RESUMO
Chikungunya virus (CHIKV) infection is one of the most challenging re-emergent diseases caused by a virus, and with no specific antiviral treatment it has now become a major public health concern. In this investigation, 25 blood samples were collected from patients with characteristic CHIKV symptoms and submitted to a virus isolation protocol, which detected 3 CHIKV isolates. These samples were evaluated by sequencing for the characterization of the strains and any homology to viruses circulating in Brazil during a recent outbreak. These viruses were used for the development of antiviral assays. Subsequently, the inhibitory effects of seaweed extracts on CHIKV replication were studied. The marine species of algae tested were Bryothamnion triquetrum, Caulerpa racemosa, Laurencia dendroidea, Osmundaria obtusiloba, Ulva fasciata, and Kappaphycus alvarezii, all of which are found in different countries including Brazil. The results revealed high levels of CHIKV inhibition, including extracts of O. obtusiloba with inhibition values of 1.25 µg/mL and a selectivity index of 420. Viral inhibition was dependent on the time of addition of extract of O. obtusiloba to the infected cells, with the optimal inhibition occurring up to 16 h after infection. Neuron evaluations with O. obtusiloba were performed and demonstrated low toxicity, and in infected neurons we observed high inhibitory activity in a dose-dependent manner. These results indicate that the algal extracts may be promising novel candidates for the development of therapeutic agents against CHIKV infections.
RESUMO
Introduction: Since its discovery in the 1980s, the human immunodeficiency virus (HIV) has been the target of many studies. Nowadays, estimates show that 36.7 million people are infected with HIV worldwide. In Brazil, HIV infection overcomes 840 thousand people. Globally, only 53% of the HIV infected people are under antiretroviral therapy. Significant advances in antiretroviral therapy have been made since the introduction of zidovudine in 1987. Objective: To advance the discoveries of the available antivirals demonstrating their functional specificities. Methods: We performed a systematic review with a bibliographic survey in the Index Medicus/MEDLINE and PubMed databases for periodical and indexed articles, from 2013 to 2018 that reported on antiretrovirals used or not in the clinical practice. Results: Currently, there are six classes of antiretroviral drugs: nucleoside reverse transcriptase inhibitors (NRTIs), non-nucleoside reverse transcriptase inhibitors (NNRTIs), protease inhibitors (PIs), fusion inhibitors (FIs), entry inhibitors (CCRIs), and HIV integrase strand transfer inhibitors (INIs or INSTIs). In summary, several antiretroviral agents under development make HIV entry, reverse transcription, integration, and maturation emerging drug become targets. Conclusion: A multifaceted approach to antiretroviral therapy, using combinations of inhibitors that target different steps of the viral life cycle, has the best potential for long-term control of HIV infection.
Introdução: Desde sua descoberta na década de 1980, o vírus da imunodeficiência humana (HIV) tem sido alvo de muitos estudos. Atualmente, as estimativas mostram que 36,7 milhões de pessoas estão infectadas pelo HIV em todo o mundo. No Brasil, a infecção pelo HIV supera 840 mil pessoas. Globalmente, apenas 53% das pessoas infectadas pelo HIV estão sob terapia antirretroviral. Avanços significativos na terapia antirretroviral (TARV) foram feitos desde a introdução da zidovudina (AZT) em 1987. Objetivo: O objetivo deste estudo foi descrever a descoberta dos antivirais disponíveis atualmente, demonstrando suas especificidades funcionais. Métodos: Foi realizada uma revisão sistemática com levantamento bibliográfico nas bases de dados Index Medicus/MEDLINE e PubMed para artigos periódicos e indexados, no período de 2013 a 2018, que relataram antirretrovirais utilizados ou não na prática clínica. Resultados: Atualmente, existem seis classes de medicamentos antirretrovirais: inibidores nucleosídeos da transcriptase reversa (NRTIs), inibidores não-nucleosídeos da transcriptase reversa (NNRTIs), inibidores da protease (IPs), inibidores de fusão (FIs), inibidores de entrada (CCRIs) e transferência da cadeia da integrase do HIV inibidores (INIs ou INSTIs). Em resumo, vários agentes antirretrovirais em desenvolvimento fazem da entrada do HIV, da transcrição reversa, da integração e da maturação, alvos dos medicamentos emergentes. Conclusão: Uma abordagem multifacetada para a TAR, usando combinações de inibidores que visam diferentes etapas do ciclo de vida viral, tem o melhor potencial para o controle da infecção pelo HIV a longo prazo.