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首页> 外文期刊>Journal of bone and mineral research: the official journal of the American Society for Bone and Mineral Research >1alpha-hydroxyvitamin D2 is less toxic but not bone selective relative to 1alpha-hydroxyvitamin D3 in ovariectomized rats.
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1alpha-hydroxyvitamin D2 is less toxic but not bone selective relative to 1alpha-hydroxyvitamin D3 in ovariectomized rats.

机译:在卵巢切除的大鼠中,相对于1α-羟基维生素D3,1α-羟基维生素D2毒性较小,但对骨骼没有选择性。

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摘要

Identification of bone selective vitamin D analogues would provide an interesting substance class for the treatment of osteoporosis. The synthetic prodrug 1alpha-hydroxyvitamin D2 [1alpha(OH)D2] has been shown to combine equal bone-preserving activity with distinctly reduced calcemic effects relative to 1alpha-hydroxyvitamin D3 [1alpha(OH)D3] in 3-month-old ovariectomized (OVX) rats. Therefore, 1alpha(OH)D2 may be a bone-selective compound. The aim of this study was to compare the bone protective and the calcemic activities of chronically administered 1alpha(OH)D2 and 1alpha(OH)D3 in 6-month-old OVX rats over a broad dose range from ineffective to toxic doses. Ninety-six female 6-month-old Fischer-344 rats were used for this experiment. Eighty rats were bilaterally OVX, 8 rats were sham-operated (SHAM), and 8 rats were killed at the time of surgery as a baseline control. Groups of OVX rats received vehicle alone (n = 16) or daily doses in the diet of 0.025, 0.05, 0.1, and 0.2 microg of 1alpha(OH)D2 or 1alpha(OH)D3 per kg body weight (BW) per day (n = 8 each). After calcein double-labeling, all animals were killed 3 months post-OVX. Orally administered 1alpha(OH)D2 was significantly less toxic compared with 1alpha(OH)D3 in terms of BW gain and kidney calcium content. The effects of 1alpha(OH)D2 and 1alpha(OH)D3 on serum calcium and urinary calcium excretion were generally similar at all doses in this study. Both 1alpha(OH)D2 and 1alpha(OH)D3 prevented the estrogen deficiency-induced bone loss in OVX rats, and induced profound bone anabolic effects at high dosages. 1alpha(OH)D3 and 1alpha(OH)D2 also dose-dependently increased total bone mineral density (BMD), cortical area, and cortical thickness in the tibial diaphysis of OVX rats. Bone resorption as assessed by osteoclast numbers (Oc.Ns) in vertebral cancellous bone and urinary excretion of deoxypyridinoline (DPD) was dose-dependently suppressed by 1alpha(OH)D2 and 1alpha(OH)D3. These data show that although 1alpha(OH)D2 was slightly but significantly less toxic compared with 1alpha(OH)D3, it did not have increased skeletal effects at any dose. Taken together, our findings argue against selective metabolic activation of 1alpha(OH)D2 in bone.
机译:骨选择性维生素D类似物的鉴定将为骨质疏松症的治疗提供有趣的物质类别。合成前药1α-羟基维生素D2 [1alpha(OH)D2]在3个月大的卵巢切除手术中,相对于1α-羟基维生素D3 [1alpha(OH)D3]具有相同的保骨活性和明显减少的钙减少作用。 OVX)大鼠。因此,1alpha(OH)D2可以是骨选择性化合物。这项研究的目的是比较从无效剂量到有毒剂量在6个月大的OVX大鼠中长期施用1alpha(OH)D2和1alpha(OH)D3的骨骼保护性和钙化活性。 96只雌性6个月大的Fischer-344大鼠用于该实验。将80只大鼠作为双侧OVX,对8只大鼠进行了假手术(SHAM),在手术时将8只大鼠处死作为基线对照。 OVX大鼠组单独接受媒介物(n = 16)或每天每公斤体重(BW)摄入0.025、0.05、0.1和0.2微克1alpha(OH)D2或1alpha(OH)D3( n = 8)。钙黄绿素双重标记后,OVX后3个月将所有动物处死。就体重增加和肾脏钙含量而言,口服1alpha(OH)D2的毒性明显低于1alpha(OH)D3。在本研究中,所有剂量下1alpha(OH)D2和1alpha(OH)D3对血清钙和尿钙排泄的影响通常相似。 1alpha(OH)D2和1alpha(OH)D3都可以防止雌激素缺乏引起的OVX大鼠骨丢失,并在高剂量时引起深刻的骨合成代谢作用。 1alpha(OH)D3和1alpha(OH)D2也剂量依赖性地增加了OVX大鼠胫骨干骨的总骨矿物质密度(BMD),皮质区域和皮质厚度。通过破骨细胞数(Oc.Ns)评估的椎骨松质骨吸收和脱氧吡啶并啉(DPD)的尿排泄被1alpha(OH)D2和1alpha(OH)D3剂量依赖性抑制。这些数据表明,尽管1alpha(OH)D2的毒性比1alpha(OH)D3略低,但毒性要低得多,但在任何剂量下其骨骼作用都没有增加。综上所述,我们的发现反对骨骼中1alpha(OH)D2的选择性代谢活化。

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