Phase I Trial of 16 Formulations of a Tetravalent Live-attenuated Dengue Vaccine

Overview

Journal Am J Trop Med Hyg

Specialty Tropical Medicine

Date 2004 Jan 27

PMID 14740955

Citations 53

Authors

Robert Edelman

Steven S Wasserman

Sacared A Bodison

Robert J Putnak

Kenneth H Eckels

Douglas Tang

Niranjan Kanesa-Thasan

David W Vaughn

Bruce L Innis

Wellington Sun

Affiliations

Soon will be listed here.

Abstract

Laboratory-attenuated strains of each of the four dengue serotypes previously tested as monovalent vaccines in volunteers were combined and tested for immunogenicity, safety, and reactogenicity in 16 dosage combinations. Tetravalent vaccines made using combinations of high (10(5-6) plaque-forming units [PFU]/dose) or low (10(3.5-4.5) PFU/dose) dosage formulations of each of the four viruses were inoculated in 64 flavivirus non-immune adult volunteers to determine which, if any, formulation raised neutralizing antibodies in at least 75% of volunteers to at least three of four dengue serotypes following one or two inoculations. Such formulations, if safe and sufficiently non-reactogenic, would be considered for an expanded Phase II trial in the future. Formulations 1-15 were each inoculated into three or four volunteers (total = 54) on days 0 and 28. Formulation 16 was tested in 10 volunteers, five volunteers inoculated on days 0 and 30, one volunteer on days 0 and 120, and four volunteers on days 0, 30, and 120. Blood was drawn for serologic assays immediately before and one month after each vaccination, and for viremia assay on day 10 after each vaccination. The 16 formulations were safe, but variably reactogenic after the first vaccination, and nearly non-reactogenic after the second and third vaccinations. Reactogenicity was positively correlated with immunogenicity. Similar proportions of volunteers seroconverted to dengue-1 (69%), dengue-2 (78%), and dengue-3 (69%), but significantly fewer volunteers seroconverted to dengue-4 (38%). The geometric mean 50% plaque reduction neutralization test titers in persons who seroconverted were significantly higher to dengue-1 (1:94) than to dengue-2 (1:15), dengue-3 (1:10), and dengue-4 (1:2). Seven formulations met the serologic criteria required for an expanded trial, and three of these were sufficiently attenuated clinically to justify further testing.

Citing Articles

Enhancing Virus with Celcradle™ Bioreactor: A Comparative Study with Traditional Cell Culture Methods.

Guo H, Ding X, Hua D, Liu M, Yang M, Gong Y Vaccines (Basel). 2024; 12(6).

PMID: 38932292 PMC: 11209354. DOI: 10.3390/vaccines12060563.

Is new dengue vaccine efficacy data a relief or cause for concern?.

Thomas S NPJ Vaccines. 2023; 8(1):55.

PMID: 37061527 PMC: 10105158. DOI: 10.1038/s41541-023-00658-2.

Adenovirus vector-based vaccines as forefront approaches in fighting the battle against flaviviruses.

Shoushtari M, Roohvand F, Salehi-Vaziri M, Arashkia A, Bakhshi H, Azadmanesh K Hum Vaccin Immunother. 2022; 18(5):2079323.

PMID: 35714271 PMC: 9481145. DOI: 10.1080/21645515.2022.2079323.

A phase I randomized, double-blind, placebo-controlled study to evaluate the safety, tolerability, and immunogenicity of a live-attenuated quadrivalent dengue vaccine in flavivirus-naïve and flavivirus-experienced healthy adults.

Russell K, Rupp R, Morales-Ramirez J, Diaz-Perez C, Andrews C, Lee A Hum Vaccin Immunother. 2022; 18(5):2046960.

PMID: 35290152 PMC: 9225326. DOI: 10.1080/21645515.2022.2046960.

Enhanced dengue vaccine virus replication and neutralizing antibody responses in immune primed rhesus macaques.

McCracken M, Kuklis C, Kannadka C, Barvir D, Sanborn M, Waickman A NPJ Vaccines. 2021; 6(1):77.

PMID: 34021159 PMC: 8140083. DOI: 10.1038/s41541-021-00339-y.