Fracture Healing in the Setting of Endocrine Diseases, Aging, and Cellular Senescence.

IF 22 1区 医学 Q1 ENDOCRINOLOGY & METABOLISM
Dominik Saul, Sundeep Khosla
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引用次数: 12

Abstract

More than 2.1 million age-related fractures occur in the United States annually, resulting in an immense socioeconomic burden. Importantly, the age-related deterioration of bone structure is associated with impaired bone healing. Fracture healing is a dynamic process which can be divided into four stages. While the initial hematoma generates an inflammatory environment in which mesenchymal stem cells and macrophages orchestrate the framework for repair, angiogenesis and cartilage formation mark the second healing period. In the central region, endochondral ossification favors soft callus development while next to the fractured bony ends, intramembranous ossification directly forms woven bone. The third stage is characterized by removal and calcification of the endochondral cartilage. Finally, the chronic remodeling phase concludes the healing process. Impaired fracture healing due to aging is related to detrimental changes at the cellular level. Macrophages, osteocytes, and chondrocytes express markers of senescence, leading to reduced self-renewal and proliferative capacity. A prolonged phase of "inflammaging" results in an extended remodeling phase, characterized by a senescent microenvironment and deteriorating healing capacity. Although there is evidence that in the setting of injury, at least in some tissues, senescent cells may play a beneficial role in facilitating tissue repair, recent data demonstrate that clearing senescent cells enhances fracture repair. In this review, we summarize the physiological as well as pathological processes during fracture healing in endocrine disease and aging in order to establish a broad understanding of the biomechanical as well as molecular mechanisms involved in bone repair.

骨折愈合在内分泌疾病、衰老和细胞衰老的背景下。
美国每年发生超过210万例与年龄有关的骨折,造成了巨大的社会经济负担。重要的是,与年龄相关的骨结构退化与骨愈合受损有关。骨折愈合是一个动态过程,可分为四个阶段。最初的血肿产生炎症环境,其中间充质干细胞和巨噬细胞协调修复框架,血管生成和软骨形成标志着第二个愈合期。在中心区域,软骨内骨化有利于软骨痂的发育,而在骨折的骨端附近,膜内骨化直接形成编织骨。第三阶段的特征是软骨内软骨的移除和钙化。最后,慢性重塑阶段结束了愈合过程。老化导致的骨折愈合受损与细胞水平的有害变化有关。巨噬细胞、骨细胞和软骨细胞表达衰老标志物,导致自我更新和增殖能力降低。延长的“炎症”阶段导致延长的重塑阶段,其特征是微环境衰老和愈合能力恶化。尽管有证据表明,在损伤的情况下,至少在某些组织中,衰老细胞可能在促进组织修复中发挥有益作用,但最近的数据表明,清除衰老细胞可以增强骨折的修复。在这篇综述中,我们总结了在内分泌疾病和衰老中骨折愈合的生理和病理过程,以建立对骨修复中涉及的生物力学和分子机制的广泛理解。
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来源期刊
Endocrine reviews
Endocrine reviews 医学-内分泌学与代谢
CiteScore
42.00
自引率
1.00%
发文量
29
期刊介绍: Endocrine Reviews, published bimonthly, features concise timely reviews updating key mechanistic and clinical concepts, alongside comprehensive, authoritative articles covering both experimental and clinical endocrinology themes. The journal considers topics informing clinical practice based on emerging and established evidence from clinical research. It also reviews advances in endocrine science stemming from studies in cell biology, immunology, pharmacology, genetics, molecular biology, neuroscience, reproductive medicine, and pediatric endocrinology.
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