Enviar artigo por via de e-mail Antioxidant and antihypoxic properties of neuroprotective drugs
- Autores: Poloznikov A.A.1, Smirnova N.A.1, Khristichenko A.Y.1, Hushpulian D.M.1, Nikulin S.V.1, Tishkov V.I.2,3, Gaisina I.N.4, Gazaryan I.G.1,2
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Afiliações:
- D. Rogachev National Research Center of Pediatric Hematology, Oncology and Immunology
- Department of Chemistry, M. V. Lomonosov Moscow State University
- Innovation and High Technologies MSU Ltd.
- Department of Medicinal Chemistry and Pharmacognosy, University of Illinois at Chicago
- Edição: Volume 65, Nº 12 (2016)
- Páginas: 2970-2977
- Seção: Full Articles
- URL: https://ogarev-online.ru/1066-5285/article/view/239737
- DOI: https://doi.org/10.1007/s11172-016-1687-2
- ID: 239737
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Resumo
The screening of the library containing 320 drugs and biologically active compounds was carried out. The library was created for testing potent agents on Rett syndrome models (SMART library) using new-generation luciferase reporters to identify stabilizers of transcription factors triggering genetic programs for defense against hypoxia and oxidative stress (HIF1 and Nrf2, respectively). Nine compounds proved to be activators of HIF1, and 18 compounds were shown to activate Nrf2. A histone deacetylase inhibitor (oxamflatin) and a carbonic anhydrase inhibitor (ethamide) were found to be the most powerful Nrf2 activators, which are equipotent or superior to sulforaphane and quercetin. Oxamflatin was also shown to activate HIF with potency comparable or superior to the commercial HIF activators developed by Fibrogen (USA) and GlaxoSmithKline (UK), but it was a significantly weaker activator than branched tail oxyquinolines, developed in our previous studies. The structural motif identified in oxamflatin can be used in the future design of branched oxyquinolines having higher activity and/or more specific against individual isoforms of HIF prolyl hydroxylase.
Sobre autores
A. Poloznikov
D. Rogachev National Research Center of Pediatric Hematology, Oncology and Immunology
Autor responsável pela correspondência
Email: andrey.poloznikov@gmail.com
Rússia, 1 ul. Samory Mashela, Moscow, 117997
N. Smirnova
D. Rogachev National Research Center of Pediatric Hematology, Oncology and Immunology
Email: andrey.poloznikov@gmail.com
Rússia, 1 ul. Samory Mashela, Moscow, 117997
A. Khristichenko
D. Rogachev National Research Center of Pediatric Hematology, Oncology and Immunology
Email: andrey.poloznikov@gmail.com
Rússia, 1 ul. Samory Mashela, Moscow, 117997
D. Hushpulian
D. Rogachev National Research Center of Pediatric Hematology, Oncology and Immunology
Email: andrey.poloznikov@gmail.com
Rússia, 1 ul. Samory Mashela, Moscow, 117997
S. Nikulin
D. Rogachev National Research Center of Pediatric Hematology, Oncology and Immunology
Email: andrey.poloznikov@gmail.com
Rússia, 1 ul. Samory Mashela, Moscow, 117997
V. Tishkov
Department of Chemistry, M. V. Lomonosov Moscow State University; Innovation and High Technologies MSU Ltd.
Email: andrey.poloznikov@gmail.com
Rússia, Build. 3, 1 Leninskie Gory, Moscow, 119992; 16 ul. Tsimlyanskaya, Moscow, 109451
I. Gaisina
Department of Medicinal Chemistry and Pharmacognosy, University of Illinois at Chicago
Email: andrey.poloznikov@gmail.com
Estados Unidos da América, 833 South Wood Street, Chicago, IL, 60612
I. Gazaryan
D. Rogachev National Research Center of Pediatric Hematology, Oncology and Immunology; Department of Chemistry, M. V. Lomonosov Moscow State University
Email: andrey.poloznikov@gmail.com
Rússia, 1 ul. Samory Mashela, Moscow, 117997; Build. 3, 1 Leninskie Gory, Moscow, 119992
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