Rodyti trumpą aprašą

dc.contributor.authorBironaitė, Daiva
dc.contributor.authorPetronienė, Jūratė Jolanta
dc.contributor.authorMiksiunas, Rokas
dc.contributor.authorZinovičius, Antanas
dc.contributor.authorMorkvėnaitė-Vilkončienė, Inga
dc.contributor.authorRamanavičius, Arūnas
dc.date.accessioned2023-09-18T16:39:37Z
dc.date.available2023-09-18T16:39:37Z
dc.date.issued2023
dc.identifier.issn0013-4686
dc.identifier.other(crossref_id)146927746
dc.identifier.urihttps://etalpykla.vilniustech.lt/handle/123456789/115581
dc.description.abstractIntroduction The human skeletal muscle-derived mesenchymal stem/stromal cells (SM-MSCs) possess myogenic differentiation potential and participate in the muscle regeneration process. However, the question of how to improve human skeletal muscle regeneration remains actual. In this study, the total SM-MSCs population was separated into subpopulations according to the neural cell adhesion molecule (NCAM, CD56), stimulated with an alternating electric field (AC) using scanning electrochemical microscopy (AC-SECM) and the intracellular redox changes, and myogenic differentiation markers were evaluated. Methods The total SM-MSC population was isolated from the postoperative human skeletal muscle biopsies by an enzymatic digestion method. The myogenic differentiation of the total SM-MSCs population before and after AC stimulation was evaluated immunohistochemically by the levels of desmin and myogenin. The effect of AC stimulation on the redox capacity of CD56(+) and CD56(-) cell subpopulations as well as on the level of myogenin on indium tin oxide (ITO) surface were also investigated. Results The total SM-MSCs population grown on a glass coverslip weakly responded to AC stimulus, i.e. the level of desmin was slightly increased by the 3rd day of differentiation, while in the not stimulated cells, it increased only by the 7th day. The level of myogenin did not change after AC stimulation. However, the CD56(+) and CD56(-) subpopulations had different redox activities and myogenic differentiation potential: the CD56(+) cells had stronger natural diffusion and were more redox active compared to the CD56(-) cells; the redox activity of CD56(+) cells was more actively stimulated by an alternating electric field than in CD56(-) cells; at control level, the CD56(+) cells had more myogenic differentiation-regulating transcription factor myogenin, which was more intensively stimulated by AC than in CD56(-) cells. Data show that the total population of human SM-MSCs is heterogeneous with different regenerating potential cells that do not equally respond to extracellular stimuli. The SECM can be used in both ways: (i) for extracellular stimulation and (ii) for the investigation of intracellular redox changes of the human SM-MSCs or their subpopulations allowing a deeper understanding of the mechanisms mediating skeletal tissue regeneration both in vitro and in vivo.eng
dc.formatPDF
dc.format.extentp. 1-9
dc.format.mediumtekstas / txt
dc.language.isoeng
dc.relation.isreferencedbyScience Citation Index Expanded (Web of Science)
dc.relation.isreferencedbyScopus
dc.relation.isreferencedbyScienceDirect
dc.source.urihttps://www.sciencedirect.com/science/article/pii/S0013468623005674
dc.titleScanning electrochemical microscopy for the stimulation and investigation of human skeletal muscle-derived mesenchymal stem/stromal cells
dc.typeStraipsnis Web of Science DB / Article in Web of Science DB
dcterms.references51
dc.type.pubtypeS1 - Straipsnis Web of Science DB / Web of Science DB article
dc.contributor.institutionValstybinis mokslinių tyrimų institutas Inovatyvios medicinos centras
dc.contributor.institutionValstybinis mokslinių tyrimų institutas Fizinių ir technologijos mokslų centras Vilniaus universitetas
dc.contributor.institutionState Research Institute Centre for Innovative Medicine
dc.contributor.institutionVilniaus Gedimino technikos universitetas
dc.contributor.institutionValstybinis mokslinių tyrimų institutas Fizinių ir technologijos mokslų centras Vilniaus Gedimino technikos universitetas
dc.contributor.facultyMechanikos fakultetas / Faculty of Mechanics
dc.subject.researchfieldN 003 - Chemija / Chemistry
dc.subject.enHuman skeletal muscle-derived mesenchymal stem/stromal cells (SM-MSCs)
dc.subject.enAlternating electric field based scanning electrochemical microscopy (AC-SECM)
dc.subject.enBioelectrochemistry
dc.subject.enCD56 receptor
dcterms.sourcetitleElectrochimica acta
dc.description.volumevol. 455
dc.publisher.nameElsevier BV
dc.publisher.cityOxford
dc.identifier.doi146927746
dc.identifier.doi1-s2.0-S0013468623005674
dc.identifier.doiS0013-4686(23)00567-4
dc.identifier.doi85153051149
dc.identifier.doi2-s2.0-85153051149
dc.identifier.doi0
dc.identifier.doiS0013468623005674
dc.identifier.doi000988630800001
dc.identifier.doi10.1016/j.electacta.2023.142389
dc.identifier.elaba163764286


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