- 作者:Davide Gatti Davide.Gatti@univr.it ; Ombretta Viapiana Ombretta.Viapiana@univr.it ; Silvano Adami ; Silvano.Adami@univr.it ; Luca Idolazzi Luca.Idolazzi@yahoo.it ; Elena Fracassi Elena.Fracassi@univr.it ; Maurizio Rossini Maurizio.Rossini@univr.it
- 关键词:Sclerostin ; Bone turnover markers ; Bisphosphonates ; Osteoporosis ; Menopause
- 刊名:Bone
- 出版年:2012
- 出版时间:March 2012
- 年:2012
- 卷:50
- 期:3
- 页码:739-742
- 全文大小:316 K
This is an ancillary observation from patients participating in a 12 months, phase 2, randomized clinical trial. We analyzed 107 patients given either monthly intramuscular neridronate (12.5, 25 or 50 mg) or placebo.
Serum C-terminal telopeptide of type I collagen (sCTX, a bone-resorption marker) decreased by 61 % , 75 % and 73 % in the 12.5, 25 and 50 mg dose groups, respectively.
Mean changes in bone alkaline phosphatase (bAP) at 12 months were ?#xA0;47 % , ?#xA0;60.0 % and ?#xA0;52.6 % in the groups receiving 12.5, 25 or 50 mg neridronate, respectively. Serum DKK1 remained unchanged at all time points in the 3 groups. Serum sclerostin increased versus placebo group gradually and significantly only in patients treated with 25 or 50 mg neridronate monthly, reaching 138-148 % of baseline values (P < 0.001). Changes in serum sclerostin at 12 months were negatively correlated with changes in bAP (P < 0.001) even when data were adjusted for sCTX changes and only treated patients were included.
In conclusions, decreased bone formation after several months of bisphosphonate therapy is associated with increased serum levels of sclerostin. This might suggest that Wnt signaling may play a role in the coupling between resorption and formation.