一种新的维生素D受体激动剂VS-105在绝经后骨质疏松大鼠模型中改善骨密度而不影响血清钙。

J Ruth Wu-Wong, Jerry L Wessale, Yung-Wu Chen, Theresa Chen, Maysaa Oubaidin, Phimon Atsawasuwan
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引用次数: 1

摘要

背景和目的:VS-105是一种新型维生素D受体激动剂,其高钙血症副作用明显小于骨化三醇,是研究非高钙血症剂量维生素D受体激动剂是否能改善骨密度(BMD)的有用工具。方法:在去卵巢骨质疏松大鼠模型和颅骨骨器官培养中评价VS-105和骨化三醇的作用。结果:OVX大鼠经VS-105(0.1、0.2或0.5 μg/kg,腹腔注射,3次/周,持续90天)治疗后,L3腰椎骨密度呈剂量依赖性显著改善(假手术vs. OVX/对照:324±14 vs. 279±10 mg/cm2;VS-105在0.1、0.2和0.5 μg/kg时分别为:306±9、329±12和327±10 mg/cm2),不影响血清钙(Ca)。0.1 μg/kg骨化三醇可显著提高骨密度,提高血清钙、VS-105含量;骨化三醇可显著抑制血清甲状旁腺激素分泌,促进胫骨生长。骨重塑生物标志物方面,骨化三醇和VS-105均显著升高血清骨钙素。在颅骨骨器官培养中,vs -105处理组的净钙释放量明显低于骨化三醇组。结论:VS-105在不影响血清钙的剂量范围内可有效改善OVX大鼠的骨密度;VS-105对骨密度的改善是由于成骨细胞活性的增加和破骨细胞骨吸收的减少。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A Novel Vitamin D Receptor Agonist, VS-105, Improves Bone Mineral Density without Affecting Serum Calcium in a Postmenopausal Osteoporosis Rat Model.

A Novel Vitamin D Receptor Agonist, VS-105, Improves Bone Mineral Density without Affecting Serum Calcium in a Postmenopausal Osteoporosis Rat Model.

Background and objectives: VS-105, a novel vitamin D receptor agonist with significantly less hypercalcemic side effects than calcitriol, is a useful tool to investigate whether or not a vitamin D receptor agonist at non-hypercalcemic doses could improve bone mineral density (BMD).

Methods: VS-105 and calcitriol were evaluated in an ovariectomized (OVX) osteoporosis rat model and in calvariae bone organ culture.

Results: Treatment of OVX rats by VS-105 (0.1, 0.2 or 0.5 μg/kg, intraperitoneal, 3×/week, for 90 days) significantly improved BMD in the L3 lumbar vertebra in a dose-dependent manner (sham vs. OVX/vehicle: 324 ± 14 vs. 279 ± 10 mg/cm2; VS-105 at 0.1, 0.2 and 0.5 μg/kg: 306 ± 9, 329 ± 12, and 327 ± 10 mg/cm2, respectively) without affecting serum calcium (Ca). Calcitriol at 0.1 μg/kg significantly increased BMD but it also increased serum Ca. VS-105 and calcitriol at the test doses significantly suppressed serum parathyroid hormone and promoted tibia bone growth. With respect to biomarkers of bone remodeling, calcitriol and VS-105 both significantly elevated serum osteocalcin. In the calvariae bone organ culture, net Ca release was significantly less in VS-105-treated groups (vs. calcitriol).

Conclusions: VS-105 is efficacious in improving BMD in a dose range that does not affect serum Ca in OVX rats; the improvement in BMD by VS-105 is attributable to increased osteoblastic activity and reduced osteoclastic bone resorption.

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