Does Aging Activate T-cells to Reduce Bone Mass and Quality?

IF 4.2 2区 医学 Q1 ENDOCRINOLOGY & METABOLISM Current Osteoporosis Reports Pub Date : 2022-10-01 DOI:10.1007/s11914-022-00745-8
Rajeev Aurora, Deborah Veis
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引用次数: 1

Abstract

Purpose of review: Aging leads to decline in bone mass and quality starting at age 30 in humans. All mammals undergo a basal age-dependent decline in bone mass. Osteoporosis is characterized by low bone mass and changes in bone microarchitecture that increases the risk of fracture. About a third of men over the age of 50 years are osteoporotic because they have higher than basal bone loss. In women, there is an additional acute decrement in bone mass, atop the basal rate, associated with loss of ovarian function (menopause) causing osteoporosis in about half of the women. Both genetics and environmental factors such as smoking, chronic infections, diet, microbiome, and metabolic disease can modulate basal age-dependent bone loss and eventual osteoporosis. Here, we review recent studies on the etiology of age-dependent decline in bone mass and propose a mechanism that integrates both genetic and environmental factors.

Recent findings: Recent findings support that aging and menopause dysregulate the immune system leading to sterile low-grade inflammation. Both animal models and human studies demonstrate that certain kinds of inflammation, in both men and women, mediate bone loss. Senolytics, meant to block a wide array of age-induced effects by preventing cellular senescence, have been shown to improve bone mass in aged mice. Based on a synthesis of the recent data, we propose that aging activates long-lived tissue resident memory T-cells to become senescent and proinflammatory, leading to bone loss. Targeting this population may represent a promising osteoporosis therapy. Emerging data indicates that there are several mechanisms that lead to sterile low-grade chronic inflammation, inflammaging, that cause age- and estrogen-loss dependent osteoporosis in men and women.

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衰老是否激活t细胞以减少骨量和骨质?
综述的目的:衰老导致人类从30岁开始骨量和质量下降。所有哺乳动物的骨量都会随着年龄的增长而下降。骨质疏松症的特点是骨量低,骨微结构改变,增加骨折的风险。大约三分之一的50岁以上的男性患有骨质疏松症,因为他们的骨质流失高于基础骨质流失。在女性中,骨量在基础率之上还有一个额外的急性减少,与卵巢功能丧失(更年期)有关,导致大约一半的女性骨质疏松症。遗传和环境因素,如吸烟、慢性感染、饮食、微生物群和代谢性疾病,都可以调节基础年龄依赖性骨质流失和最终的骨质疏松症。在这里,我们回顾了最近关于年龄依赖性骨量下降的病因学研究,并提出了一种整合遗传和环境因素的机制。最近的发现:最近的发现支持衰老和更年期失调的免疫系统导致无菌低度炎症。动物模型和人体研究都表明,在男性和女性中,某些类型的炎症都会介导骨质流失。抗衰老药物,即通过防止细胞衰老来阻止一系列由年龄引起的影响,已被证明可以改善老年小鼠的骨量。基于最近数据的综合,我们提出衰老激活长寿命的组织常驻记忆t细胞变得衰老和促炎,导致骨质流失。针对这一人群可能是一种很有前途的骨质疏松症治疗方法。新出现的数据表明,有几种机制导致无菌低级别慢性炎症,炎症,导致年龄和雌激素损失依赖性骨质疏松症的男性和女性。
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来源期刊
Current Osteoporosis Reports
Current Osteoporosis Reports Medicine-Endocrinology, Diabetes and Metabolism
CiteScore
8.80
自引率
2.30%
发文量
44
期刊介绍: This journal intends to provide clear, insightful, balanced contributions by international experts that review the most important, recently published clinical findings related to the diagnosis, treatment, management, and prevention of osteoporosis. We accomplish this aim by appointing international authorities to serve as Section Editors in key subject areas, such as current and future therapeutics, epidemiology and pathophysiology, and evaluation and management. Section Editors, in turn, select topics for which leading experts contribute comprehensive review articles that emphasize new developments and recently published papers of major importance, highlighted by annotated reference lists. An international Editorial Board reviews the annual table of contents, suggests articles of special interest to their country/region, and ensures that topics are current and include emerging research. Commentaries from well-known figures in the field are also provided.
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