In-depth characterization of congenital Zika syndrome in immunocompetent mice: Antibody-dependent enhancement and an antiviral peptide therapy

Vidyleison N. Camargos; Giselle Foureaux; Daniel C. Medeiros; Vivian T. da Silveira; Celso M. Queiroz-Junior; Ana Luisa B. Matosinhos; André F.A. Figueiredo; Carla D.F. Sousa; Thaiane P. Moreira; Victória F. Queiroz; Ana Carolina F. Dias; Karina T.O. Santana; Ingredy Passos; Ana Luíza C.V. Real; Ludmila C. Silva; Flávio A.G. Mourão; Natália T. Wnuk; Milton A.P. Oliveira; Soraia Macari; Tarcília Silva; Gustavo P. Garlet; Joshua A. Jackman; Frederico M. Soriani; Márcio F.D. Moraes; Eduardo M.A.M. Mendes; Fabíola M. Ribeiro; Guilherme M.J. Costa; Antônio L. Teixeira; Nam Joon Cho; Antônio C.P. Oliveira; Mauro M. Teixeira; Vivian V. Costa; Danielle G. Souza

doi:10.1016/j.ebiom.2019.05.014

In-depth characterization of congenital Zika syndrome in immunocompetent mice: Antibody-dependent enhancement and an antiviral peptide therapy

Vidyleison N. Camargos, Giselle Foureaux, Daniel C. Medeiros, Vivian T. da Silveira, Celso M. Queiroz-Junior, Ana Luisa B. Matosinhos, André F.A. Figueiredo, Carla D.F. Sousa, Thaiane P. Moreira, Victória F. Queiroz, Ana Carolina F. Dias, Karina T.O. Santana, Ingredy Passos, Ana Luíza C.V. Real, Ludmila C. Silva, Flávio A.G. Mourão, Natália T. Wnuk, Milton A.P. Oliveira, Soraia Macari, Tarcília SilvaGustavo P. Garlet, Joshua A. Jackman, Frederico M. Soriani, Márcio F.D. Moraes, Eduardo M.A.M. Mendes, Fabíola M. Ribeiro, Guilherme M.J. Costa, Antônio L. Teixeira, Nam Joon Cho, Antônio C.P. Oliveira, Mauro M. Teixeira, Vivian V. Costa, Danielle G. Souza

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34 Citas (Scopus)

Resumen

Background: Zika virus (ZIKV) infection during pregnancy may cause major congenital defects, including microcephaly, ocular, articular and muscle abnormalities, which are collectively defined as Congenital Zika Syndrome. Here, we performed an in-depth characterization of the effects of congenital ZIKV infection (CZI) in immunocompetent mice. Methods: Pregnant dams were inoculated with ZIKV on embryonic day 5.5 in the presence or absence of a sub-neutralizing dose of a pan-flavivirus monoclonal antibody (4G2) to evaluate the potential role of antibody-dependent enhancement phenomenon (ADE) during short and long outcomes of CZI. Findings: ZIKV infection induced maternal immune activation (MIA), which was associated with occurrence of foetal abnormalities and death. Therapeutic administration of AH-D antiviral peptide during the early stages of pregnancy prevented ZIKV replication and death of offspring. In the post-natal period, CZI was associated with a decrease in whole brain volume, ophthalmologic abnormalities, changes in testicular morphology, and disruption in bone microarchitecture. Some alterations were enhanced in the presence of 4G2 antibody. Interpretation: Our results reveal that early maternal ZIKV infection causes several birth defects in immunocompetent mice, which can be potentiated by ADE phenomenon and are associated with MIA. Additionally, antiviral treatment with AH-D peptide may be beneficial during early maternal ZIKV infection. Fund: This work was supported by the Brazilian National Science Council (CNPq, Brazil), Minas Gerais Foundation for Science (FAPEMIG), Funding Authority for Studies and Projects (FINEP), Coordination of Superior Level Staff Improvement (CAPES), National Research Foundation of Singapore and Centre for Precision Biology at Nanyang Technological University.

Idioma original	English (US)
Páginas (desde-hasta)	516-529
Número de páginas	14
Publicación	EBioMedicine
Volumen	44
DOI	https://doi.org/10.1016/j.ebiom.2019.05.014
Estado	Published - jun 2019
Publicado de forma externa	Sí

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

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10.1016/j.ebiom.2019.05.014

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Camargos, V. N., Foureaux, G., Medeiros, D. C., da Silveira, V. T., Queiroz-Junior, C. M., Matosinhos, A. L. B., Figueiredo, A. F. A., Sousa, C. D. F., Moreira, T. P., Queiroz, V. F., Dias, A. C. F., Santana, K. T. O., Passos, I., Real, A. L. C. V., Silva, L. C., Mourão, F. A. G., Wnuk, N. T., Oliveira, M. A. P., Macari, S., ... Souza, D. G. (2019). In-depth characterization of congenital Zika syndrome in immunocompetent mice: Antibody-dependent enhancement and an antiviral peptide therapy. EBioMedicine, 44, 516-529. https://doi.org/10.1016/j.ebiom.2019.05.014

Camargos, VN, Foureaux, G, Medeiros, DC, da Silveira, VT, Queiroz-Junior, CM, Matosinhos, ALB, Figueiredo, AFA, Sousa, CDF, Moreira, TP, Queiroz, VF, Dias, ACF, Santana, KTO, Passos, I, Real, ALCV, Silva, LC, Mourão, FAG, Wnuk, NT, Oliveira, MAP, Macari, S, Silva, T, Garlet, GP, Jackman, JA, Soriani, FM, Moraes, MFD, Mendes, EMAM, Ribeiro, FM, Costa, GMJ, Teixeira, AL, Cho, NJ, Oliveira, ACP, Teixeira, MM, Costa, VV & Souza, DG 2019, 'In-depth characterization of congenital Zika syndrome in immunocompetent mice: Antibody-dependent enhancement and an antiviral peptide therapy', EBioMedicine, vol. 44, pp. 516-529. https://doi.org/10.1016/j.ebiom.2019.05.014

@article{cb8f715c35264c768467f6a092147de4,

title = "In-depth characterization of congenital Zika syndrome in immunocompetent mice: Antibody-dependent enhancement and an antiviral peptide therapy",

abstract = "Background: Zika virus (ZIKV) infection during pregnancy may cause major congenital defects, including microcephaly, ocular, articular and muscle abnormalities, which are collectively defined as Congenital Zika Syndrome. Here, we performed an in-depth characterization of the effects of congenital ZIKV infection (CZI) in immunocompetent mice. Methods: Pregnant dams were inoculated with ZIKV on embryonic day 5.5 in the presence or absence of a sub-neutralizing dose of a pan-flavivirus monoclonal antibody (4G2) to evaluate the potential role of antibody-dependent enhancement phenomenon (ADE) during short and long outcomes of CZI. Findings: ZIKV infection induced maternal immune activation (MIA), which was associated with occurrence of foetal abnormalities and death. Therapeutic administration of AH-D antiviral peptide during the early stages of pregnancy prevented ZIKV replication and death of offspring. In the post-natal period, CZI was associated with a decrease in whole brain volume, ophthalmologic abnormalities, changes in testicular morphology, and disruption in bone microarchitecture. Some alterations were enhanced in the presence of 4G2 antibody. Interpretation: Our results reveal that early maternal ZIKV infection causes several birth defects in immunocompetent mice, which can be potentiated by ADE phenomenon and are associated with MIA. Additionally, antiviral treatment with AH-D peptide may be beneficial during early maternal ZIKV infection. Fund: This work was supported by the Brazilian National Science Council (CNPq, Brazil), Minas Gerais Foundation for Science (FAPEMIG), Funding Authority for Studies and Projects (FINEP), Coordination of Superior Level Staff Improvement (CAPES), National Research Foundation of Singapore and Centre for Precision Biology at Nanyang Technological University.",

keywords = "Antibody-dependent enhancement (ADE), Congenital Zika Syndrome (CZS), Congenital Zika virus infection (CZI), Maternal immune activation (MIA), Short and long-term outcomes",

author = "Camargos, {Vidyleison N.} and Giselle Foureaux and Medeiros, {Daniel C.} and {da Silveira}, {Vivian T.} and Queiroz-Junior, {Celso M.} and Matosinhos, {Ana Luisa B.} and Figueiredo, {Andr{\'e} F.A.} and Sousa, {Carla D.F.} and Moreira, {Thaiane P.} and Queiroz, {Vict{\'o}ria F.} and Dias, {Ana Carolina F.} and Santana, {Karina T.O.} and Ingredy Passos and Real, {Ana Lu{\'i}za C.V.} and Silva, {Ludmila C.} and Mour{\~a}o, {Fl{\'a}vio A.G.} and Wnuk, {Nat{\'a}lia T.} and Oliveira, {Milton A.P.} and Soraia Macari and Tarc{\'i}lia Silva and Garlet, {Gustavo P.} and Jackman, {Joshua A.} and Soriani, {Frederico M.} and Moraes, {M{\'a}rcio F.D.} and Mendes, {Eduardo M.A.M.} and Ribeiro, {Fab{\'i}ola M.} and Costa, {Guilherme M.J.} and Teixeira, {Ant{\^o}nio L.} and Cho, {Nam Joon} and Oliveira, {Ant{\^o}nio C.P.} and Teixeira, {Mauro M.} and Costa, {Vivian V.} and Souza, {Danielle G.}",

note = "Publisher Copyright: {\textcopyright} 2019",

year = "2019",

month = jun,

doi = "10.1016/j.ebiom.2019.05.014",

language = "English (US)",

volume = "44",

pages = "516--529",

journal = "EBioMedicine",

issn = "2352-3964",

publisher = "Elsevier B.V.",

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TY - JOUR

T1 - In-depth characterization of congenital Zika syndrome in immunocompetent mice

T2 - Antibody-dependent enhancement and an antiviral peptide therapy

AU - Camargos, Vidyleison N.

AU - Foureaux, Giselle

AU - Medeiros, Daniel C.

AU - da Silveira, Vivian T.

AU - Queiroz-Junior, Celso M.

AU - Matosinhos, Ana Luisa B.

AU - Figueiredo, André F.A.

AU - Sousa, Carla D.F.

AU - Moreira, Thaiane P.

AU - Queiroz, Victória F.

AU - Dias, Ana Carolina F.

AU - Santana, Karina T.O.

AU - Passos, Ingredy

AU - Real, Ana Luíza C.V.

AU - Silva, Ludmila C.

AU - Mourão, Flávio A.G.

AU - Wnuk, Natália T.

AU - Oliveira, Milton A.P.

AU - Macari, Soraia

AU - Silva, Tarcília

AU - Garlet, Gustavo P.

AU - Jackman, Joshua A.

AU - Soriani, Frederico M.

AU - Moraes, Márcio F.D.

AU - Mendes, Eduardo M.A.M.

AU - Ribeiro, Fabíola M.

AU - Costa, Guilherme M.J.

AU - Teixeira, Antônio L.

AU - Cho, Nam Joon

AU - Oliveira, Antônio C.P.

AU - Teixeira, Mauro M.

AU - Costa, Vivian V.

AU - Souza, Danielle G.

PY - 2019/6

Y1 - 2019/6

N2 - Background: Zika virus (ZIKV) infection during pregnancy may cause major congenital defects, including microcephaly, ocular, articular and muscle abnormalities, which are collectively defined as Congenital Zika Syndrome. Here, we performed an in-depth characterization of the effects of congenital ZIKV infection (CZI) in immunocompetent mice. Methods: Pregnant dams were inoculated with ZIKV on embryonic day 5.5 in the presence or absence of a sub-neutralizing dose of a pan-flavivirus monoclonal antibody (4G2) to evaluate the potential role of antibody-dependent enhancement phenomenon (ADE) during short and long outcomes of CZI. Findings: ZIKV infection induced maternal immune activation (MIA), which was associated with occurrence of foetal abnormalities and death. Therapeutic administration of AH-D antiviral peptide during the early stages of pregnancy prevented ZIKV replication and death of offspring. In the post-natal period, CZI was associated with a decrease in whole brain volume, ophthalmologic abnormalities, changes in testicular morphology, and disruption in bone microarchitecture. Some alterations were enhanced in the presence of 4G2 antibody. Interpretation: Our results reveal that early maternal ZIKV infection causes several birth defects in immunocompetent mice, which can be potentiated by ADE phenomenon and are associated with MIA. Additionally, antiviral treatment with AH-D peptide may be beneficial during early maternal ZIKV infection. Fund: This work was supported by the Brazilian National Science Council (CNPq, Brazil), Minas Gerais Foundation for Science (FAPEMIG), Funding Authority for Studies and Projects (FINEP), Coordination of Superior Level Staff Improvement (CAPES), National Research Foundation of Singapore and Centre for Precision Biology at Nanyang Technological University.

AB - Background: Zika virus (ZIKV) infection during pregnancy may cause major congenital defects, including microcephaly, ocular, articular and muscle abnormalities, which are collectively defined as Congenital Zika Syndrome. Here, we performed an in-depth characterization of the effects of congenital ZIKV infection (CZI) in immunocompetent mice. Methods: Pregnant dams were inoculated with ZIKV on embryonic day 5.5 in the presence or absence of a sub-neutralizing dose of a pan-flavivirus monoclonal antibody (4G2) to evaluate the potential role of antibody-dependent enhancement phenomenon (ADE) during short and long outcomes of CZI. Findings: ZIKV infection induced maternal immune activation (MIA), which was associated with occurrence of foetal abnormalities and death. Therapeutic administration of AH-D antiviral peptide during the early stages of pregnancy prevented ZIKV replication and death of offspring. In the post-natal period, CZI was associated with a decrease in whole brain volume, ophthalmologic abnormalities, changes in testicular morphology, and disruption in bone microarchitecture. Some alterations were enhanced in the presence of 4G2 antibody. Interpretation: Our results reveal that early maternal ZIKV infection causes several birth defects in immunocompetent mice, which can be potentiated by ADE phenomenon and are associated with MIA. Additionally, antiviral treatment with AH-D peptide may be beneficial during early maternal ZIKV infection. Fund: This work was supported by the Brazilian National Science Council (CNPq, Brazil), Minas Gerais Foundation for Science (FAPEMIG), Funding Authority for Studies and Projects (FINEP), Coordination of Superior Level Staff Improvement (CAPES), National Research Foundation of Singapore and Centre for Precision Biology at Nanyang Technological University.

KW - Antibody-dependent enhancement (ADE)

KW - Congenital Zika Syndrome (CZS)

KW - Congenital Zika virus infection (CZI)

KW - Maternal immune activation (MIA)

KW - Short and long-term outcomes

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UR - http://www.scopus.com/inward/citedby.url?scp=85065903019&partnerID=8YFLogxK

U2 - 10.1016/j.ebiom.2019.05.014

DO - 10.1016/j.ebiom.2019.05.014

M3 - Article

C2 - 31130472

AN - SCOPUS:85065903019

SN - 2352-3964

VL - 44

SP - 516

EP - 529

JO - EBioMedicine

JF - EBioMedicine

ER -

In-depth characterization of congenital Zika syndrome in immunocompetent mice: Antibody-dependent enhancement and an antiviral peptide therapy

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