Your search keyword '"Meyer, Stéphanie"' showing total 2 results

1. From bench to clinic: the development of VLA1553/IXCHIQ, a live-attenuated chikungunya vaccine.

Author

Chen, Lin H, Fritzer, Andrea, Hochreiter, Romana, Dubischar, Katrin, and Meyer, Stéphanie

Subjects

CHIKUNGUNYA virus, CLINICAL trials, VIRUS diseases, ANTIBODY titer, CHIKUNGUNYA

Abstract

Background Over the past 20 years, over 5 million cases of chikungunya, a mosquito-transmitted viral disease, have been reported in over 110 countries. Until recently, preventative strategies for chikungunya were largely ineffective, relying on vector control and individual avoidance of mosquito bites. Methods This review outlines the preclinical and clinical efficacy and safety data that led to the approval of VLA1553 (IXCHIQ®), a live-attenuated vaccine against chikungunya disease. It also describes the innovative development pathway of VLA1553, based on an immunological surrogate of protection, and discusses ongoing and future post-licensure studies. Results In mice and non-human primate models, VLA1553 elicited high titres of neutralizing antibodies, conferred protection against wild-type chikungunya virus challenge and raised no safety concerns. A Phase 1 clinical trial of VLA1553 demonstrated 100% seroconversion among 120 healthy participants, with sustained neutralizing antibody titres after 12 months. These results and determination of a surrogate marker of protection led to advancement of VLA1553 directly into Phase 3 clinical development, as agreed with the US Food and Drug Administration (FDA) and the European Medicines Agency. The pivotal Phase 3 trial met its primary immunogenicity endpoint, achieving seroprotective levels based on immuno-bridging in baseline seronegative participants 28 days post-vaccination. These findings enabled submission of a Biologics Licence Application to the FDA for accelerated approval of VLA1553 in the US for adults aged ≥18 years. Ongoing and planned studies will confirm the clinical efficacy/effectiveness and safety of VLA1553 in adults and younger individuals, and will generate data in chikungunya endemic countries that have the highest unmet need. Conclusion VLA1553 is the first vaccine approved for the prevention of chikungunya disease in adults, following accelerated development based on a serological surrogate marker of protection. VLA1553 adds to strategies to reduce the spread and burden of chikungunya in endemic populations and travellers. [ABSTRACT FROM AUTHOR]

Published

2024

2. Immunogenicity and Safety of a Tetravalent Dengue Vaccine Administered Concomitantly or Sequentially With Tdap Vaccine

Author

Santos, Jaime, Montellano, May Emmeline, Solante, Rontgene, Perreras, Nicole, Meyer, Stéphanie, Toh, Myew-Ling, Zocchetti, Céline, Vigne, Claire, and Mascareñas, Cesar

Subjects

safety, Adult, Male, Adolescent, Philippines, Dengue Vaccines, immunogenicity, Middle Aged, Antibodies, Viral, Diphtheria-Tetanus-acellular Pertussis Vaccines, Antibodies, Bacterial, Vaccine Reports, Healthy Volunteers, Dengue, Young Adult, Immunogenicity, Vaccine, dengue vaccine, ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, Humans, Female, Immunization, Vaccines, Combined, Child, Tdap vaccine, Immunization Schedule

Abstract

Supplemental Digital Content is available in the text., Background: Incorporating dengue vaccination into existing childhood vaccination programs could increase vaccine coverage. This study assessed the safety and immunogenicity of concomitant versus sequential administration of the combined tetanus toxoid, reduced diphtheria toxoid and acellular pertussis (Tdap) vaccine and the tetravalent dengue vaccine (CYD-TDV). Methods: This phase IIIb, randomized, open-label, multicenter study was conducted in the Philippines in individuals 9–≤60 years of age (NCT02992418). Participants were to receive 3 CYD-TDV doses 6 months apart, the first dose administered either concomitantly or sequentially (28 days post-Tdap). Antibody levels were measured at baseline and 28 days post-first doses of Tdap vaccine and CYD-TDV, using enzyme-linked immunosorbent assay (pertussis, tetanus), micrometabolic inhibition test-toxin neutralization assay (diphtheria) and plaque reduction neutralization test (dengue). Immunogenicity was assessed for all participants, and statistical analysis reported for baseline dengue seropositive participants. Safety was assessed throughout. Results: Among 688 randomized participants, 629 (91.4%) were baseline dengue seropositive (concomitant group, n = 314 and sequential group, n = 315). After the first dose, non-inferiority of immune responses between concomitant and sequential vaccination was achieved; between-group geometric mean antibody concentration ratios were close to 1 for anti-PT, anti-FHA, anti-PRN and anti-FIM, between-group differences in percent achieving seroprotection (titers ≥0.1 IU/mL) were 0.26% (diphtheria) and 0.66% (tetanus), and between-group geometric mean antibody titer ratios were close to 1 for dengue serotypes 1–4. Safety profiles in both study groups were comparable. Conclusions: CYD-TDV and Tdap vaccine administered concomitantly or sequentially in baseline dengue seropositive participants elicited comparable immunogenicity and safety profiles.

Published

2021