用甲状旁腺激素(1-84)对骨骼成熟的去卵巢恒河猴进行16个月的治疗,可增加骨形成和骨密度,并改善腰椎的小梁结构和生物力学性能。
Treatment of skeletally mature ovariectomized rhesus monkeys with PTH(1-84) for 16 months increases bone formation and density and improves trabecular architecture and biomechanical properties at the lumbar spine.
作者信息
Fox John, Miller Michael A, Newman Michael K, Turner Charles H, Recker Robert R, Smith Susan Y
机构信息
NPS Pharmaceuticals, Salt Lake City, Utah 84108, USA.
出版信息
J Bone Miner Res. 2007 Feb;22(2):260-73. doi: 10.1359/jbmr.061101.
UNLABELLED
Histomorphometric studies of treatments for osteoporosis in humans are restricted to iliac crest biopsies. We studied the effects of PTH(1-84) treatment at the lumbar spine of skeletally mature ovariectomized rhesus monkeys. PTH increased bone turnover, rapidly normalized BMD, and increased vertebral compressive strength. PTH increased trabecular bone volume primarily by increasing trabecular number by markedly increasing intratrabecular tunneling.
INTRODUCTION
Histomorphometric studies of the anabolic properties of PTH(1-84) (PTH) and related peptides in human bone are restricted to iliac crest biopsies. The ovariectomized (OVX) monkey is an accepted model of human postmenopausal bone loss and was used to study the effects of PTH treatment at clinically relevant skeletal sites.
MATERIALS AND METHODS
Skeletally mature rhesus monkeys were OVX or sham-operated and, after a bone depletion period of 9 months, treated daily for 16 months with PTH (5, 10, or 25 microg/kg). Markers of bone formation (serum osteocalcin) and resorption (urine N-telopeptide [NTX]) and lumbar spine BMD were measured throughout the study. Trabecular architecture and vertebral biomechanical properties were quantified at 16 months.
RESULTS
PTH treatment induced dose-dependent increases in bone turnover but did not increase serum calcium. Osteocalcin was significantly increased above OVX controls by 1 month. NTX was significantly elevated at 1 month with the highest dose, but not until 12 months with the 5 and 10 microg/kg doses. Lumbar spine BMD was 5% lower in OVX than in sham animals when treatment was started. All PTH doses increased BMD rapidly, with sham levels restored by 3-7 months with 10 and 25 microg/kg and by 16 months with 5 microg/kg. PTH treatment increased trabecular bone volume (BV/TV), primarily by increasing trabecular number, and dose-dependently increased bone formation rate (BFR) solely by increasing mineralizing surface. The largest effects on BV/TV and yield load occurred with the 10 microg/kg dose. The highest dose reduced trabecular thickness by markedly increasing intratrabecular tunneling.
CONCLUSIONS
PTH treatment of OVX rhesus monkeys increased bone turnover and increased BV/TV, BMD, and strength at the lumbar spine. All PTH doses were safe, but the 10 microg/kg dose was generally optimal, possibly because the highest dose resulted in too marked a stimulation of bone remodeling.
未标注
人体骨质疏松症治疗的组织形态计量学研究仅限于髂嵴活检。我们研究了甲状旁腺激素(1 - 84)[PTH(1 - 84)]治疗对骨骼成熟的去卵巢恒河猴腰椎的影响。PTH增加了骨转换,迅速使骨密度正常化,并提高了椎体抗压强度。PTH主要通过显著增加小梁内隧道形成从而增加小梁数量,进而增加了小梁骨体积。
引言
PTH(1 - 84)(PTH)及相关肽在人体骨骼中合成代谢特性的组织形态计量学研究仅限于髂嵴活检。去卵巢(OVX)猴是公认的人类绝经后骨质流失模型,用于研究PTH治疗在临床相关骨骼部位的效果。
材料与方法
将骨骼成熟的恒河猴进行去卵巢手术或假手术,在9个月的骨质流失期后,每天用PTH(5、10或25微克/千克)治疗16个月。在整个研究过程中测量骨形成标志物(血清骨钙素)和骨吸收标志物(尿N - 端肽[NTX])以及腰椎骨密度。在16个月时对小梁结构和椎体生物力学特性进行量化。
结果
PTH治疗引起骨转换呈剂量依赖性增加,但未增加血清钙。骨钙素在1个月时显著高于OVX对照组。最高剂量组在1个月时NTX显著升高,而5微克/千克和10微克/千克剂量组直到12个月时NTX才显著升高。开始治疗时,OVX组的腰椎骨密度比假手术动物低5%。所有PTH剂量均迅速增加骨密度,10微克/千克和25微克/千克剂量组在3 - 7个月时恢复到假手术组水平,5微克/千克剂量组在16个月时恢复到假手术组水平。PTH治疗增加了小梁骨体积(BV/TV),主要是通过增加小梁数量实现的,并且仅通过增加矿化表面剂量依赖性地增加了骨形成率(BFR)。对BV/TV和屈服载荷影响最大的是10微克/千克剂量。最高剂量通过显著增加小梁内隧道形成降低了小梁厚度。
结论
PTH治疗OVX恒河猴增加了骨转换,并增加了腰椎的BV/TV、骨密度和强度。所有PTH剂量都是安全的,但10微克/千克剂量通常是最佳的,可能是因为最高剂量导致对骨重塑的刺激过于明显。
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