Her2-Targeted, Degradable Core Cross-Linked Micelles for Specific and Dual Ph-Sensitive Dox Release

dc.contributor.author Bayram, N.N.
dc.contributor.author Ulu, G.T.
dc.contributor.author Topuzoğulları, M.
dc.contributor.author Baran, Y.
dc.contributor.author Dinçer, İşoğlu, S.
dc.date.accessioned 2024-01-06T07:22:36Z
dc.date.available 2024-01-06T07:22:36Z
dc.date.issued 2022
dc.description.abstract Here, a targeted, dual-pH responsive, and stable micelle nanocarrier is designed, which specifically selects an HER2 receptor on breast cancer cells. Intracellularly degradable and stabilized micelles are prepared by core cross-linking via reversible addition−fragmentation chain-transfer (RAFT) polymerization with an acid-sensitive cross-linker followed by the conjugation of maleimide–doxorubicin to the pyridyl disulfide-modified micelles. Multifunctional nanocarriers are obtained by coupling HER2-specific peptide. Formation of micelles, addition of peptide and doxorubicin (DOX) are confirmed structurally by spectroscopical techniques. Size and morphological characterization are performed by Zetasizer and transmission electron microscope (TEM). For the physicochemical verification of the synergistic acid-triggered degradation induced by acetal and hydrazone bond degradation, Infrared spectroscopy and particle size measurements are used. Drug release studies show that DOX release is accelerated at acidic pH. DOX-conjugated HER2-specific peptide-carrying nanocarriers significantly enhance cytotoxicity toward SKBR-3 cells. More importantly, no selectivity toward MCF-10A cells is observed compared to HER2(+) SKBR-3 cells. Formulations cause apoptosis depending on Bax and Caspase-3 and cell cycle arrest in G2 phase. This study shows a novel system for HER2-targeted therapy of breast cancer with a multifunctional nanocarrier, which has higher stability, dual pH-sensitivity, selectivity, and it can be an efficient way of targeted anticancer drug delivery. © 2021 Wiley-VCH GmbH en_US
dc.description.sponsorship Türkiye Bilimsel ve Teknolojik Araştirma Kurumu, TÜBITAK: 116R057; Hacettepe Üniversitesi en_US
dc.identifier.doi 10.1002/mabi.202100375
dc.identifier.issn 1616-5187
dc.identifier.issn 1616-5195
dc.identifier.scopus 2-s2.0-85118678301
dc.identifier.uri https://doi.org/10.1002/mabi.202100375
dc.identifier.uri https://hdl.handle.net/11147/14201
dc.language.iso en en_US
dc.publisher John Wiley and Sons Inc en_US
dc.relation.ispartof Macromolecular Bioscience en_US
dc.rights info:eu-repo/semantics/closedAccess en_US
dc.subject Cell death en_US
dc.subject Controlled drug delivery en_US
dc.subject Diseases en_US
dc.subject Infrared spectroscopy en_US
dc.subject Living polymerization en_US
dc.subject Particle size en_US
dc.subject Peptides en_US
dc.subject pH sensors en_US
dc.subject Sulfur compounds en_US
dc.subject Targeted drug delivery en_US
dc.subject Transmission electron microscopy en_US
dc.subject Breast Cancer en_US
dc.subject Cross-linked micelles en_US
dc.subject Doxorubicin en_US
dc.subject Dual ph-responsiveness en_US
dc.subject HER2 targeting en_US
dc.subject Micelle nanocarrier en_US
dc.subject Multifunctional nanocarrier en_US
dc.subject Nanocarriers en_US
dc.subject Ph responsiveness en_US
dc.subject Reversible addition-fragmentation chain transfer polymerization en_US
dc.subject Micelles en_US
dc.subject antineoplastic agent en_US
dc.subject doxorubicin en_US
dc.subject drug carrier en_US
dc.subject chemistry en_US
dc.subject drug release en_US
dc.subject human en_US
dc.subject micelle en_US
dc.subject pH en_US
dc.subject Antineoplastic Agents en_US
dc.subject Doxorubicin en_US
dc.subject Drug Carriers en_US
dc.subject Drug Liberation en_US
dc.subject Humans en_US
dc.subject Hydrogen-Ion Concentration en_US
dc.subject Micelles en_US
dc.title Her2-Targeted, Degradable Core Cross-Linked Micelles for Specific and Dual Ph-Sensitive Dox Release en_US
dc.type Article en_US
dspace.entity.type Publication
gdc.author.institutional
gdc.author.scopusid 57325811500
gdc.author.scopusid 57215384419
gdc.author.scopusid 16744519800
gdc.author.scopusid 9636164400
gdc.author.scopusid 55751559400
gdc.bip.impulseclass C4
gdc.bip.influenceclass C5
gdc.bip.popularityclass C4
gdc.coar.access metadata only access
gdc.coar.type text::journal::journal article
gdc.collaboration.industrial false
gdc.description.department İzmir Institute of Technology en_US
gdc.description.departmenttemp Bayram, N.N., Department of Bioengineering, Faculty of Life and Natural Sciences, Abdullah Gül University, Kayseri, 38080, Turkey; Ulu, G.T., Molecular Biology and Genetics, Faculty of Science, İzmir Institute of Technology, İzmir, 35430, Turkey; Topuzoğulları, M., Department of Bioengineering, Faculty of Chemical and Metallurgical Engineering, Yildiz Technical University, İstanbul, 34210, Turkey; Baran, Y., Molecular Biology and Genetics, Faculty of Science, İzmir Institute of Technology, İzmir, 35430, Turkey; Dinçer İşoğlu, S., Department of Bioengineering, Faculty of Life and Natural Sciences, Abdullah Gül University, Kayseri, 38080, Turkey en_US
gdc.description.issue 1 en_US
gdc.description.publicationcategory Makale - Uluslararası Hakemli Dergi - Kurum Öğretim Elemanı en_US
gdc.description.scopusquality Q2
gdc.description.volume 22 en_US
gdc.description.wosquality Q2
gdc.identifier.openalex W3208306589
gdc.identifier.pmid 34708562
gdc.index.type Scopus
gdc.index.type PubMed
gdc.oaire.diamondjournal false
gdc.oaire.impulse 8.0
gdc.oaire.influence 2.9200242E-9
gdc.oaire.isgreen true
gdc.oaire.keywords Drug Carriers
gdc.oaire.keywords Drug Liberation
gdc.oaire.keywords Doxorubicin
gdc.oaire.keywords Humans
gdc.oaire.keywords Antineoplastic Agents
gdc.oaire.keywords Hydrogen-Ion Concentration
gdc.oaire.keywords Micelles
gdc.oaire.popularity 9.522182E-9
gdc.oaire.publicfunded false
gdc.oaire.sciencefields 02 engineering and technology
gdc.oaire.sciencefields 0210 nano-technology
gdc.openalex.collaboration National
gdc.openalex.fwci 1.12226792
gdc.openalex.normalizedpercentile 0.68
gdc.openalex.toppercent TOP 1%
gdc.opencitations.count 9
gdc.plumx.crossrefcites 7
gdc.plumx.mendeley 11
gdc.plumx.pubmedcites 5
gdc.plumx.scopuscites 13
gdc.scopus.citedcount 13
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relation.isOrgUnitOfPublication.latestForDiscovery 9af2b05f-28ac-4013-8abe-a4dfe192da5e

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