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Antiremodeling Agents Influence Osteoblast Activity Differently in Modeling and Remodeling Sites of Canine Rib

机译:抗重塑剂在犬肋骨的建模和重塑部位对成骨细胞活性的影响不同

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摘要

Antiremodeling agents reduce bone loss in part through direct actions on osteoclasts. Their effects on osteoblasts and bone formation activity are less clear and may differ at sites undergoing modeling vs. remodeling. Skeletally mature intact beagles, 1–2 years old at the start of the study, were treated daily with clinically relevant doses of alendronate (0.10 or 0.20 mg/kg), risedronate (0.05 or 0.10 mg/kg), raloxifene (0.50 mg/kg), or vehicle (1 mL/kg). Dynamic bone formation parameters were histologically assessed on periosteal, endocortical/trabecular, and intracortical bone envelopes of the rib. Raloxifene significantly increased periosteal surface mineral apposition rate (MAR), a measure of osteoblast activity, compared to all other treatments (+108 to +175%, P < 0.02), while having no significant effect on MAR at either the endocortical/trabecular or intracortical envelope. Alendronate (both 0.10 and 0.20 doses) and risedronate (only the 0.10 dose) significantly (P ≤ 0.05) suppressed MAR on the endocortical/trabecular envelope, while none of the bisphosphonate doses significantly altered MAR at either the periosteal or intracortical envelopes compared to vehicle. Based on these results, we conclude that (1) at clinically relevant doses the two classes of antiremodeling agents, bisphosphonates and selective estrogen receptor modulators, exert differential effects on osteoblast activity in the canine rib and (2) this effect depends on whether modeling or remodeling is the predominant mechanism of bone formation.
机译:抗重塑剂部分通过对破骨细胞的直接作用来减少骨质流失。它们对成骨细胞和骨形成活性的影响尚不清楚,并且在进行建模与重塑的部位可能有所不同。在研究开始时,骨骼成熟的完整小猎犬(1-2岁)每天接受临床相关剂量的阿仑膦酸盐(0.10或0.20 mg / kg),利塞膦酸盐(0.05或0.10 mg / kg),雷洛昔芬(0.50 mg / kg)或媒介物(1 mL / kg)。在肋骨的骨膜,皮质内/小梁和皮质内骨包膜上通过组织学评估动态骨形成参数。与所有其他治疗相比,雷洛昔芬显着提高了骨膜表面矿物质沉积率(MAR),这是成骨细胞活性的一种指标(+108至+ 175%,P <0.02),而在皮质内/小梁或皮下对MAR均无显着影响皮层内包膜。阿仑膦酸盐(0.10和0.20剂量)和利塞膦酸盐(仅0.10剂量)显着(P≤0.05)抑制了皮质/小梁包膜的MAR,而双膦酸酯剂量均未显着改变骨膜或皮质内包膜的MAR 。根据这些结果,我们得出结论:(1)在临床上相关剂量下,两类抗重塑剂,双膦酸盐和选择性雌激素受体调节剂,对犬肋骨成骨细胞的活性产生不同的作用,(2)这种作用取决于模型还是模型重塑是骨骼形成的主要机制。

著录项

  • 来源
    《Calcified Tissue International》 |2006年第4期|255-261|共7页
  • 作者单位

    Department of Anatomy and Cell Biology Indiana University School of Medicine;

    Department of Anatomy and Cell Biology Indiana University School of Medicine;

    Department of Anatomy and Cell Biology Indiana University School of Medicine;

    Department of Anatomy and Cell Biology Indiana University School of MedicineLilly Research Laboratories;

    Department of Anatomy and Cell Biology Indiana University School of MedicineDepartment of Orthopedic Surgery Indiana University School of MedicineDepartment of Biomedical Engineering Indiana University-Purdue University at Indianapolis;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    Bisphosphonate; Raloxifene; Alendronate; Risedronate; Periosteal;

    机译:双膦酸盐;雷洛昔芬;阿仑膦酸盐;利塞膦酸盐;骨膜;

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