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High-throughput screening of NOX inhibitors
Zielonka, J. ✉
;
Zielonka, M.
;
Cheng, G.
;
Hardy, M. ✉
;
Kalyanaraman, B. ✉
Angol nyelvű Könyvfejezet (Könyvrészlet) Tudományos
Megjelent:
Knaus Ulla G.. NADPH Oxidases. (2019) ISBN:9781493994236; 9781493994243
pp. 429-446
Azonosítók
MTMT: 30756664
DOI:
10.1007/978-1-4939-9424-3_25
WoS:
000487828500026
Scopus:
85067079084
Development of new, selective inhibitors of nicotinamide adenine dinucleotide phosphate oxidase (NOX) isoforms is important both for basic studies on the role of these enzymes in cellular redox signaling, cell physiology, and proliferation and for development of new drugs for diseases carrying a component of increased NOX activity, such as several types of cancer and cardiovascular and neurodegenerative diseases. High-throughput screening (HTS) of large libraries of compounds remains the major approach for development of new NOX inhibitors. Here, we describe the protocol for the HTS campaign for NOX inhibitors using rigorous assays for superoxide radical anion and hydrogen peroxide, based on oxidation of hydropropidine, coumarin boronic acid, and Amplex Red. We propose using these three probes to screen for and identify new inhibitors, by selecting positive hits that show inhibitory effects in all three assays. Protocols for the synthesis of hydropropidine and for confirmatory assays, including oxygen consumption measurements, electron paramagnetic resonance spin trapping of superoxide, and simultaneous monitoring of superoxide and hydrogen peroxide, are also provided. © Springer Science+Business Media, LLC, part of Springer Nature 2019.
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2025-04-24 16:14
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