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DC FieldValueLanguage
dc.contributor.author하정미-
dc.date.accessioned2023-12-22T02:04:37Z-
dc.date.available2023-12-22T02:04:37Z-
dc.date.issued2023-07-
dc.identifier.citationPharmaceuticals, v. 16, NO. 7, article no. 1009, Page. 1.0-20.0-
dc.identifier.issn1424-8247;1424-8247-
dc.identifier.urihttps://www.proquest.com/docview/2843085017?accountid=11283en_US
dc.identifier.urihttps://repository.hanyang.ac.kr/handle/20.500.11754/187881-
dc.description.abstractKinases play an important role in regulating various intracellular signaling pathways that control cell proliferation, differentiation, survival, and other cellular processes, and their deregulation causes more than 400 diseases. Consequently, macrocyclization can be considered a noteworthy approach to developing new therapeutic agents for human diseases. Macrocyclization has emerged as an effective drug discovery strategy over the past decade to improve target selectivity and potency of small molecules. Small compounds with linear structures upon macrocyclization can lead to changes in their physicochemical and biological properties by firmly reducing conformational flexibility. A number of distinct protein kinases exhibit similar binding sites. Comparison of protein binding sites provides crucial insights for drug discovery and development. Binding site similarities are helpful in understanding polypharmacology, identifying potential off-targets, and repurposing known drugs. In this review, we focused on comparing the binding sites of those kinases for which macrocyclic inhibitors are available/studied so far. Furthermore, we calculated the volume of the binding site pocket for each targeted kinase and then compared it with the binding site pocket of the kinase for which only acyclic inhibitors were designed to date. Our review and analysis of several explored kinases might be useful in targeting new protein kinases for macrocyclic drug discovery. © 2023 by the authors.-
dc.description.sponsorshipThis work was financially supported by a National Research Foundation of Korea grant, NRF-2020R1A6A1A03042854 (Center for Proteinopathy), and Hanyang University (HY-2023).-
dc.languageen-
dc.publisherMultidisciplinary Digital Publishing Institute (MDPI)-
dc.subjectdrug discovery-
dc.subjecthuman diseases-
dc.subjectkinases-
dc.subjectmacrocyclic inhibitors-
dc.titleAn Intriguing Purview on the Design of Macrocyclic Inhibitors for Unexplored Protein Kinases through Their Binding Site Comparison-
dc.typeArticle-
dc.relation.no7-
dc.relation.volume16-
dc.identifier.doi10.3390/ph16071009-
dc.relation.page1.0-20.0-
dc.relation.journalPharmaceuticals-
dc.contributor.googleauthorBhujbal, Swapnil P.-
dc.contributor.googleauthorHah, Jung-Mi-
dc.sector.campusE-
dc.sector.daehak약학대학-
dc.sector.department약학과-
dc.identifier.pidjhah-
dc.identifier.article1009-


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