosis, disease progression and susceptibility to ARV therapy was also investigated. Finally, the nature, dynamics and prevalence of transmitted drug resistance (TDR) was determined in untreated HIV-1 infected patients. In Angola, practically all HIV-1 genetic forms were found, including almost all subtypes, untypable (U) strains, CRFs and URFs. Recombinants (first and second generation) were present in 47.1% of the patients. HIV/AIDS epidemic in Angola probably started in 1961, the major cause being the independence war, subsequently spreading to Portugal. In Maputo, 81% of the patients were infected with subtype C viruses. Subtype G, U and recombinants such as CRF37_cpx, were also present. The results suggest that HIV-1 epidemic in Mozambique is evolving rapidly in genetic complexity. In Cape Verde, where HIV-1 and HIV-2 co-circulate, subtype G is the prevailed subtype. Subtypes B, C, F1, U, CRF02_AG and other recombinant strains were also found. HIV-2 isolates belonged to group A, some being closely related to the original ROD isolate. In all three countries numerous new polymorphisms were identified in the RT and PR of HIV-1 viruses. Mutations conferring resistance to the NRTIs or NNRTIs were found in isolates from 2 (2%) patients from Angola, 4 (6%) from Mozambique and 3 (12%) from Cape Verde. None of the isolates containing TDR mutations would be fully sensitive to the standard first-line therapeutic regimens used in these countries. Close surveillance in treated and untreated populations will be crucial to prevent further transmission of drug resistant strains and maximize the efficacy of ARV therapy. In Portugal, investigation of a seronegative case infection with rapid progression to AIDS and death revealed that the patient was infected with a CRF14_BG-like R5-tropic strain selectively transmitted by his seropositive sexual partner. The results suggest a massive infection with a highly aggressive CRF14_BG like strain and/or the presence of an unidentified immunological problem that prevented the formation of HIV-1-specific antibodies. Near full-length genomic sequences obtained from three unrelated patients enabled the first molecular and phylogenomic characterization of CRF14_BG from Portugal; all sequences were strongly related with CRF14_BG Spanish isolates. The mean date of origin of CRF14_BG was estimated to be 1992. We propose that CRF14_BG emerged in Portugal in the early 1990s, spread to Spain in late 1990s as a consequence of IDUs migration and then to the rest of Europe. Most CRF14_BG strains were predicted to use CXCR4 and were associated with rapid CD4 depletion and disease progression. Finally, we provide evidence suggesting that the X4 tropism of CRF14_BG may have resulted from convergent evolution of the V3 loop possibly driven by an effective escape from neutralizing antibody response.