Understanding human aging and the fundamental cell signaling link in age-related diseases: the middle-aging hypovascularity hypoxia hypothesis.

IF 3.3 Q2 GERIATRICS & GERONTOLOGY
Frontiers in aging Pub Date : 2023-06-13 eCollection Date: 2023-01-01 DOI:10.3389/fragi.2023.1196648
Teow J Phua
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引用次数: 0

Abstract

Aging-related hypoxia, oxidative stress, and inflammation pathophysiology are closely associated with human age-related carcinogenesis and chronic diseases. However, the connection between hypoxia and hormonal cell signaling pathways is unclear, but such human age-related comorbid diseases do coincide with the middle-aging period of declining sex hormonal signaling. This scoping review evaluates the relevant interdisciplinary evidence to assess the systems biology of function, regulation, and homeostasis in order to discern and decipher the etiology of the connection between hypoxia and hormonal signaling in human age-related comorbid diseases. The hypothesis charts the accumulating evidence to support the development of a hypoxic milieu and oxidative stress-inflammation pathophysiology in middle-aged individuals, as well as the induction of amyloidosis, autophagy, and epithelial-to-mesenchymal transition in aging-related degeneration. Taken together, this new approach and strategy can provide the clarity of concepts and patterns to determine the causes of declining vascularity hemodynamics (blood flow) and physiological oxygenation perfusion (oxygen bioavailability) in relation to oxygen homeostasis and vascularity that cause hypoxia (hypovascularity hypoxia). The middle-aging hypovascularity hypoxia hypothesis could provide the mechanistic interface connecting the endocrine, nitric oxide, and oxygen homeostasis signaling that is closely linked to the progressive conditions of degenerative hypertrophy, atrophy, fibrosis, and neoplasm. An in-depth understanding of these intrinsic biological processes of the developing middle-aged hypoxia could provide potential new strategies for time-dependent therapies in maintaining healthspan for healthy lifestyle aging, medical cost savings, and health system sustainability.

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了解人类衰老和年龄相关疾病中的基本细胞信号传导联系:中年低血管缺氧假说。
衰老相关的缺氧、氧化应激和炎症病理生理学与人类年龄相关的致癌和慢性疾病密切相关。然而,低氧和激素细胞信号通路之间的联系尚不清楚,但这种与年龄相关的人类共病确实与性激素信号下降的中年期相吻合。这篇范围界定综述评估了相关的跨学科证据,以评估功能、调节和稳态的系统生物学,从而识别和破译人类年龄相关共病中缺氧和激素信号之间联系的病因。该假说描绘了越来越多的证据,支持中年人缺氧环境和氧化应激炎症病理生理学的发展,以及衰老相关变性中淀粉样变性、自噬和上皮-间质转化的诱导。总之,这种新的方法和策略可以提供清晰的概念和模式,以确定血管血流动力学(血流)和生理氧合灌注(氧生物利用度)下降的原因,与导致缺氧的氧稳态和血管性(低血管性缺氧)有关。中年低血管性缺氧假说可以提供连接内分泌、一氧化氮和氧稳态信号的机制接口,这与退行性肥大、萎缩、纤维化和肿瘤的进行性条件密切相关。深入了解中年缺氧的这些内在生物学过程,可以为维持健康寿命、健康生活方式衰老、医疗成本节约和卫生系统可持续性的时间依赖性疗法提供潜在的新策略。
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CiteScore
3.00
自引率
0.00%
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审稿时长
13 weeks
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