Your search keyword '"M Datoo"' showing total 2 results

1. High Efficacy of a Low Dose Candidate Malaria Vaccine, R21 in 1 Adjuvant Matrix-M™, with Seasonal Administration to Children in Burkina Faso

Author

Karim Derra, Innocent Valea, Reshma Kailath, Katie J. Ewer, Jenny M. Reimer, Fernando Ramos-Lopez, Moubarak Tegneri, Federica Cappuccini, Benedict O. Orindi, Halidou Tinto, Seydou Sawadogo, Rachel Roberts, Toussaint Rouamba, Hermann Sorgho, Daniel Valia, Gregory M. Glenn, Florence Ouedraogo, D Bellamy, Louis Fries, Eli Rouamba, Faizatou Sorgho, Nicola Williams, Athanase M Some, Matthew Cairns, M Datoo, Amy Flaxman, Ousmane Traore, Adrian V. S. Hill, Sean C. Elias, E Mukhopadhyay, Prisca Yameogo, Umesh Shaligram, Alison M. Lawrie, Andres Noe, Rachidatou Soma, and Hamtandi Magloire Natama

Subjects

medicine.medical_specialty, Malaria vaccine, business.industry, medicine.medical_treatment, Vaccine efficacy, medicine.disease, law.invention, Clinical trial, Vaccination, Rabies vaccine, Randomized controlled trial, law, Internal medicine, parasitic diseases, medicine, business, Adjuvant, Malaria, medicine.drug

Abstract

Background: Stalled progress in controlling Plasmodium falciparum malaria highlights the need for an effective and deployable vaccine. RTS,S/AS01, the most effective malaria vaccine candidate to date, demonstrated 55·8% (97·5% confidence interval [CI], 51-60) efficacy over 12 months in African children. Methods: We conducted a double-blind, randomised, controlled trial of a low-dose circumsporozoite protein-based vaccine, R21, with two different doses of adjuvant, Matrix-M™ (MM), in children aged 5-17 months in Nanoro, Burkina Faso, a highly seasonal malaria transmission setting. Three vaccinations were administered at 4-week intervals prior to the malaria season with a fourth dose one year later. Vaccine safety, immunogenicity and efficacy were evaluated over one year. Findings: 450 children were randomised to receive the R21/MM vaccine or a control rabies vaccine. R21/MM had a 43 favourable safety profile and was well-tolerated. At 6 months, 43/146 (29·5%) who received R21/MM with low44 dose adjuvant, 38/146 (26%) who received R21/MM with high-dose adjuvant, and 105/147 (71·4%) who received the rabies vaccine developed clinical malaria. Vaccine efficacy (VE) was 74% (95% CI, 63-82) and 77% (95% CI, 67-84) in the low- and high-dose adjuvant groups, respectively. At 1 year, VE remained high at 77% (95% CI, 67-84) in the high-dose adjuvant group. Participants vaccinated with R21/MM showed high titres of malaria-specific anti-NANP antibodies 28 days after the third vaccination, which were almost doubled with the higher adjuvant dose. Titres waned but were boosted to levels similar to peak titres following the primary series of vaccinations after a fourth dose administered one year later. Interpretation: R21/Matrix-M appears safe and very immunogenic in African children, and demonstrates promising high-level efficacy. Trial Registration: ClinicalTrials.gov number: NCT03896724. Funding: The European & Developing Countries Clinical Trials Partnership (EDCTP), The Wellcome Trust and the NIHR Oxford Biomedical Research Centre. Declaration of Interest: AVSH and KJE are named as co-inventors on patent applications related to R21. GG, LF, JR and PP-A are employees of Novavax, developers of the Matrix-M adjuvant, and US is an employee of the Serum Institute of India Private Ltd, co-developer of the R21/MM vaccine. Other authors declare no competing interests. Ethical Approval: The trial was approved by the Comite d’Ethique pour la Recherche en Sante, Burkina Faso (CERS, reference number 2019-01-012), and by the national regulatory authority, Agence National de Regulation Pharmaceutique, Burkina Faso (ANRP, reference number 5005420193EC0000). Ethical approval was also granted in the United Kingdom by the Oxford Tropical Research Ethics Committee (OxTREC reference number 19-19).

Published

2021

2. Reduced blood-stage malaria growth and immune correlates in humans following RH5 vaccination

Author

Carolin Loos, Carole A. Long, Saul N. Faust, Anna Goodman, David Pulido, Fay L. Nugent, Jordan R. Barrett, Robert Smith, Katherine J. Ellis, Tatiana Ogrina, Ashlin R. Michell, Raquel Lopez Ramon, M Datoo, Galit Alter, Thomas A. Rawlinson, Michael Marks, Megan Baker, Lorraine Soisson, Nick J. Edwards, Eleanor Berrie, Ababacar Diouf, Angela M. Minassian, Willem A. de Jongh, Sarah E. Silk, Rebecca Ashfield, Doris Quinkert, D Silman, Michael T. White, Carter L. Diggs, Alison M. Lawrie, Nathan J Brendish, Alexander D. Douglas, Iona J. Taylor, Hector Maxwell-Scott, Yrene Themistocleous, Ruth O. Payne, Jonathan K. Fallon, Kazutoyo Miura, Rahul Batra, Lea Barfod, Antonio Querol-Rubiera, Celia Mitton, P M Folegatti, Ian D. Poulton, Jing Jin, Carolyn M. Nielsen, Fernando Ramos Lopez, Karen Bisnauthsing, Amy R. Noe, and Simon J. Draper

Subjects

Adult, Plasmodium falciparum, Parasitemia, Immunoglobulin G, blood-stage, vaccine, Malaria Vaccines, medicine, Humans, Malaria, Falciparum, systems serology, Clinical Trials as Topic, Vaccines, Synthetic, biology, Malaria vaccine, business.industry, Immunogenicity, Vaccination, Clinical Advances, clinical trial, General Medicine, medicine.disease, biology.organism_classification, Malaria, RH5, Immunology, biology.protein, CHMI, Antibody, business

Abstract

Summary Background Development of an effective vaccine against the pathogenic blood-stage infection of human malaria has proved challenging, and no candidate vaccine has affected blood-stage parasitemia following controlled human malaria infection (CHMI) with blood-stage Plasmodium falciparum. Methods We undertook a phase I/IIa clinical trial in healthy adults in the United Kingdom of the RH5.1 recombinant protein vaccine, targeting the P. falciparum reticulocyte-binding protein homolog 5 (RH5), formulated in AS01B adjuvant. We assessed safety, immunogenicity, and efficacy against blood-stage CHMI. Trial registered at ClinicalTrials.gov, NCT02927145. Findings The RH5.1/AS01B formulation was administered using a range of RH5.1 protein vaccine doses (2, 10, and 50 μg) and was found to be safe and well tolerated. A regimen using a delayed and fractional third dose, in contrast to three doses given at monthly intervals, led to significantly improved antibody response longevity over ∼2 years of follow-up. Following primary and secondary CHMI of vaccinees with blood-stage P. falciparum, a significant reduction in parasite growth rate was observed, defining a milestone for the blood-stage malaria vaccine field. We show that growth inhibition activity measured in vitro using purified immunoglobulin G (IgG) antibody strongly correlates with in vivo reduction of the parasite growth rate and also identify other antibody feature sets by systems serology, including the plasma anti-RH5 IgA1 response, that are associated with challenge outcome. Conclusions Our data provide a new framework to guide rational design and delivery of next-generation vaccines to protect against malaria disease. Funding This study was supported by USAID, UK MRC, Wellcome Trust, NIAID, and the NIHR Oxford-BRC., Graphical abstract, Highlights The RH5.1/AS01B vaccine is safe, well tolerated, and immunogenic in healthy adults A delayed fractional third dose significantly improves antibody response longevity In vivo blood-stage P. falciparum growth rate is significantly lower in vaccinees In vitro IgG-mediated growth inhibition activity is associated with challenge outcome, Context and significance A highly effective vaccine against the human malaria parasite Plasmodium falciparum is urgently needed. One vaccine strategy aims to prevent parasite growth in the blood, protecting against clinical disease; however, this has proved exceptionally challenging. Here we show that a candidate vaccine (reticulocyte-binding protein homolog 5.1 [RH5.1]/AS01B) is safe in a phase I/IIa clinical trial and identify a vaccination regimen that improves the durability of the human antibody response, which is critical for long-term protection. Following experimental challenge of vaccinated adults with malaria, we observed that the vaccine could reduce parasite growth in the blood and identified immune responses that could predict how well the vaccine performs. These data will help guide the design of improved vaccines in the future., Minassian et al. report that the RH5.1/AS01B vaccine against blood-stage Plasmodium falciparum malaria is safe and immunogenic in a phase I/IIa clinical trial. They demonstrate a significantly reduced blood-stage parasite growth rate in vaccinees following controlled human malaria infection and identify that in vitro antibody-mediated growth inhibition activity is associated with challenge outcome.

Published

2021