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dc.contributor.authorAleksiuk, Viktorija
dc.contributor.authorBaleišis, Justinas
dc.contributor.authorKirdaitė, Gailutė
dc.contributor.authorUzieliene, Ilona
dc.contributor.authorDenkovskij, Jaroslav
dc.contributor.authorBernotas, Paulius
dc.contributor.authorIvaškienė, Tatjana
dc.contributor.authorMobasheri, Ali
dc.contributor.authorBernotienė, Eiva
dc.date.accessioned2023-12-22T07:06:20Z
dc.date.available2023-12-22T07:06:20Z
dc.date.issued2023
dc.identifier.other(WOS_ID)001071315800001
dc.identifier.urihttps://etalpykla.vilniustech.lt/xmlui/handle/123456789/153654
dc.description.abstractOsteoarthritis (OA) ranks as the prevailing type of arthritis on a global scale, for which no effective treatments are currently available. Arterial hypertension is a common comorbidity in OA patients, and antihypertensive drugs, such as nifedipine (NIF), may affect the course of OA progression. The aim of this preclinical study was to determine the effect of nifedipine on healthy and OA cartilage, depending on its route of administration. In this study, we used the destabilization of medial meniscus to develop a mouse model of OA. Nifedipine was applied per os or intraarticularly (i.a.) for 8 weeks to both mice with OA and healthy animals. Serum biomarker concentrations were evaluated using the Luminex platform and alterations in the knee cartilage were graded according to OARSI histological scores and investigated immunohistochemically. Nifedipine treatment per os and i.a. exerted protective effects, as assessed by the OARSI histological scores. However, long-term nifedipine i.a. injections induced the deterioration of healthy cartilage. Lubricin, cartilage intermediate layer matrix protein (CILP), collagen type VI (COLVI), CILP, and Ki67 were upregulated by the nifedipine treatment. Serum biomarkers MMP-3, thrombospondin-4, and leptin were upregulated in the healthy groups treated with nifedipine, while only the levels of MMP-3 were significantly higher in the OA group treated with nifedipine per os compared to the untreated group. In conclusion, this study highlights the differential effects of nifedipine on cartilage integrity, depending on the route of administration and cartilage condition.eng
dc.formatPDF
dc.format.extentp. 1-22
dc.format.mediumtekstas / txt
dc.language.isoeng
dc.relation.isreferencedbyScience Citation Index Expanded (Web of Science)
dc.relation.isreferencedbyScopus
dc.source.urihttps://www.mdpi.com/2227-9059/11/9/2443
dc.titleEvaluation of cartilage integrity following administration of oral and intraarticular nifedipine in a murine model of osteoarthritis
dc.typeStraipsnis Web of Science DB / Article in Web of Science DB
dcterms.accessRightsThis article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https:// creativecommons.org/licenses/by/ 4.0/).
dcterms.licenseCreative Commons – Attribution – 4.0 International
dcterms.references60
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 Inovatyvios medicinos centras University of Oulu Université de Liège First Affiliated Hospital of Sun Yat-sen University
dc.subject.researchfieldN 010 - Biologija / Biology
dc.subject.researchfieldT 009 - Mechanikos inžinerija / Mechanical enginering
dc.subject.enosteoarthritis
dc.subject.enmouse
dc.subject.encartilage damage
dc.subject.enmeniscus
dc.subject.encalcium
dc.subject.enL-type channel blockers
dc.subject.ennifedipine
dc.subject.enbiomarkers
dcterms.sourcetitleBiomedicines: Biologics for Bone and Soft Tissue Regeneration: What Is New, What Is True
dc.description.issueiss. 9
dc.description.volumevol. 11
dc.publisher.nameMDPI
dc.publisher.cityBasel
dc.identifier.doi001071315800001
dc.identifier.doi152799544
dc.identifier.doi2-s2.0-85172802131
dc.identifier.doi85172802131
dc.identifier.doi1
dc.identifier.doi10.3390/biomedicines11092443
dc.identifier.elaba178705965


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