Zika virus (ZIKV) emerged on a global scale and no licensed vaccine ensures long-lasting anti-ZIKV immunity. Here we report the design and comparative evaluation of four replication-deficient chimpanzee adenoviral (ChAdOx1) ZIKV vaccine candidates comprising the addition or deletion of precursor membrane (prM) and envelope, with or without its transmembrane domain (TM). A single, non-adjuvanted vaccination of ChAdOx1 ZIKV vaccines elicits suitable levels of protective responses in mice challenged with ZIKV. ChAdOx1 prME ∆TM encoding prM and envelope without TM provides 100% protection, as well as long-lasting anti-envelope immune responses and no evidence of in vitro antibody-dependent enhancement to dengue virus. Deletion of prM and addition of TM reduces protective efficacy and yields lower anti-envelope responses. Our finding that immunity against ZIKV can be enhanced by modulating antigen membrane anchoring highlights important parameters in the design of viral vectored ZIKV vaccines to support further clinical assessments

Abbink, Peter

Badamchi-Zadeh, Alex

Barouch, Dan H.

Boyd, Michael

Coelho, Danilo F.

De Lorenzo, Giuditta

Dejnirattisai, Wanwisa

Doig, Jennifer

Donald, Claire L.

Dorrell, Lucy

Gilbert, Sarah C.

Hill, Adrian V. S.

Kim, Young Chan

Kohl, Alain

Larocca, Rafael A.

López-Camacho, César

Mongkolsapaya, Juthathip

Neto, Roberto Dias Lins

Owsianka, Ania

Patel, Arvind H.

Reyes-Sandoval, Arturo

Screaton, Gavin R.

Velazquez, Ricardo Sanchez

Wallace, Zoë R.

Nature Communications

AbstractZika virus (ZIKV) emerged on a global scale and no licensed vaccine ensures long-lasting anti-ZIKV immunity. Here we report the design and comparative evaluation of four replication-deficient chimpanzee adenoviral (ChAdOx1) ZIKV vaccine candidates comprising the addition or deletion of precursor membrane (prM) and envelope, with or without its transmembrane domain (TM). A single, non-adjuvanted vaccination of ChAdOx1 ZIKV vaccines elicits suitable levels of protective responses in mice challenged with ZIKV. ChAdOx1 prME ∆TM encoding prM and envelope without TM provides 100% protection, as well as long-lasting anti-envelope immune responses and no evidence of in vitro antibody-dependent enhancement to dengue virus. Deletion of prM and addition of TM reduces protective efficacy and yields lower anti-envelope responses. Our finding that immunity against ZIKV can be enhanced by modulating antigen membrane anchoring highlights important parameters in the design of viral vectored ZIKV vaccines to support further clinical assessments.</jats:p

César López-Camacho

Peter Abbink

Rafael A. Larocca

Wanwisa Dejnirattisai

Michael Boyd

Alex Badamchi-Zadeh

Zoë R. Wallace

Jennifer Doig

Ricardo Sanchez Velazquez

Roberto Dias Lins Neto

Danilo F. Coelho

Young Chan Kim

Claire L. Donald

Ania Owsianka

Giuditta De Lorenzo

Alain Kohl

Sarah C. Gilbert

Lucy Dorrell

Juthathip Mongkolsapaya

Arvind H. Patel

Gavin R. Screaton

Dan H. Barouch

Adrian V. S. Hill

Arturo Reyes-Sandoval

Crossref

Rational Zika vaccine design via the modulation of antigen membrane anchors in chimpanzee adenoviral vectors

1The Jenner Institute, Nuffield Department of Medicine, University of Oxford, The Henry Wellcome Building for Molecular Physiology, Roosevelt Drive, Oxford, OX3 7BN UK
2Center for Virology and Vaccine Research, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA 02215 USA
3Division of Immunology and Inflammation, Department of Medicine, Hammersmith Campus, Imperial College London, London, W12 0NN UK
4Nuffield Department of Medicine and Oxford NIHR Biomedical Research Centre, University of Oxford, Oxford, OX3 7FZ UK
5MRC-University of Glasgow Centre for Virus Research, University of Glasgow, Glasgow,, G61 1QH Scotland UK
6Aggeu Magalhães Institute, Oswaldo Cruz Foundation, 50670-465 Recife, Brazil
7The Jenner Institute, Nuffield Department of Medicine, University of Oxford, Old Road Campus Research Building, Roosevelt Drive, Oxford, OX3 7DQ UK
8Dengue Hemorrhagic Fever Research Unit, Office for Research and Development, Faculty of Medicine Siriraj Hospital, Mahidol University, Bangkok, 10700 Thailand
9Division of Medical Sciences, John Radcliffe Hospital, University of Oxford, Oxford, OX3 9DU UKConselho de Pesquisa Médica do Reino Unido [MC_UU_12014 (AHP e AK ) e MR / N017552 / 1 (AK)]. Juthathip Mongkolsapaya é apoiado por uma bolsa do Fundo MRC-Newton, Gavin Screaton é um investigador sênior da Wellcome Trust.Múltipla - ver em NotasZika virus (ZIKV) emerged on a global scale and no licensed vaccine ensures long-lasting anti-ZIKV immunity. Here we report the design and comparative evaluation of four replication-deficient chimpanzee adenoviral (ChAdOx1) ZIKV vaccine candidates comprising the addition or deletion of precursor membrane (prM) and envelope, with or without its transmembrane domain (TM). A single, non-adjuvanted vaccination of ChAdOx1 ZIKV vaccines elicits suitable levels of protective responses in mice challenged with ZIKV. ChAdOx1 prME ∆TM encoding prM and envelope without TM provides 100% protection, as well as long-lasting anti-envelope immune responses and no evidence of in vitro antibody-dependent enhancement to dengue virus. Deletion of prM and addition of TM reduces protective efficacy and yields lower anti-envelope responses. Our finding that immunity against ZIKV can be enhanced by modulating antigen membrane anchoring highlights important parameters in the design of viral vectored ZIKV vaccines to support further clinical assessments

LAReferencia - Red Federada de Repositorios Institucionales de Publicaciones Científicas Latinoamericanas

Rational Zika vaccine design via the modulation of antigen membrane anchors in chimpanzee adenoviral vectors

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