Your browser doesn't support javascript.
loading
Safety and Immunogenicity of Novel Adenovirus Type 26- and Modified Vaccinia Ankara-Vectored Ebola Vaccines: A Randomized Clinical Trial.
Milligan, Iain D; Gibani, Malick M; Sewell, Richard; Clutterbuck, Elizabeth A; Campbell, Danielle; Plested, Emma; Nuthall, Elizabeth; Voysey, Merryn; Silva-Reyes, Laura; McElrath, M Juliana; De Rosa, Stephen C; Frahm, Nicole; Cohen, Kristen W; Shukarev, Georgi; Orzabal, Nicola; van Duijnhoven, Wilbert; Truyers, Carla; Bachmayer, Nora; Splinter, Daniel; Samy, Nathaly; Pau, Maria Grazia; Schuitemaker, Hanneke; Luhn, Kerstin; Callendret, Benoit; Van Hoof, Johan; Douoguih, Macaya; Ewer, Katie; Angus, Brian; Pollard, Andrew J; Snape, Matthew D.
Afiliación
  • Milligan ID; Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford, United Kingdom.
  • Gibani MM; Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford, United Kingdom.
  • Sewell R; Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford, United Kingdom.
  • Clutterbuck EA; Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford, United Kingdom.
  • Campbell D; Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford, United Kingdom.
  • Plested E; Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford, United Kingdom.
  • Nuthall E; Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford, United Kingdom.
  • Voysey M; Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford, United Kingdom2Nuffield Department of Primary Care Health Sciences, University of Oxford, Oxford, United Kingdom.
  • Silva-Reyes L; Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford, United Kingdom.
  • McElrath MJ; Vaccine and Infectious Disease Division, Fred Hutchinson Cancer Research Center, Seattle, Washington.
  • De Rosa SC; Vaccine and Infectious Disease Division, Fred Hutchinson Cancer Research Center, Seattle, Washington.
  • Frahm N; Vaccine and Infectious Disease Division, Fred Hutchinson Cancer Research Center, Seattle, Washington.
  • Cohen KW; Vaccine and Infectious Disease Division, Fred Hutchinson Cancer Research Center, Seattle, Washington.
  • Shukarev G; Janssen, Pharmaceutical Companies of Johnson & Johnson, Leiden, the Netherlands.
  • Orzabal N; Janssen, Pharmaceutical Companies of Johnson & Johnson, Leiden, the Netherlands.
  • van Duijnhoven W; Janssen, Pharmaceutical Companies of Johnson & Johnson, Leiden, the Netherlands.
  • Truyers C; Janssen, Pharmaceutical Companies of Johnson & Johnson, Leiden, the Netherlands.
  • Bachmayer N; Janssen, Pharmaceutical Companies of Johnson & Johnson, Leiden, the Netherlands.
  • Splinter D; Janssen, Pharmaceutical Companies of Johnson & Johnson, Leiden, the Netherlands.
  • Samy N; Bavarian Nordic, Martinsried, Germany.
  • Pau MG; Janssen, Pharmaceutical Companies of Johnson & Johnson, Leiden, the Netherlands.
  • Schuitemaker H; Janssen, Pharmaceutical Companies of Johnson & Johnson, Leiden, the Netherlands.
  • Luhn K; Janssen, Pharmaceutical Companies of Johnson & Johnson, Leiden, the Netherlands.
  • Callendret B; Janssen, Pharmaceutical Companies of Johnson & Johnson, Leiden, the Netherlands.
  • Van Hoof J; Janssen, Pharmaceutical Companies of Johnson & Johnson, Leiden, the Netherlands.
  • Douoguih M; Janssen, Pharmaceutical Companies of Johnson & Johnson, Leiden, the Netherlands.
  • Ewer K; Jenner Institute, Centre for Clinical Vaccinology and Tropical Medicine, University of Oxford, Oxford, United Kingdom7National Institute for Health Research (NIHR) Oxford Biomedical Research Centre, Oxford, United Kingdom.
  • Angus B; Nuffield Department of Medicine, University of Oxford, Oxford, United Kingdom.
  • Pollard AJ; Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford, United Kingdom7National Institute for Health Research (NIHR) Oxford Biomedical Research Centre, Oxford, United Kingdom.
  • Snape MD; Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford, United Kingdom7National Institute for Health Research (NIHR) Oxford Biomedical Research Centre, Oxford, United Kingdom.
JAMA ; 315(15): 1610-23, 2016 Apr 19.
Article en En | MEDLINE | ID: mdl-27092831
IMPORTANCE: Developing effective vaccines against Ebola virus is a global priority. OBJECTIVE: To evaluate an adenovirus type 26 vector vaccine encoding Ebola glycoprotein (Ad26.ZEBOV) and a modified vaccinia Ankara vector vaccine, encoding glycoproteins from Ebola virus, Sudan virus, Marburg virus, and Tai Forest virus nucleoprotein (MVA-BN-Filo). DESIGN, SETTING, AND PARTICIPANTS: Single-center, randomized, placebo-controlled, observer-blind, phase 1 trial performed in Oxford, United Kingdom, enrolling healthy 18- to 50-year-olds from December 2014; 8-month follow-up was completed October 2015. INTERVENTIONS: Participants were randomized into 4 groups, within which they were simultaneously randomized 5:1 to receive study vaccines or placebo. Those receiving active vaccines were primed with Ad26.ZEBOV (5 × 10(10) viral particles) or MVA-BN-Filo (1 × 10(8) median tissue culture infective dose) and boosted with the alternative vaccine 28 or 56 days later. A fifth, open-label group received Ad26.ZEBOV boosted by MVA-BN-Filo 14 days later. MAIN OUTCOMES AND MEASURES: The primary outcomes were safety and tolerability. All adverse events were recorded until 21 days after each immunization; serious adverse events were recorded throughout the trial. Secondary outcomes were humoral and cellular immune responses to immunization, as assessed by enzyme-linked immunosorbent assay and enzyme-linked immunospot performed at baseline and from 7 days after each immunization until 8 months after priming immunizations. RESULTS: Among 87 study participants (median age, 38.5 years; 66.7% female), 72 were randomized into 4 groups of 18, and 15 were included in the open-label group. Four participants did not receive a booster dose; 67 of 75 study vaccine recipients were followed up at 8 months. No vaccine-related serious adverse events occurred. No participant became febrile after MVA-BN-Filo, compared with 3 of 60 participants (5%; 95% CI, 1%-14%) receiving Ad26.ZEBOV in the randomized groups. In the open-label group, 4 of 15 Ad26.ZEBOV recipients (27%; 95% CI, 8%-55%) experienced fever. In the randomized groups, 28 of 29 Ad26.ZEBOV recipients (97%; 95% CI, 82%- 99.9%) and 7 of 30 MVA-BN-Filo recipients (23%; 95% CI, 10%-42%) had detectable Ebola glycoprotein-specific IgG 28 days after primary immunization. All vaccine recipients had specific IgG detectable 21 days postboost and at 8-month follow-up. Within randomized groups, at 7 days postboost, at least 86% of vaccine recipients showed Ebola-specific T-cell responses. CONCLUSIONS AND RELEVANCE: In this phase 1 study of healthy volunteers, immunization with Ad26.ZEBOV or MVA-BN-Filo did not result in any vaccine-related serious adverse events. An immune response was observed after primary immunization with Ad26.ZEBOV; boosting by MVA-BN-Filo resulted in sustained elevation of specific immunity. These vaccines are being further assessed in phase 2 and 3 studies. TRIAL REGISTRATION: clinicaltrials.gov Identifier: NCT02313077.
Asunto(s)

Texto completo: 1 Banco de datos: MEDLINE Asunto principal: Fiebre Hemorrágica Ebola / Vacunas contra el Virus del Ébola / Ebolavirus / Inmunidad Humoral Tipo de estudio: Clinical_trials Límite: Adult / Female / Humans / Male / Middle aged Idioma: En Revista: JAMA Año: 2016 Tipo del documento: Article País de afiliación: Reino Unido

Texto completo: 1 Banco de datos: MEDLINE Asunto principal: Fiebre Hemorrágica Ebola / Vacunas contra el Virus del Ébola / Ebolavirus / Inmunidad Humoral Tipo de estudio: Clinical_trials Límite: Adult / Female / Humans / Male / Middle aged Idioma: En Revista: JAMA Año: 2016 Tipo del documento: Article País de afiliación: Reino Unido