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髋关节骨折患者股骨头内新骨形成的芽与低骨细胞硬化素区同时出现。

Buds of new bone formation within the Femoral Head of Hip Fracture Patients Coincide with Zones of Low Osteocyte Sclerostin.

机构信息

Department of Medicine, University of Cambridge, Cambridge, UK.

Niigata Bone Science Institute, Niigata, Japan.

出版信息

J Bone Miner Res. 2023 Nov;38(11):1603-1611. doi: 10.1002/jbmr.4898. Epub 2023 Sep 29.

Abstract

Romosozumab treatment reduces the rate of hip fractures and increases hip bone density, increasing bone formation by inhibiting sclerostin protein. We studied the normal pattern of bone formation and osteocyte expression in the human proximal femur because it is relevant to both antisclerostin treatment effects and fracture. Having visualized and quantified buds of new bone formation in trabeculae, we hypothesized that they would coincide with areas of (a) higher mechanical stress and (b) low sclerostin expression by osteocytes. In patients with hip fracture, we visualized each bud of active modeling-based formation (forming minimodeling structure [FMiS]) in trabecular cores taken from different parts of the femoral head. Trabecular bone structure was also measured with high-resolution imaging. More buds of new bone formation (by volume) were present in the higher stress superomedial zone (FMiS density, N.FMiS/T.Ar) than lower stress superolateral (p < 0.05), and inferomedial (p < 0.001) regions. There were fewer sclerostin expressing osteocytes close to or within FMiS. FMiS density correlated with greater amount, thickness, number, and connectivity of trabeculae (bone volume BV/TV, r = 0.65, p < 0.0001; bone surface BS/TV, r = 0.47, p < 0.01; trabecular thickness Tb.Th, r = 0.55, p < 0.001; trabecular number Tb.N, r = 0.47, p < 0.01; and connectivity density Conn.D, r = 0.40, p < 0.05) and lower trabecular separation (Tb.Sp, r = -0.56, p < 0.001). These results demonstrate modeling-based bone formation in femoral trabeculae from patients with hip fracture as a potential therapeutic target to enhance bone structure. © 2023 American Society for Bone and Mineral Research (ASBMR).

摘要

罗莫佐单抗治疗可降低髋部骨折发生率并增加髋部骨密度,通过抑制硬骨素蛋白增加骨形成。我们研究了人近端股骨的正常骨形成和骨细胞表达模式,因为这与抗硬骨素治疗效果和骨折都有关。我们已经可视化和量化了骨小梁中新骨形成的芽,假设它们将与(a)较高机械应力和(b)骨细胞中低硬骨素表达的区域重合。在髋部骨折患者中,我们在取自股骨头不同部位的骨小梁核心中可视化了每个活跃基于模型形成的新骨形成芽(形成最小模型结构 [FMiS])。还使用高分辨率成像测量了骨小梁的结构。在较高的机械应力的Superomedial 区(FMiS 密度,N.FMiS/T.Ar)中存在更多的新骨形成芽(按体积计)(p < 0.05),而在较低的机械应力的Superolateral 区(p < 0.05)和 Inferomedial 区(p < 0.001)中则较少。靠近或在 FMiS 内的硬骨素表达骨细胞较少。FMiS 密度与小梁的更多数量、厚度、数量和连接性相关(骨体积 BV/TV,r = 0.65,p < 0.0001;骨表面 BS/TV,r = 0.47,p < 0.01;骨小梁厚度 Tb.Th,r = 0.55,p < 0.001;骨小梁数量 Tb.N,r = 0.47,p < 0.01;和连接密度 Conn.D,r = 0.40,p < 0.05)以及较低的骨小梁分离(Tb.Sp,r = -0.56,p < 0.001)。这些结果表明,从髋部骨折患者的股骨小梁中观察到基于模型的骨形成是增强骨结构的潜在治疗靶点。 © 2023 美国骨矿研究学会(ASBMR)。

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