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dc.contributor.authorTemnik, M.-
dc.contributor.authorRudyk, M.-
dc.contributor.authorBalakin, A.-
dc.contributor.authorGurin, S.-
dc.contributor.authorDovbynchuk, T.-
dc.contributor.authorByshovets, R.-
dc.contributor.authorDzubenko, N.-
dc.contributor.authorTolstanova, G.-
dc.contributor.authorSkivka, L.-
dc.date.accessioned2026-02-27T08:08:11Z-
dc.date.available2026-02-27T08:08:11Z-
dc.date.issued2025-
dc.identifier.issnhttps://doi.org/10.1038/s41598-025-97830-6-
dc.identifier.urihttp://ir.librarynmu.com/handle/123456789/18146-
dc.description.abstractAlzheimer disease (AD) is a debilitating progressive dementia, whose pathophysiology is not fully understood. Chronic inflammation is now widely accepted as one of the key features of AD pathogenesis. Because of this, anti-inflammatory preparations are considered as putative disease modifying agents. A new compound of zinc aspartate with enriched light atoms 64Zn (64Zn-asp) was evaluated as a possible anti-AD agent using Aβ1-40-induced AD model. Intrahippocampal Aβ1-40 injection resulted in pronounced neuroinflammation, as was evidenced by increased phagocytic activity, augmented reactive oxygen species generation, and up-regulated CD86 and CD206 expression by microglia. In rats with Aβ1-40-induced AD, persistent systemic inflammation was also registered, as was ascertained by signifcantly increased white blood cell-based inflammatory indices and development of anemia of inflammation. Neuro- and systemic inflammation in rats was accompanied by hippocampal dopamine neuron loss, as well as by impairment of short-term and remote spatial memory and cognitive flexibility. Intravenous 64Zn-asp administration rats with AD was associated with returning all microglia indicators to normal range. All aforementioned features of systemic inflammation were not observed in these animals. Anti-inflammatory 64Zn-asp effect was strongly correlated with improvement of short-term spatial memory and cognitive flexibility, and moderately—with betterment of remote spatial memory. These results demonstrated that i.v. 64Zn-asp administration could reverse the inflammatory and, as a result, cognitive effects of intra-hippocampal Aβ1-40 in rats. Therefore, its use may be a viable approach in the complex therapeutic strategy for AD.uk_UA
dc.language.isoenuk_UA
dc.publisherScientifc Reportsuk_UA
dc.subjectAlzheimer disease, Stable light isotope enriched zinc aspartate, Anti-inflammatory agent, Inflammation, Neuroinflammation, Cognitive improvementuk_UA
dc.titleAnti-inflammatory effects of 64Zn-aspartate is accompanied by cognitive improvements in rats with Aβ1-40-induced alzheimer diseaseuk_UA
dc.typeArticleuk_UA
Розташовується у зібраннях:Наукові публікації кафедри внутрішньої медицини стоматологічного факультету

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