UKRAINIAN HEALTHCARE SCIENCE
Українська наука охорони здоров’я

Cell-free cryopreserved biological agents for cardiac protection in autoimmune myocarditis: a morphofunctional animal model study

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dc.contributor.author Гладких, Ф.В.
dc.contributor.author Лядова, Т.І.
dc.contributor.author Коморовський, Р.Р.
dc.date.accessioned 2025-05-01T10:04:01Z
dc.date.available 2025-05-01T10:04:01Z
dc.date.issued 2025-06-01
dc.identifier.citation Scripta Medica. 2025; 6(2):233–43. uk_UA
dc.identifier.uri https://doi.org/10.5937/scriptamed56-56858
dc.identifier.uri https://aseestant.ceon.rs/index.php/scriptamed/article/view/56858
dc.identifier.uri https://pubmed.com.ua/xmlui/handle/123456789/1149
dc.description Hladkykh FV, Liadova TI, Komorovsky RR. Cell-free cryopreserved biological agents for cardiac protection in autoimmune myocarditis: a morphofunctional animal model study. Scripta Medica. 2025; 6(2):233–43. DOI: https://doi.org/10.5937/scriptamed56-56858. Режим доступу: https://aseestant.ceon.rs/index.php/scriptamed/article/view/56858 uk_UA
dc.description.abstract Background/Aim: Autoimmune myocarditis (AIM) is a condition characterised by inflammation of the heart muscle, which can lead to heart failure. The development of effective treatments is crucial for improving cardiac function and recovery. Cell-free cryopreserved biological agents (CF-CBAs), including cell-free placenta extract (CEP), cell-free spleen extract (CES) and mesenchymal stem cell-conditioned medium (CM-MSC), have shown promise in preclinical models for their potential to improve heart function in autoimmune myocarditis. This study aimed to evaluate the efficacy of CEP, CES and CM-MSC in improving cardiac function and structure in a rat model of autoimmune myocarditis. Methods: CEP and CES were prepared through cryopreservation and water-salt extraction processes from placenta and spleen tissues, respectively. CM-MSC was obtained from umbilical mesenchymal stem cells cultured in serum-free medium. All biological agents were standardised for protein content and administered intramuscularly to rats with induced AIM. The rats were divided into six groups, with treatments administered on days 14, 17, 20, 23 and 26 of the experiment. Electrocardiogram (ECG) and echocardiographic studies were performed to assess heart function on day 28. Results: The administration of CEP, CES and CM-MSC significantly improved several echocardiographic parameters. Notably, CM-MSC treatment resulted in the most pronounced effects, including a 6.5 % reduction in the end-diastolic diameter of the left ventricle, a 103.4 % increase in ejection fraction, and a 57.3 % improvement in stroke volume. CEP and CES also improved heart function, but to a lesser extent. These treatments reduced left ventricular dilation, improved myocardial contractility and normalised heart wall thickness, with CM-MSC showing superior cardioprotective effects compared to CEP and CES. Conclusions: The study demonstrates that CEP, CES and CM-MSC have therapeutic potential for improving cardiac function in autoimmune myocarditis. CM-MSC was the most effective in reducing left ventricular dilation and enhancing cardiac output, suggesting its clinical potential for treating autoimmune myocarditis and other cardiovascular diseases. uk_UA
dc.language.iso en_US uk_UA
dc.subject Cardioprotection uk_UA
dc.subject Cryoextracts uk_UA
dc.subject Mesenchymal stem cells uk_UA
dc.title Cell-free cryopreserved biological agents for cardiac protection in autoimmune myocarditis: a morphofunctional animal model study uk_UA
dc.title.alternative Cell-free cryopreserved biological agents for cardiac protection in autoimmune myocarditis: a morphofunctional animal model study uk_UA
dc.type Article uk_UA


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