The clinically approved antiviral drug sofosbuvir inhibits Zika virus replication

Carolina Q. Sacramento; Gabrielle R. de Melo; Caroline S. de Freitas; Natasha Rocha; Lucas Villas Bôas Hoelz; Milene Dias Miranda; Natalia Fintelman‐Rodrigues; Andressa Marttorelli; André C. Ferreira; Giselle Barbosa-Lima; Juliana L. Abrantes; Yasmine Rangel Vieira; Mônica M. Bastos; Eduardo de Mello Volotão; Estêvão Portela Nunes; Diogo A. Tschoeke; Luciana Leomil; Erick Correia Loiola; Pablo Trindade; Stevens K. Rehen; Fernando A. Bozza; Patrı́cia T. Bozza; Núbia Boechat; Fabiano L. Thompson; Ana María Bispo de Filippis; Karin Brüning; Thiago Moreno L. Souza

doi:10.1038/srep40920

The clinically approved antiviral drug sofosbuvir inhibits Zika virus replication

Carolina Q. Sacramento(Fundação Oswaldo Cruz), Gabrielle R. de Melo(Fundação Oswaldo Cruz), Caroline S. de Freitas(Fundação Oswaldo Cruz), Natasha Rocha(Fundação Oswaldo Cruz), Lucas Villas Bôas Hoelz(Fundação Oswaldo Cruz), Milene Dias Miranda(Universidade Federal do Rio de Janeiro), Natalia Fintelman‐Rodrigues(Fundação Oswaldo Cruz), Andressa Marttorelli(Fundação Oswaldo Cruz), André C. Ferreira(Fundação Oswaldo Cruz), Giselle Barbosa-Lima(Fundação Oswaldo Cruz), Juliana L. Abrantes(Universidade Federal do Rio de Janeiro), Yasmine Rangel Vieira(Fundação Oswaldo Cruz), Mônica M. Bastos(Fundação Oswaldo Cruz), Eduardo de Mello Volotão(Fundação Oswaldo Cruz), Estêvão Portela Nunes, Diogo A. Tschoeke(Universidade Federal do Rio de Janeiro), Luciana Leomil(Universidade Federal do Rio de Janeiro), Erick Correia Loiola(D’Or Institute for Research and Education), Pablo Trindade(D’Or Institute for Research and Education), Stevens K. Rehen(Universidade Federal do Rio de Janeiro), Fernando A. Bozza(Fundação Oswaldo Cruz), Patrı́cia T. Bozza(Fundação Oswaldo Cruz), Núbia Boechat(Fundação Oswaldo Cruz), Fabiano L. Thompson(Universidade Federal do Rio de Janeiro), Ana María Bispo de Filippis(Fundação Oswaldo Cruz), Karin Brüning(Bruning (Brazil)), Thiago Moreno L. Souza(Fundação Oswaldo Cruz)

Scientific Reports

January 18, 2017

10.1038/srep40920

Cited by 241Open Access

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Abstract

Zika virus (ZIKV) is a member of the Flaviviridae family, along with other agents of clinical significance such as dengue (DENV) and hepatitis C (HCV) viruses. Since ZIKV causes neurological disorders during fetal development and in adulthood, antiviral drugs are necessary. Sofosbuvir is clinically approved for use against HCV and targets the protein that is most conserved among the members of the Flaviviridae family, the viral RNA polymerase. Indeed, we found that sofosbuvir inhibits ZIKV RNA polymerase, targeting conserved amino acid residues. Sofosbuvir inhibited ZIKV replication in different cellular systems, such as hepatoma (Huh-7) cells, neuroblastoma (SH-Sy5y) cells, neural stem cells (NSC) and brain organoids. In addition to the direct inhibition of the viral RNA polymerase, we observed that sofosbuvir also induced an increase in A-to-G mutations in the viral genome. Together, our data highlight a potential secondary use of sofosbuvir, an anti-HCV drug, against ZIKV.

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