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http://dspace.zsmu.edu.ua/handle/123456789/23970
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| Название: | Impact of chronic social stress on molecular markers of skin regeneration during experimental excisional wounding |
| Авторы: | Makyeyeva, L. V. Belenichev, I. F. Aliyeva, O. H. Frolov, O. Petakh, P. Kamyshnyi, O. Макєєва, Людмила Валеріївна Бєленічев, Ігор Федорович Алієва, Олена Геннадіївна |
| Ключевые слова: | wound healing chronic social stress apoptosis transcription factors skin |
| Issue Date: | 2025 |
| Библиографическое описание: | Impact of chronic social stress on molecular markers of skin regeneration during experimental excisional wounding / L. Makyeyeva, I. Belenichev, O. Aliyeva, O. Frolov, P. Petakh, O. Kamyshnyi // Frontiers in Immunology. - 2025. - Vol. 16. - Art. 1656214. - https://doi.org/10.3389/fimmu.2025.1656214. |
| Аннотация: | Background: The second decade of the 21st century has seen increased
environmental stressors, global pandemics, and armed conflicts, all
contributing to heightened population morbidity and mortality. Among the
affected health outcomes, wound healing has emerged as a critical
physiological process vulnerable to impairment by psycho-emotional and
social stress. Chronic stress is known to delay tissue repair, disrupt
inflammatory responses, and exacerbate oxidative damage, yet the molecular
mechanisms linking social stress to impaired skin regeneration remain
insufficiently understood.
Methods: This study investigated the impact of chronic social stress (CSS) on
molecular pathways involved in apoptosis, cytoprotection, and proliferation
during skin wound healing in a rat model. A total of 120 male Wistar rats
were allocated into experimental (CSS-exposed), aggressor, and control
groups based on behavioral assessments. CSS was induced by combining
social isolation and continuous exposure to aggressive conspecifics for 21
days. Full-thickness excisional wounds were created, and skin samples were
collected during wounding and at days 1, 3, 7, 14, and 30 post-injury to
correspond with the inflammatory, proliferative, and remodeling phases of
healing. Immunohistochemical analyses were performed to assess the
expression of key markers: HIF1a, BCL2, caspase-3, caspase-9, NRF2, SOX2,
PDGFRB, CGRP, p62, and LC3BB. |
| URI: | http://dspace.zsmu.edu.ua/handle/123456789/23970 |
| Appears in Collections: | Наукові праці. (Фармакологія та МР) Наукові праці. (Гістологія, цитологія)
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