| Literature DB >> 29338172 |
Irina N Gaisina1, Sue H Lee1, Navneet A Kaidery2, Manel Ben Aissa1, Manuj Ahuja2, Natalya N Smirnova3, Sushama Wakade2, Arsen Gaisin4, Megan W Bourassa5,6, Rajiv R Ratan5,6, Sergey V Nikulin3, Andrey A Poloznikov3, Bobby Thomas2, Gregory R J Thatcher1, Irina G Gazaryan3,5,6,7.
Abstract
Activation of HIF-1α and Nrf2 is a primary component of cellular response to oxidative stress, and activation of HIF-1α and Nrf2 provides neuroprotection in models of neurodegenerative disorders, including ischemic stroke, Alzheimer's and Parkinson's diseases. Screening a library of CNS-targeted drugs using novel reporters for HIF-1α and Nrf2 elevation in neuronal cells revealed histone deacetylase (HDAC) inhibitors as potential activators of these pathways. We report the identification of phenylhydroxamates as single agents exhibiting tripartite inhibition of HDAC6, inhibition of HIF-1 prolyl hydroxylase (PHD), and activation of Nrf2. Two superior tripartite agents, ING-6 and ING-66, showed neuroprotection against various cellular insults, associated with stabilization of both Nrf2 and HIF-1, and expression of their respective target genes in vitro and in vivo. Discovery of the innate ability of phenylhydroxamate HDAC inhibitors to activate Nrf2 and HIF provides a novel route to multifunctional neuroprotective agents and cautions against HDAC6 selective inhibitors as chemical probes of specific HDAC isoform function.Entities:
Keywords: HIF-1 activators; Nrf2 activators; Phenylhydroxamates; histone deacetylase inhibitors; neuroprotection; oxidative stress
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Year: 2018 PMID: 29338172 PMCID: PMC5955769 DOI: 10.1021/acschemneuro.7b00435
Source DB: PubMed Journal: ACS Chem Neurosci ISSN: 1948-7193 Impact factor: 4.418