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Kinome Profiling Identifies Druggable Targets for Novel Human Cytomegalovirus (HCMV) Antivirals.
Arend, Kyle C; Lenarcic, Erik M; Vincent, Heather A; Rashid, Naim; Lazear, Eric; McDonald, Ian M; Gilbert, Thomas S K; East, Michael P; Herring, Laura E; Johnson, Gary L; Graves, Lee M; Moorman, Nathaniel J.
Afiliación
  • Arend KC; From the ‡Department of Microbiology & Immunology.
  • Lenarcic EM; ¶Lineberger Comprehensive Cancer Center.
  • Vincent HA; From the ‡Department of Microbiology & Immunology.
  • Rashid N; ¶Lineberger Comprehensive Cancer Center.
  • Lazear E; From the ‡Department of Microbiology & Immunology.
  • McDonald IM; ¶Lineberger Comprehensive Cancer Center.
  • Gilbert TS; ¶Lineberger Comprehensive Cancer Center.
  • East MP; ‖Department of Biostatistics.
  • Herring LE; From the ‡Department of Microbiology & Immunology.
  • Johnson GL; ¶Lineberger Comprehensive Cancer Center.
  • Graves LM; §Department of Pharmacology.
  • Moorman NJ; §Department of Pharmacology.
Mol Cell Proteomics ; 16(4 suppl 1): S263-S276, 2017 04.
Article en En | MEDLINE | ID: mdl-28237943
Human cytomegalovirus (HCMV) is a significant cause of disease in immune-compromised adults and immune naïve newborns. No vaccine exists to prevent HCMV infection, and current antiviral therapies have toxic side effects that limit the duration and intensity of their use. There is thus an urgent need for new strategies to treat HCMV infection. Repurposing existing drugs as antivirals is an attractive approach to limit the time and cost of new antiviral drug development. Virus-induced changes in infected cells are often driven by changes in cellular kinase activity, which led us to hypothesize that defining the complement of kinases (the kinome), whose abundance or expression is altered during infection would identify existing kinase inhibitors that could be repurposed as new antivirals. To this end, we applied a kinase capture technique, multiplexed kinase inhibitor bead-mass spectrometry (MIB-MS) kinome, to quantitatively measure perturbations in >240 cellular kinases simultaneously in cells infected with a laboratory-adapted (AD169) or clinical (TB40E) HCMV strain. MIB-MS profiling identified time-dependent increases and decreases in MIB binding of multiple kinases including cell cycle kinases, receptor tyrosine kinases, and mitotic kinases. Based on the kinome data, we tested the antiviral effects of kinase inhibitors and other compounds, several of which are in clinical use or development. Using a novel flow cytometry-based assay and a fluorescent reporter virus we identified three compounds that inhibited HCMV replication with IC50 values of <1 µm, and at doses that were not toxic to uninfected cells. The most potent inhibitor of HCMV replication was OTSSP167 (IC50 <1.2 nm), a MELK inhibitor, blocked HCMV early gene expression and viral DNA accumulation, resulting in a >3 log decrease in virus replication. These results show the utility of MIB-MS kinome profiling for identifying existing kinase inhibitors that can potentially be repurposed as novel antiviral drugs.
Asunto(s)

Texto completo: 1 Colección: 01-internacional Base de datos: MEDLINE Asunto principal: Antivirales / Citomegalovirus / Inhibidores de Proteínas Quinasas Límite: Humans Idioma: En Revista: Mol Cell Proteomics Asunto de la revista: BIOLOGIA MOLECULAR / BIOQUIMICA Año: 2017 Tipo del documento: Article

Texto completo: 1 Colección: 01-internacional Base de datos: MEDLINE Asunto principal: Antivirales / Citomegalovirus / Inhibidores de Proteínas Quinasas Límite: Humans Idioma: En Revista: Mol Cell Proteomics Asunto de la revista: BIOLOGIA MOLECULAR / BIOQUIMICA Año: 2017 Tipo del documento: Article
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