| Literature DB >> 24838008 |
Marianne Lucas-Hourani1, Hélène Munier-Lehmann2, Olivier Helynck2, Anastassia Komarova1, Philippe Desprès3, Frédéric Tangy1, Pierre-Olivier Vidalain4.
Abstract
RNA viruses are responsible for major human diseases such as flu, bronchitis, dengue, Hepatitis C or measles. They also represent an emerging threat because of increased worldwide exchanges and human populations penetrating more and more natural ecosystems. A good example of such an emerging situation is chikungunya virus epidemics of 2005-2006 in the Indian Ocean. Recent progresses in our understanding of cellular pathways controlling viral replication suggest that compounds targeting host cell functions, rather than the virus itself, could inhibit a large panel of RNA viruses. Some broad-spectrum antiviral compounds have been identified with host target-oriented assays. However, measuring the inhibition of viral replication in cell cultures using reduction of cytopathic effects as a readout still represents a paramount screening strategy. Such functional screens have been greatly improved by the development of recombinant viruses expressing reporter enzymes capable of bioluminescence such as luciferase. In the present report, we detail a high-throughput screening pipeline, which combines recombinant measles and chikungunya viruses with cellular viability assays, to identify compounds with a broad-spectrum antiviral profile.Entities:
Mesh:
Substances:
Year: 2014 PMID: 24838008 PMCID: PMC4172263 DOI: 10.3791/51222
Source DB: PubMed Journal: J Vis Exp ISSN: 1940-087X Impact factor: 1.355