Gutteridge D H, Stewart G O, Prince R L, Price R I, Retallack R W, Dhaliwal S S, Stuckey B G A, Drury P, Jones C E, Faulkner D L, Kent G N, Bhagat C I, Nicholson G C, Jamrozik K
Department of Endocrinology, Sir Charles Gairdner Hospital, Nedlands, WA, Australia.
Osteoporos Int. 2002;13(2):158-70. doi: 10.1007/s001980200008.
Postmenopausal Caucasian women aged less than 80 years (n = 99) with one or more atraumatic vertebral fracture and no hip fractures, were treated by cyclical administration of enteric coated sodium fluoride (NaF) or no NaF for 27 months, with precautions to prevent excessive stimulation of bone turnover. In the first study 65 women, unexposed to estrogen (-E study), age 70.8 +/- 0.8 years (mean +/- SEM) were all treated with calcium (Ca) 1.0-1.2 g daily and ergocalciferol (D) 0.25 mg per 25 kg once weekly and were randomly assigned to cyclical NaF (6 months on, 3 months off, initial dose 60 mg/day; group F CaD, n = 34) or no NaF (group CaD, n = 31). In the second study 34 patients, age 65.5 +/- 1.2 years, on hormone replacement therapy (E) at baseline, had this standardized, and were all treated with Ca and D and similarly randomized (FE CaD, n = 17; E CaD, n = 17) (+E study). The patients were stratified according to E status and subsequently assigned randomly to +/- NaF. Seventy-five patients completed the trial. Both groups treated with NaF showed an increase in lumbar spinal density (by DXA) above baseline by 27 months: FE CaD + 16.2% and F CaD +9.3% (both p = 0.0001). In neither group CaD nor E CaD did lumbar spinal density increase. Peripheral bone loss occurred at most sites in the F CaD group at 27 months: tibia/fibula shaft -7.3% (p = 0.005); femoral shaft -7.1% (p = 0.004); distal forearm -4.0% (p=0.004); total hip -4.1% (p = 0.003); and femoral neck -3.5% (p = 0.006). No significant loss occurred in group FE CaD. Differences between the two NaF groups were greatest at the total hip at 27 months but were not significant [p < 0.05; in view of the multiple bone mineral density (BMD) sites, an alpha of 0.01 was employed to denote significance in BMD changes throughout this paper]. Using Cox's proportional hazards model, in the -E study there were significantly more patients with first fresh vertebral fractures in those treated with NaF than in those not so treated (RR = 24.2, p = 0.008, 95% CI 2.3-255). Patients developing first fresh fractures in the first 9 months were markedly different between groups: -23% of F CaD, 0 of CaD, 29% of FE CaD and 0 of E CaD. The incidence of incomplete (stress) fractures was similar in the two NaF-treated groups. Complete nonvertebral fractures did not occur in the two +E groups; there were no differences between groups F CaD and CaD. Baseline BMD (spine and femoral neck) was related to incident vertebral fractures in the control groups (no NaF), but not in the two NaF groups. Our results and a literature review indicate that fluoride salts, if used, should be at low dosage, with pretreatment and co-treatment with a bone resorption inhibitor.
年龄小于80岁的绝经后白种女性(n = 99),有一处或多处非创伤性椎体骨折且无髋部骨折,接受肠溶氟化钠(NaF)周期性给药或不使用NaF治疗27个月,并采取预防措施防止过度刺激骨转换。在第一项研究中,65名未接受雌激素治疗的女性(-E研究),年龄70.8±0.8岁(均值±标准误),均每日服用1.0 - 1.2 g钙(Ca)和每25 kg体重每周一次服用0.25 mg麦角钙化醇(D),并随机分为周期性NaF组(服用6个月,停用3个月,初始剂量60 mg/天;F CaD组,n = 34)或不使用NaF组(CaD组,n = 31)。在第二项研究中,34名患者,年龄65.5±1.2岁,基线时接受激素替代治疗(E),进行了标准化处理,均接受Ca和D治疗并同样随机分组(FE CaD组,n = 17;E CaD组,n = 17)(+E研究)。患者根据E状态分层,随后随机分为±NaF组。75名患者完成了试验。两个接受NaF治疗的组在27个月时腰椎骨密度(通过双能X线吸收法测定)均较基线有所增加:FE CaD组增加16.2%,F CaD组增加9.3%(均p = 0.00<span style="font-family: Arial, sans-serif;">01)。CaD组和E CaD组腰椎骨密度均未增加。在27个月时,F CaD组大多数部位出现外周骨量丢失:胫骨干/腓骨干 -7.3%(p = 0.005);股骨干 -7.1%(p = 0.004);前臂远端 -4.0%(p = 0.004);全髋 -4.1%(p = 0.003);股骨颈 -3.5%(p = 0.006)。FE CaD组未出现明显骨量丢失。两个NaF组之间的差异在27个月时全髋处最大,但无统计学意义[p<0.05;鉴于多个骨矿物质密度(BMD)测量部位,本文采用α = 0.01来表示BMD变化具有统计学意义]。使用Cox比例风险模型,在-E研究中,接受NaF治疗的患者首次发生新鲜椎体骨折的人数显著多于未接受NaF治疗的患者(风险比 = 24.2,p = 0.008,95%可信区间2.3 - 255)。在最初9个月内发生首次新鲜骨折的患者在组间有显著差异:F CaD组为23%,CaD组为0,FE CaD组为29%,E CaD组为0。两个接受NaF治疗的组不完全(应力性)骨折的发生率相似。两个+E组均未发生完全性非椎体骨折;F CaD组和CaD组之间无差异。对照组(未使用NaF)的基线BMD(脊柱和股骨颈)与椎体骨折发生率相关,但在两个NaF组中无关。我们的结果及文献综述表明,如果使用氟盐,应采用低剂量,并在预处理和联合治疗时使用骨吸收抑制剂。
