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氟化物的药代动力学以及腰椎和髋部骨矿物质密度的变化

Fluoride pharmacokinetics and changes in lumbar spine and hip bone mineral density.

作者信息

Patel S, Chan J K, Hosking D J

机构信息

Medical Research Centre, City Hospital, Nottingham, UK.

出版信息

Bone. 1996 Dec;19(6):651-5. doi: 10.1016/s8756-3282(96)00262-1.

DOI:10.1016/s8756-3282(96)00262-1
PMID:8968033
Abstract

Debate about the use of fluoride for the treatment of vertebral osteoporosis has centered not only on whether fluoride treatment decreases vertebral fractures, but also the interindividual vertebral bone mineral density (BMD) response, the potential for nonvertebral fractures, as well as side effects and tolerability. These effects may be dose dependent and, in this study, we examine the pharmacokinetics of sodium monofluorophosphate (MFP) in osteoporotic patients and relate this to changes in BMD. Plasma fluoride absorption curves were measured from 0 to 6 h after ingestion of MFP at baseline and during long-term dosing in 21 patients with vertebral osteoporosis (T scores < or = 2). BMD was measured at baseline and at 12 months at the lumbar spine (LS), femoral neck (FN), trochanter, and Ward's triangle. We found that fluoride elimination was inversely related to creatinine clearance. LS BMD increased from a median of 0.77 g/cm2 (range 0.69 to 0.99) at baseline to 0.88 g/cm2 (0.75 to 1.13) (p < 0.001) after 12 months. This equates to a median increase of 12% (range -1.2 to 37). Median femoral neck BMD decreased from 0.75 g/cm2 (0.62 to 0.94) at baseline to 0.69 g/cm2 (0.62 to 0.92) (p = 0.13) after 12 months. This equates to a decrease of -2% (-19 to 10). BMD at the other hip sites also decreased slightly. Changes in LS and FN BMD were not significantly related (r = 0.28, p = 0.29). The various pharmacokinetic parameters measured were not related to changes in LS BMD; however, there was an inverse relationship between trough fluoride concentration during long-term dosing and change in FN BMD. Further studies are required to see if this relationship can be used to monitor osteoporotic patients treated with fluoride and prevent significant decreases in FN BMD and possibly fractures at this site.

摘要

关于使用氟化物治疗椎体骨质疏松症的争论不仅集中在氟化物治疗是否能减少椎体骨折,还包括个体间椎体骨密度(BMD)反应、非椎体骨折的可能性以及副作用和耐受性。这些影响可能取决于剂量,在本研究中,我们检测了骨质疏松症患者中一氟磷酸钠(MFP)的药代动力学,并将其与骨密度变化相关联。在21例椎体骨质疏松症患者(T值≤2)中,于基线期及长期给药期间,测量摄入MFP后0至6小时的血浆氟吸收曲线。在基线期及12个月时,测量腰椎(LS)、股骨颈(FN)、大转子和沃德三角区的骨密度。我们发现氟消除与肌酐清除率呈负相关。腰椎骨密度从基线期的中位数0.77g/cm²(范围0.69至0.99)增加到12个月后的0.88g/cm²(0.75至1.13)(p<0.001)。这相当于中位数增加了12%(范围-1.2至37)。股骨颈骨密度中位数从基线期的0.75g/cm²(0.62至0.94)降至12个月后的0.69g/cm²(0.62至0.92)(p = 0.13)。这相当于下降了-2%(-19至10)。其他髋部部位的骨密度也略有下降。腰椎和股骨颈骨密度的变化无显著相关性(r = 0.28,p = 0.29)。所测量的各种药代动力学参数与腰椎骨密度变化无关;然而,长期给药期间的氟谷浓度与股骨颈骨密度变化之间存在负相关。需要进一步研究以确定这种关系是否可用于监测接受氟化物治疗的骨质疏松症患者,并预防股骨颈骨密度显著下降以及该部位可能发生的骨折。

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