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单次注射甲状旁腺激素可改善大鼠应力性骨折部位破骨细胞的改建参数。

Single injection of PTH improves osteoclastic parameters of remodeling at a stress fracture site in rats.

机构信息

School of Medical Sciences and Menzies Health Institute Queensland, Griffith University, Queensland, 4222, Australia.

School of Dentistry and Oral Health, Griffith University, Queensland, 4222, Australia.

出版信息

J Orthop Res. 2019 May;37(5):1172-1182. doi: 10.1002/jor.24262. Epub 2019 Mar 21.

Abstract

Stress fractures (SFx) result from repetitive cyclical loading of bone. They are frequent athletic injuries and underlie atypical femoral fractures following long-term bisphosphonate (BP) therapy. We investigated the effect of a single PTH injection on the healing of SFx in the rat ulna. SFx was induced in 120 female Wistar rats (300 ± 15 g) during a single loading session. A single PTH (8 µg.100g ) or vehicle (VEH) saline injection was administered 24 h after loading. Rats were divided into four groups (n = 15) and ulnae were examined 1, 2, 6, or 10 weeks following SFx. Two Toluidine Blue and TRAP-stained sections of the SFx were examined for histomorphometric analysis using Osteomeasure™ software. An increase in osteoclast number (N.Oc) and perimeter (Oc.Pm) was observed two weeks following PTH treatment (p < 0.01). At 6 weeks, bone formation was the main activity in BMUs. At 10 weeks, the proportion of healing along the SFx line remained 50% greater in PTH groups (p = 0.839), leading to a 43% reduction in the porosity area of BMU (p = 0.703). The main effect of time was a significant variable along the entire SFx remodeling cycle, with significant interactions between time and treatment type affecting (N.Oc) (p = 0.047) and (Oc.Pm) (p = 0.002). We conclude that a single PTH injection increases osteoclastogenesis by the second week of the remodeling cycle in a SFx in vivo. © 2019 Orthopaedic Research Society. Published by Wiley Periodicals, Inc. J Orthop Res.

摘要

应力性骨折(SFx)是由骨骼反复周期性受力引起的。它们是常见的运动损伤,也是长期双膦酸盐(BP)治疗后非典型股骨骨折的基础。我们研究了单次 PTH 注射对大鼠尺骨 SFx 愈合的影响。在单次加载过程中,120 只雌性 Wistar 大鼠(300±15g)中诱导 SFx。负荷后 24 小时给予单次 PTH(8μg.100g)或载体(VEH)生理盐水注射。将大鼠分为四组(n=15),并在 SFx 后 1、2、6 或 10 周检查尺骨。使用 Osteomeasure™软件对 SFx 的两个甲苯胺蓝和 TRAP 染色切片进行组织形态计量分析。PTH 治疗后两周观察到破骨细胞数量(N.Oc)和周长(Oc.Pm)增加(p<0.01)。6 周时,BMU 中的主要活动是骨形成。10 周时,PTH 组 SFx 线上的愈合比例仍增加 50%(p=0.839),导致 BMU 孔隙面积减少 43%(p=0.703)。时间的主要影响是整个 SFx 重塑周期的一个重要变量,时间和治疗类型之间的显著相互作用影响(N.Oc)(p=0.047)和(Oc.Pm)(p=0.002)。我们得出结论,单次 PTH 注射可在体内 SFx 重塑周期的第二周增加破骨细胞生成。©2019 矫形研究协会。由 Wiley Periodicals,Inc. 出版。J Orthop Res.

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