Unveiling frailty: comprehensive and sex-specific characterization in prematurely aging PolgA mice.

IF 3.3 Q2 GERIATRICS & GERONTOLOGY Frontiers in aging Pub Date : 2024-09-20 eCollection Date: 2024-01-01 DOI:10.3389/fragi.2024.1365716
Dilara Yılmaz, Amit Singh, Esther Wehrle, Gisela A Kuhn, Neashan Mathavan, Ralph Müller
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Abstract

Frailty, a geriatric syndrome, is assessed using the frailty phenotype (FP) and frailty index (FI). While these approaches have been applied to aging mice, their effectiveness in prematurely aging mouse models such as PolgAD257A/D257A (PolgA) has not been completely explored. We demonstrated that frailty became evident in PolgA mice around 40 weeks, validated through body weight loss, reduced walking speed, decreased physical activity, and weaker grip strength. Moreover, we also identified sex differences in these mice with females exhibiting slightly more physical decline compared to males. Frailty prevalence in PolgA mice at 40 weeks parallels that observed in naturally aging mice at 27 months and aging humans at 65-70 years. These findings contribute to understanding frailty onset and sex-specific patterns in this prematurely aging mouse model, emphasizing the significance of the PolgA mouse model in investigating aging and related disorders.

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揭示虚弱:早衰 PolgA 小鼠的全面性和性别特异性特征。
衰弱是一种老年综合症,可通过衰弱表型(FP)和衰弱指数(FI)进行评估。虽然这些方法已被应用于衰老小鼠,但它们在过早衰老小鼠模型(如 PolgAD257A/D257A(PolgA))中的有效性尚未得到全面探讨。我们发现,PolgA 小鼠在 40 周左右就会出现明显的虚弱现象,体重减轻、行走速度降低、体力活动减少以及握力减弱都证明了这一点。此外,我们还发现了这些小鼠的性别差异,与雄性小鼠相比,雌性小鼠的体力衰退程度略高。PolgA小鼠40周时的衰弱发生率与自然衰老小鼠27个月时的衰弱发生率以及衰老人类65-70岁时的衰弱发生率相似。这些发现有助于了解这种过早衰老小鼠模型的衰弱发生和性别特异性模式,强调了 PolgA 小鼠模型在研究衰老和相关疾病方面的重要性。
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