骨细胞
骨重建
皮质骨
1型糖尿病
内分泌学
内科学
硬骨素
医学
骨细胞
成骨细胞
糖尿病
病理
生物
细胞生物学
信号转导
体外
生物化学
Wnt信号通路
作者
Sofie Kolibova,Eva Maria Wölfel,Haniyeh Hemmatian,Petar Milovanović,Herbert Mushumba,Birgit Wulff,Maximilian Neidhardt,Klaus Püschel,Antonio Virgilio Failla,Annegreet G. Veldhuis‐Vlug,Alexander Schlaefer,Benjamin Ondruschka,Michael Amling,Lorenz C. Hofbauer,Martina Rauner,Björn Busse,Katharina Jähn
标识
DOI:10.1016/j.actbio.2023.02.037
摘要
Bone fragility is a profound complication of type 1 diabetes mellitus (T1DM), increasing patient morbidity. Within the mineralized bone matrix, osteocytes build a mechanosensitive network that orchestrates bone remodeling; thus, osteocyte viability is crucial for maintaining bone homeostasis. In human cortical bone specimens from individuals with T1DM, we found signs of accelerated osteocyte apoptosis and local mineralization of osteocyte lacunae (micropetrosis) compared with samples from age-matched controls. Such morphological changes were seen in the relatively young osteonal bone matrix on the periosteal side, and micropetrosis coincided with microdamage accumulation, implying that T1DM drives local skeletal aging and thereby impairs the biomechanical competence of the bone tissue. The consequent dysfunction of the osteocyte network hampers bone remodeling and decreases bone repair mechanisms, potentially contributing to the enhanced fracture risk seen in individuals with T1DM. STATEMENT OF SIGNIFICANCE: Type 1 diabetes mellitus (T1DM) is a chronic autoimmune disease that causes hyperglycemia. Increased bone fragility is one of the complications associated with T1DM. Our latest study on T1DM-affected human cortical bone identified the viability of osteocytes, the primary bone cells, as a potentially critical factor in T1DM-bone disease. We linked T1DM with increased osteocyte apoptosis and local accumulation of mineralized lacunar spaces and microdamage. Such structural changes in bone tissue suggest that T1DM speeds up the adverse effects of aging, leading to the premature death of osteocytes and potentially contributing to diabetes-related bone fragility.
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