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Development of Dengue virus type 2 replicons capable of prolonged expression in host cells

Published by National Institutes of Health | U.S. Department of Health & Human Services | Metadata Last Checked: September 07, 2025 | Last Modified: 2025-09-06
Background As part of a program to develop a Dengue virus vaccine which avoids the deleterious effects of antibody dependent enhancement (ADE) of infection mediated by antibodies to Dengue virus structural proteins, we have begun to investigate the possibility of designing Dengue vaccines based on non-structural proteins. Results Dengue constructs which lack major structural proteins replicate intracellularly in tissue culture. These replicons are capable of prolonged expression of Dengue virus non-structural proteins for at least seven days in culture. Conclusions Dengue virus genomes lacking major structural proteins can, like other flaviviruses, replicate intracellularly and express virus non-structural proteins with minimal toxicity to host cells. These findings pave the way for the development of dengue virus replicons as a form of live, attenuated virus vaccine.

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Complete Metadata
@type dcat:Dataset
accessLevel public
bureauCode 
                                            [
  "009:25"
]
contactPoint 
                                            {
  "fn": "NIH",
  "@type": "vcard:Contact",
  "hasEmail": "mailto:info@nih.gov"
}
description Background As part of a program to develop a Dengue virus vaccine which avoids the deleterious effects of antibody dependent enhancement (ADE) of infection mediated by antibodies to Dengue virus structural proteins, we have begun to investigate the possibility of designing Dengue vaccines based on non-structural proteins. Results Dengue constructs which lack major structural proteins replicate intracellularly in tissue culture. These replicons are capable of prolonged expression of Dengue virus non-structural proteins for at least seven days in culture. Conclusions Dengue virus genomes lacking major structural proteins can, like other flaviviruses, replicate intracellularly and express virus non-structural proteins with minimal toxicity to host cells. These findings pave the way for the development of dengue virus replicons as a form of live, attenuated virus vaccine.
distribution 
                                            [
  {
    "@type": "dcat:Distribution",
    "title": "Official Government Data Source",
    "mediaType": "text/html",
    "description": "Visit the original government dataset for complete information, documentation, and data access.",
    "downloadURL": "https://www.ncbi.nlm.nih.gov/pmc/articles/PMC56997/"
  }
]
identifier https://healthdata.gov/api/views/wpns-us4a
issued 2025-07-14
keyword 
                                            [
  "dengue-virus",
  "nih",
  "vaccine-development",
  "viral-replicons"
]
landingPage https://healthdata.gov/d/wpns-us4a
modified 2025-09-06
programCode 
                                            [
  "009:033"
]
publisher 
                                            {
  "name": "National Institutes of Health",
  "@type": "org:Organization"
}
theme 
                                            [
  "NIH"
]
title Development of Dengue virus type 2 replicons capable of prolonged expression in host cells

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