Stilbenoid derivatives as potent inhibitors of HIF-1α-centric cancer metabolism under hypoxia

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dc.contributor.authorTae Hee Han-
dc.contributor.authorJ Lee-
dc.contributor.authorD S Harmalkar-
dc.contributor.authorH Kang-
dc.contributor.authorG Jin-
dc.contributor.authorM K Park-
dc.contributor.authorM Kim-
dc.contributor.authorHyun A Yang-
dc.contributor.authorJinsu Kim-
dc.contributor.authorS J Kwon-
dc.contributor.authorTae-Su Han-
dc.contributor.authorY Choi-
dc.contributor.authorMi Sun Won-
dc.contributor.authorHyun Seung Ban-
dc.contributor.authorK Lee-
dc.date.accessioned2024-05-31T16:32:53Z-
dc.date.available2024-05-31T16:32:53Z-
dc.date.issued2024-
dc.identifier.issn0753-3322-
dc.identifier.urihttps://oak.kribb.re.kr/handle/201005/35171-
dc.description.abstractHypoxia-inducible factor (HIF)-1α is a crucial transcription factor associated with cancer metabolism and is regarded as a potent anticancer therapeutic strategy within the hypoxic microenvironment of cancer. In this study, stilbenoid derivatives were designed, synthesized, and assessed for their capacity to inhibit HIF-1α-associated cancer metabolism and evaluated for inhibition of cancer cell viability and HIF activation. Through the structure-activity relationship studies, compound 28e was identified as the most potent derivative. Specifically, under the hypoxic condition, 28e reduced the accumulation of HIF-1α protein and the expression of its target genes related to glucose metabolism without affecting the expression of HIF-1α mRNA. Furthermore, 28e inhibited glucose uptake, glycolytic metabolism, and mitochondrial respiration, decreasing cellular ATP production under hypoxic conditions. In addition, 28e displayed significant anti-tumor effects and effectively suppressed the accumulation of HIF-1α protein in tumor tissue in vivo xenograft model. These findings suggest that our stilbenoid derivatives exert their anticancer effects by targeting HIF-1α-centered cancer metabolism under hypoxic conditions.-
dc.publisherElsevier-
dc.titleStilbenoid derivatives as potent inhibitors of HIF-1α-centric cancer metabolism under hypoxia-
dc.title.alternativeStilbenoid derivatives as potent inhibitors of HIF-1α-centric cancer metabolism under hypoxia-
dc.typeArticle-
dc.citation.titleBiomedicine & Pharmacotherapy-
dc.citation.number0-
dc.citation.endPage116838-
dc.citation.startPage116838-
dc.citation.volume176-
dc.contributor.affiliatedAuthorTae Hee Han-
dc.contributor.affiliatedAuthorHyun A Yang-
dc.contributor.affiliatedAuthorJinsu Kim-
dc.contributor.affiliatedAuthorTae-Su Han-
dc.contributor.affiliatedAuthorMi Sun Won-
dc.contributor.affiliatedAuthorHyun Seung Ban-
dc.contributor.alternativeName한태희-
dc.contributor.alternativeName이주한-
dc.contributor.alternativeNameHarmalkar-
dc.contributor.alternativeName강혜슬-
dc.contributor.alternativeName진광해-
dc.contributor.alternativeName박민경-
dc.contributor.alternativeName김민경-
dc.contributor.alternativeName양현아-
dc.contributor.alternativeName김진수-
dc.contributor.alternativeName권수정-
dc.contributor.alternativeName한태수-
dc.contributor.alternativeName최용석-
dc.contributor.alternativeName원미선-
dc.contributor.alternativeName반현승-
dc.contributor.alternativeName이경-
dc.identifier.bibliographicCitationBiomedicine & Pharmacotherapy, vol. 176, pp. 116838-116838-
dc.identifier.doi10.1016/j.biopha.2024.116838-
dc.subject.keywordStilbenoid analogs-
dc.subject.keywordAnticancer activity-
dc.subject.keywordHypoxic cancer-
dc.subject.keywordHIF-1α-
dc.subject.keywordCancer metabolism-
dc.subject.localAnti-cancer activity-
dc.subject.localAnticancer activity-
dc.subject.localanticancer activity-
dc.subject.localHIF-1α-
dc.subject.localHIF1α-
dc.subject.localHif1α-
dc.subject.localCancer metabolism-
dc.subject.localcancer metabolism-
dc.subject.localcancer metabolsm-
dc.subject.localCancer Metabolism-
dc.description.journalClassY-
Appears in Collections:
Division of A.I. & Biomedical Research > Biotherapeutics Translational Research Center > 1. Journal Articles
Division of A.I. & Biomedical Research > Genomic Medicine Research Center > 1. Journal Articles
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