Endothelial IGF- 1R deficiency disrupts microvascular homeostasis, impairing skeletal muscle perfusion and endurance: implications for age-related sarcopenia

IF 5.4 2区 医学 Q1 GERIATRICS & GERONTOLOGY GeroScience Pub Date : 2025-04-08 DOI:10.1007/s11357-025-01653-2
Adam Nyul-Toth, Santny Shanmugarama, Roland Patai, Rafal Gulej, Janet Faakye, Dorina Nagy, Mark Nagykaldi, Tamas Kiss, Tamas Csipo, Madison Milan, Shoba Ekambaram, Sharon Negri, Raghavendra Y. Nagaraja, Anna Csiszar, Jacob L. Brown, Holly Van Remmen, Anna Ungvari, Andriy Yabluchanskiy, Stefano Tarantini, Zoltan Ungvari
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Abstract

Aging is associated with a progressive decline in circulating insulin-like growth factor- 1 (IGF- 1) levels in humans, which has been implicated in the pathogenesis of sarcopenia. IGF- 1 is an anabolic hormone that plays a dual role in maintaining skeletal muscle health, acting both directly on muscle fibers to promote growth and indirectly by supporting the vascular network that sustains muscle perfusion. However, the microvascular consequences of IGF- 1 deficiency in aging muscle remain poorly understood. To elucidate how impaired IGF- 1 input affects skeletal muscle vasculature, we examined the effects of endothelial-specific IGF- 1 receptor (IGF- 1R) deficiency using a mouse model of endothelial IGF- 1R knockdown (VE-Cadherin-CreERT2/Igf1rf/f mice). These mice exhibited significantly reduced skeletal muscle endurance and attenuated hyperemic response to acetylcholine, an endothelium-dependent vasodilator. Additionally, they displayed microvascular rarefaction and impaired nitric oxide-dependent vasorelaxation, indicating a significant decline in microvascular health in skeletal muscle. These findings suggest that endothelial IGF- 1R signaling is critical for maintaining microvascular integrity, muscle perfusion, and function. Impaired IGF- 1 input to the microvascular endothelium may contribute to reduced muscle blood flow and exacerbate age-related sarcopenia. Enhancing vascular health by modulating IGF- 1 signaling could represent a potential therapeutic strategy to counteract age-related muscle decline.

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内皮 IGF- 1R 缺乏会破坏微血管平衡,损害骨骼肌灌注和耐力:对老年性肌肉疏松症的影响
衰老与人类循环胰岛素样生长因子- 1 (IGF- 1)水平的逐渐下降有关,这与肌肉减少症的发病机制有关。IGF- 1是一种合成代谢激素,在维持骨骼肌健康方面起双重作用,既直接作用于肌纤维促进生长,又间接作用于维持肌肉灌注的血管网络。然而,IGF- 1缺乏对衰老肌肉微血管的影响仍然知之甚少。为了阐明IGF- 1输入受损如何影响骨骼肌血管系统,我们使用内皮IGF- 1R敲低的小鼠模型(VE-Cadherin-CreERT2/Igf1rf/f小鼠)检测了内皮特异性IGF- 1受体(IGF- 1R)缺乏的影响。这些小鼠对乙酰胆碱(一种内皮依赖性血管扩张剂)表现出明显降低的骨骼肌耐力和减弱的充血反应。此外,他们表现出微血管稀疏和一氧化氮依赖性血管松弛受损,表明骨骼肌微血管健康显著下降。这些发现表明,内皮细胞IGF- 1R信号对于维持微血管完整性、肌肉灌注和功能至关重要。微血管内皮的IGF- 1输入受损可能导致肌肉血流量减少,加剧与年龄相关的肌肉减少症。通过调节IGF- 1信号来增强血管健康可能是一种潜在的治疗策略,可以对抗与年龄相关的肌肉衰退。
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来源期刊
GeroScience
GeroScience Medicine-Complementary and Alternative Medicine
CiteScore
10.50
自引率
5.40%
发文量
182
期刊介绍: GeroScience is a bi-monthly, international, peer-reviewed journal that publishes articles related to research in the biology of aging and research on biomedical applications that impact aging. The scope of articles to be considered include evolutionary biology, biophysics, genetics, genomics, proteomics, molecular biology, cell biology, biochemistry, endocrinology, immunology, physiology, pharmacology, neuroscience, and psychology.
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