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更深入地观察甲状旁腺激素和阿仑膦酸钠联合治疗对小梁骨的即时反应。

A closer look at the immediate trabecula response to combined parathyroid hormone and alendronate treatment.

机构信息

McKay Orthopaedic Research Laboratory, Department of Orthopaedic Surgery, Perelman School of Medicine, University of Pennsylvania, Philadelphia, PA, USA.

出版信息

Bone. 2014 Apr;61:149-57. doi: 10.1016/j.bone.2014.01.008. Epub 2014 Jan 24.

Abstract

Daily injections of parathyroid hormone (PTH) are the only FDA-approved anabolic treatment for osteoporosis; however PTH is only clinically approved for treatment periods of up to 24months. To enhance its anabolic effect, combining PTH with anti-resorptive therapy was proposed and expected to maximize the effectiveness of PTH. The current study aimed to elucidate structural mechanisms through which combination therapy can further improve bone strength over a limited treatment window of 12days, to more closely examine the early phase of the anabolic window. We examined 30 female rats treated with either vehicle (Veh), alendronate (ALN), PTH, or both PTH and ALN (PTH+ALN). Standard and individual trabecula segmentation (ITS)-based microstructural analyses were performed using in vivo micro-computed tomography. We found an increase in BV/TV in all treatments with the highest in the PTH+ALN group. Tb.Th* increased in both PTH and PTH+ALN groups well beyond that of the Veh or ALN group. SMI decreased in all treatments with PTH+ALN having the greatest tendency toward plate-like structures. ITS confirmed the trend toward more plate-like structures with increased plate Tb.N* and increased plate-to-rod ratio that was most pronounced in the PTH+ALN group. Using image-based finite element analysis, we demonstrated that stiffness increased in all treatment groups, again with the largest increase in the PTH+ALN group, indicating the resulting structural implications of increased plate-like structure. Static and dynamic bone histomorphometry and a serum resorption marker confirmed that PTH+ALN significantly increased bone formation activities and suppressed bone resorption activities. Overall the results indicate that PTH+ALN treatment has an additive effect due to a preferential increase in plate-like structures.

摘要

每日给予甲状旁腺激素(PTH)是唯一被 FDA 批准用于治疗骨质疏松症的合成代谢药物;然而,PTH 仅在临床治疗期不超过 24 个月时被批准使用。为了增强其合成代谢作用,提出了将 PTH 与抗吸收疗法联合使用的方法,并期望最大限度地提高 PTH 的有效性。本研究旨在阐明结构机制,通过联合治疗在有限的 12 天治疗窗口内进一步提高骨强度,更密切地研究合成代谢窗的早期阶段。我们检查了 30 只接受 vehicle(Veh)、阿伦膦酸钠(ALN)、PTH 或 PTH 和 ALN 联合治疗(PTH+ALN)的雌性大鼠。使用体内 micro-CT 进行标准和个体小梁分割(ITS)的微观结构分析。我们发现所有治疗组的 BV/TV 增加,其中 PTH+ALN 组增加最多。Tb.Th* 在 PTH 和 PTH+ALN 组中均增加,远远超过 Veh 或 ALN 组。SMI 在所有治疗组中均降低,而 PTH+ALN 组的板状结构倾向最大。ITS 证实了向更板状结构的趋势,板状 Tb.N*增加,板状/杆状比增加,在 PTH+ALN 组中最为明显。使用基于图像的有限元分析,我们证明了所有治疗组的刚度都增加了,PTH+ALN 组的增加最大,这表明增加板状结构的结构影响。静态和动态骨组织形态计量学以及血清吸收标志物证实,PTH+ALN 显著增加了骨形成活性并抑制了骨吸收活性。总的来说,结果表明 PTH+ALN 治疗具有协同作用,这是由于板状结构的优先增加。

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