首页> 外文期刊>The Journal of toxicological sciences >Effect of dosing frequency of teriparatide (PTH 1-34) on bone formation in rats: comparison of bone metabolism marker levels
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Effect of dosing frequency of teriparatide (PTH 1-34) on bone formation in rats: comparison of bone metabolism marker levels

机译:Teriparidide(第1-34)萜烯酮(第1-34页)对大鼠骨形成的影响:骨代谢标志水平的比较

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摘要

Teriparatide, a drug used in the treatment of osteoporosis, was administered to rats subcutaneously for the duration of 3 months, at a frequency of either once weekly or once daily to demonstrate the varying levels of anabolic action the drug can have on bone depending on the dosing frequency. The levels of biomarkers in the blood were compared and found to vary in osteocalcin (OC), a biomarker of bone formation, and cross-linked N-telopeptide of type 1 collagen (NTx), a biomarker of bone resorption, according to the dosing frequency. In the once-weekly regimen, teriparatide did not affect NTx levels at any of the doses studied, while OC levels increased with dose, peaking at 72 hr, then returning to normal before the next injection (after 1 week). Bone mineral density (BMD) levels increased moderately with no difference between doses. This was thought to result from the steady state achieved following increases in bone formation and bone absorption. In the once-daily dosing regimen, meanwhile, NTx levels increased with dose, and OC levels were markedly higher when compared to those with the once weekly dosing. BMD levels were higher than those with the once-weekly dosing, but with no difference between doses. This was considered a result of unlimited, excessive increases in bone formation due to daily administration of the drug. These results suggest that teriparatide promotes normal bone metabolism ("stationary mini-modeling") when administered once weekly, and has an anabolic action with high metabolic turnover ("high-turnover remodeling") when administered once daily.
机译:用于治疗骨质疏松症的药物,在皮下给予大鼠3个月的大鼠,以每周一次或一次每天一次,以证明药物可能在骨骼上具有不同程度的骨骼的频率。给药频率。比较血液中的生物标志物水平,发现在骨癌(OC)中变化,骨形成的生物标志物,并根据剂量的1型胶原蛋白(NTX)的交联N-腹膜肽(NTX),骨吸收的生物标志物频率。在一次每周一次的方案中,Teriparatide没有影响所研究的任何剂量的NTX水平,而OC水平随剂量增加,72小时达到峰值,然后在下一次注射之前返回正常(1周后)。骨矿物密度(BMD)水平适度增加,剂量之间没有差异。这被认为是由于骨形成和骨骼吸收增加所达到的稳态。同时,与每周给药一次的人相比,在曾经每日给药方案中,NTX水平随剂量增加,OC水平明显高。 BMD水平高于每周给药的水平,但剂量之间没有差异。这被认为是无限的,由于每日药物施用导致的骨形成的过度增加。这些结果表明,在每周施用一次时,TeripaRide促进正常骨代谢(“固定式迷你型”),并且在每日施用一次时具有高代谢转换(“高端转换重塑”)的合成代谢作用。

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