Bone H G, Downs R W, Tucci J R, Harris S T, Weinstein R S, Licata A A, McClung M R, Kimmel D B, Gertz B J, Hale E, Polvino W J
Bone and Mineral Division, Henry Ford Hospital, Detroit, Michigan 48202, USA.
J Clin Endocrinol Metab. 1997 Jan;82(1):265-74. doi: 10.1210/jcem.82.1.3682.
Alendronate (ALN) is an aminobisphosphonate employed as an antiresorptive agent in the treatment of osteoporosis. The present study was carried out to determine dose-response relationships, particularly the effects of relatively low doses of ALN, on bone mineral density (BMD), biochemical indexes of bone and mineral metabolism, and bone histology, with particular attention to effects in elderly women. This prospective, randomized, double blind, 2-yr multicenter study compared the effects of placebo with those of 1.0, 2.5, or 5.0 mg ALN daily. All subjects received supplemental calcium (500 mg daily) as the carbonate. We studied 359 women with lumbar spine BMD at least 2.0 SD below the peak young adult mean. Subjects were stratified by age, with 135 aged 60-69 yr and 224 aged 70-85 yr. Histomorphometry was performed on transiliac bone biopsies obtained from 104 subjects after 1 yr and from 83 subjects after 2 yr. This study elucidated the previously uninvestigated lower region of the dose-response curve for ALN in osteoporosis. Over 2 yr, treatment with 1.0, 2.5, or 5.0 mg/day increased lumbar spine BMD, on the average, by 0.65%, 3.54%, and 5.67%, respectively, compared with that in the placebo group (P < 0.001 vs. placebo for the 2.5 and 5 mg groups). Significant dose-related increases were also seen in BMD at appendicular sites and in total body BMD. Dose-dependent reductions in bone turnover to new steady states were indicated by serum and urine biochemical markers as well as by histomorphometry. There was also a dose-related reduction in the proportion of subjects suffering nonvertebral fractures (P < 0.05). Safety profiles were similar for the ALN and placebo groups and for both age strata. Efficacy was similar for both age strata. There was no evidence of impaired mineralization or other histological abnormalities due to ALN treatment. We conclude that treatment with ALN over a period of 2 yr was well tolerated and produced dose-dependent increases in BMD without evidence of a plateau over the dose range of 1.0-5.0 mg daily. One milligram daily did not result in a significant effect on BMD, and 5.0 mg daily produced favorable effects at all sites measured. Other studies have demonstrated somewhat greater effects on 10 mg daily. ALN, was equally effective and well tolerated in osteoporotic women over 70 yr old as in younger women with the same condition.
阿仑膦酸盐(ALN)是一种氨基双膦酸盐,用作抗骨吸收药物治疗骨质疏松症。本研究旨在确定剂量反应关系,特别是相对低剂量的ALN对骨矿物质密度(BMD)、骨与矿物质代谢的生化指标以及骨组织学的影响,尤其关注对老年女性的影响。这项前瞻性、随机、双盲、为期2年的多中心研究比较了安慰剂与每日1.0、2.5或5.0 mg ALN的效果。所有受试者均补充碳酸钙(每日500 mg)。我们研究了359名腰椎BMD至少比年轻成人峰值均值低2.0标准差的女性。受试者按年龄分层,其中135名年龄在60 - 69岁,224名年龄在70 - 85岁。对104名受试者在1年后以及83名受试者在2年后获取的髂骨活检标本进行组织形态计量学分析。本研究阐明了骨质疏松症中ALN剂量反应曲线此前未被研究的较低区域。在2年期间,与安慰剂组相比,每日服用1.0、2.5或5.0 mg ALN使腰椎BMD平均分别增加了0.65%、3.54%和5.67%(2.5 mg和5 mg组与安慰剂相比,P < 0.001)。在四肢部位的BMD以及全身BMD方面也观察到了与剂量相关的显著增加。血清和尿液生化标志物以及组织形态计量学表明骨转换呈剂量依赖性降低至新的稳定状态。在发生非椎体骨折的受试者比例方面也有与剂量相关的降低(P < 0.05)。ALN组和安慰剂组以及两个年龄层的安全性概况相似。两个年龄层的疗效相似。没有证据表明ALN治疗会导致矿化受损或其他组织学异常。我们得出结论,为期2年的ALN治疗耐受性良好,能使BMD呈剂量依赖性增加,在每日1.0 - 5.0 mg的剂量范围内没有出现平台期的迹象。每日1 mg对BMD没有显著影响,每日5.0 mg在所有测量部位均产生了有利影响。其他研究表明每日10 mg的效果稍大一些。在70岁以上的骨质疏松女性中,ALN与同龄的年轻女性一样有效且耐受性良好。
