The Pleiotropic Effects of Fisetin and Hesperetin on Human Acute Promyelocytic Leukemia Cells Are Mediated Through Apoptosis, Cell Cycle Arrest, and Alterations in Signaling Networks

dc.contributor.author Adan, Aysun
dc.contributor.author Baran, Yusuf
dc.date.accessioned 2025-09-25T10:59:32Z
dc.date.available 2025-09-25T10:59:32Z
dc.date.issued 2015
dc.description Adan, Aysun/0000-0002-3747-8580; Baran, Yusuf/0000-0002-1056-4673 en_US
dc.description.abstract Fisetin and hesperetin, flavonoids from various plants, have several pharmaceutical activities including antioxidative, anti-inflammatory, and anticancer effects. However, studies elucidating the role and the mechanism(s) of action of fisetin and hesperetin in acute promyelocytic leukemia are absent. In this study, we investigated the mechanism of the antiproliferative and apoptotic actions exerted by fisetin and hesperetin on human HL60 acute promyelocytic leukemia cells. The viability of HL60 cells was evaluated using the MTT assay, apoptosis by annexin V/propidium iodide (PI) staining and cell cycle distribution using flow cytometry, and changes in caspase-3 enzyme activity and mitochondrial transmembrane potential. Moreover, we performed whole-genome microarray gene expression analysis to reveal genes affected by fisetin and hesperetin that can be important for developing of future targeted therapy. Based on data obtained from microarray analysis, we also described biological networks modulated after fisetin and hesperetin treatment by KEGG and IPA analysis. Fisetin and hesperetin treatment showed a concentration- and time-dependent inhibition of proliferation and induced G2/M arrest for both agents and G0/G1 arrest for hesperetin at only the highest concentrations. There was a disruption of mitochondrial membrane potential together with increased caspase-3 activity. Furthermore, fisetin- and hesperetin-triggered apoptosis was confirmed by annexin V/PI analysis. The microarray gene profiling analysis revealed some important biological pathways including mitogen-activated protein kinases (MAPK) and inhibitor of DNA binding (ID) signaling pathways altered by fisetin and hesperetin treatment as well as gave a list of genes modulated a parts per thousand yen2-fold involved in cell proliferation, cell division, and apoptosis. Altogether, data suggested that fisetin and hesperetin have anticancer properties and deserve further investigation. en_US
dc.identifier.doi 10.1007/s13277-015-3597-6
dc.identifier.issn 1010-4283
dc.identifier.issn 1423-0380
dc.identifier.scopus 2-s2.0-84949109653
dc.identifier.uri https://doi.org/10.1007/s13277-015-3597-6
dc.identifier.uri https://hdl.handle.net/20.500.12573/4840
dc.language.iso en en_US
dc.publisher Sage Publications Ltd en_US
dc.relation.ispartof Tumor Biology en_US
dc.rights info:eu-repo/semantics/openAccess en_US
dc.subject Fisetin en_US
dc.subject Hesperetin en_US
dc.subject Apoptosis en_US
dc.subject Acute Promyelocytic Leukemia en_US
dc.subject Gene Profiling en_US
dc.title The Pleiotropic Effects of Fisetin and Hesperetin on Human Acute Promyelocytic Leukemia Cells Are Mediated Through Apoptosis, Cell Cycle Arrest, and Alterations in Signaling Networks en_US
dc.type Article en_US
dspace.entity.type Publication
gdc.author.id Adan, Aysun/0000-0002-3747-8580
gdc.author.id Baran, Yusuf/0000-0002-1056-4673
gdc.author.scopusid 56684634500
gdc.author.scopusid 9636164400
gdc.author.wosid Baran, Yusuf/F-8535-2012
gdc.bip.impulseclass C4
gdc.bip.influenceclass C4
gdc.bip.popularityclass C4
gdc.coar.access open access
gdc.coar.type text::journal::journal article
gdc.collaboration.industrial false
gdc.description.department Abdullah Gül University en_US
gdc.description.departmenttemp [Adan, Aysun; Baran, Yusuf] Izmir Inst Technol, Dept Mol Biol & Genet, TR-35430 Izmir, Turkey; [Baran, Yusuf] Abdullah Gul Univ, Fac Life & Nat Sci, TR-38080 Kayseri, Turkey en_US
gdc.description.endpage 8984 en_US
gdc.description.issue 11 en_US
gdc.description.publicationcategory Makale - Uluslararası Hakemli Dergi - Kurum Öğretim Elemanı en_US
gdc.description.scopusquality Q3
gdc.description.startpage 8973 en_US
gdc.description.volume 36 en_US
gdc.description.woscitationindex Science Citation Index Expanded
gdc.description.wosquality N/A
gdc.identifier.openalex W656409696
gdc.identifier.pmid 26081618
gdc.identifier.wos WOS:000366143100087
gdc.index.type WoS
gdc.index.type Scopus
gdc.index.type PubMed
gdc.oaire.accesstype GOLD
gdc.oaire.diamondjournal false
gdc.oaire.downloads 100
gdc.oaire.impulse 12.0
gdc.oaire.influence 3.669713E-9
gdc.oaire.isgreen true
gdc.oaire.keywords Flavonoids
gdc.oaire.keywords Membrane Potential, Mitochondrial
gdc.oaire.keywords Flavonols
gdc.oaire.keywords Cell Survival
gdc.oaire.keywords Hesperidin
gdc.oaire.keywords Apoptosis
gdc.oaire.keywords HL-60 Cells
gdc.oaire.keywords Cell Cycle Checkpoints
gdc.oaire.keywords Fisetin
gdc.oaire.keywords Neoplasm Proteins
gdc.oaire.keywords Gene Expression Regulation, Neoplastic
gdc.oaire.keywords Gene profiling
gdc.oaire.keywords Leukemia, Promyelocytic, Acute
gdc.oaire.keywords Acute promyelocytic leukemia
gdc.oaire.keywords Hesperetin
gdc.oaire.keywords Humans
gdc.oaire.keywords Cell Proliferation
gdc.oaire.keywords Signal Transduction
gdc.oaire.popularity 2.527957E-8
gdc.oaire.publicfunded false
gdc.oaire.sciencefields 0301 basic medicine
gdc.oaire.sciencefields 0303 health sciences
gdc.oaire.sciencefields 03 medical and health sciences
gdc.oaire.views 160
gdc.openalex.collaboration National
gdc.openalex.fwci 3.31
gdc.openalex.normalizedpercentile 0.91
gdc.openalex.toppercent TOP 10%
gdc.opencitations.count 50
gdc.plumx.crossrefcites 26
gdc.plumx.mendeley 37
gdc.plumx.pubmedcites 24
gdc.plumx.scopuscites 49
gdc.scopus.citedcount 49
gdc.virtual.author Adan, Aysun
gdc.wos.citedcount 43
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