| Literature DB >> 24149002 |
Manfred Marschall1, Ina Niemann, Karin Kosulin, Anna Bootz, Sabrina Wagner, Thomas Dobner, Thomas Herz, Bernd Kramer, Johann Leban, Daniel Vitt, Thomas Stamminger, Corina Hutterer, Stefan Strobl.
Abstract
Currently available antiviral drugs frequently induce side-effects or selection of drug-resistant viruses. We describe a novel antiviral principle based on targeting the cellular enzyme dihydroorotate dehydrogenase (DHODH). In silico drug design and biochemical evaluation identified Compound 1 (Cmp1) as a selective inhibitor of human DHODH in vitro (IC50 1.5±0.2nM). Crystallization data specified the mode of drug-target interaction. Importantly, Cmp1 displayed a very potent antiviral activity that could be reversed by co-application of uridine or other pyrimidine precursors, underlining the postulated DHODH-directed mode of activity. Human and animal cytomegaloviruses as well as adenoviruses showed strong sensitivity towards Cmp1 in cell culture-based infection systems with IC50 values in the low micromolar to nanomolar range. Particularly, broad inhibitory activity was demonstrated for various types of laboratory and clinically relevant adenoviruses. For replication of human cytomegalovirus in primary fibroblasts, antiviral mode of activity was attributed to the early stage of gene expression. A mouse in vivo model proved reduced replication of murine cytomegalovirus in various organs upon Cmp1 treatment. These findings suggested Cmp1 as drug candidate and validated DHODH as a promising cellular target for antiviral therapy.Entities:
Keywords: 4SCan drug design; Antiviral drug candidate; Broad-spectrum antiviral therapy; Cytomegaloviruses and adenoviruses; Pyrimidine biosynthesis; Target dihydroorotate dehydrogenase
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Year: 2013 PMID: 24149002 DOI: 10.1016/j.antiviral.2013.10.003
Source DB: PubMed Journal: Antiviral Res ISSN: 0166-3542 Impact factor: 5.970