阿仑膦酸钠在使用地诺单抗后的 1 年与 2 年对比:CARD 扩展研究。

IF 4.2 2区 医学 Q1 ENDOCRINOLOGY & METABOLISM
Osteoporosis International Pub Date : 2024-12-01 Epub Date: 2024-08-07 DOI:10.1007/s00198-024-07213-2
Joy N Tsai, Mackenzie Jordan, Hang Lee, Benjamin Z Leder
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引用次数: 0

摘要

停用地诺单抗后,抗骨质吸收治疗对减少高周转骨质流失至关重要。地诺单抗治疗后理想的抗骨吸收治疗时间尚不确定。这项研究表明,阿仑膦酸钠治疗1年和2年都能保持使用1年地诺单抗后获得的骨密度增长:背景:停用地诺单抗后,抗骨吸收治疗对于减轻高骨转换率骨丢失至关重要。然而,抗骨吸收治疗的理想选择和持续时间尚未确定。在 "地诺单抗治疗后阿仑膦酸钠或雷洛昔芬的比较"(CARD)研究中,我们证实阿仑膦酸钠治疗 12 个月与雷洛昔芬治疗 12 个月相比,能更好地维持地诺单抗治疗 12 个月所获得的骨密度(BMD)增长。在此次扩展研究中,我们希望确定阿仑膦酸钠 12 个月的疗程是否足以维持这些由地诺单抗引起的 BMD 增长:在 CARD 研究中,60-79 岁的绝经后骨质疏松症女性骨折风险较高,她们每 6 个月接受 12 个月的地诺单抗 60 毫克 SC 治疗,然后接受 12 个月的阿仑膦酸钠 70 毫克每周治疗(26 人)或雷洛昔芬治疗(25 人)。随后,阿仑膦酸钠治疗组的所有受试者均可参加为期一年的延长治疗,在延长治疗中,他们被随机分配继续服用阿仑膦酸钠 12 个月(10 人)或单独服用钙剂和维生素 D(8 人)。主要结果是脊柱 BMD 在第 24 个月和第 36 个月之间的变化。探索性终点包括其他解剖部位的平均 BMD(aBMD)变化以及血清骨转换标志物的变化:CARD研究表明,阿仑膦酸钠治疗12个月可有效保持地诺单抗诱导的BMD增长。在扩展研究中,无论是随机接受阿仑膦酸钠额外一年治疗的患者,还是随机接受钙/维生素 D 单独治疗的患者,其脊柱、全髋关节和股骨颈的 aBMD 都得到了维持。不过,我们确实观察到,在第 24-30 个月期间,钙/维生素 D 组的全髋关节(P = 0.008)和股骨颈(P = 0.040)的骨密度出现了短暂的比较性下降。在为期 24 个月的 CARD 研究结束时,两组的骨转换标志物血清 c-telopeptide (CTX) 和 I 型胶原原 N-肽 (PINP) 均受到抑制,然后在 24-36 个月期间,钙/维生素 D 组比阿仑膦酸钠组增加得更多(CTX 的 P = 0.051,P1NP 的 P = 0.030)。两组的 CTX 和 PINP 均保持在低于 0 月基线的水平(P尽管我们的样本量较小,但这些数据表明,阿仑膦酸钠治疗 1 年和 2 年可有效维持使用地诺单抗 1 年后获得的 BMD 增益,并防止骨转换标志物水平反弹至使用地诺单抗前的基线以上。这是首个评估短期地诺单抗后双膦酸盐最短持续时间的随机试验,可能有助于指导临床治疗。在使用更长时间的地诺单抗后进行类似研究将有助于进一步确定最佳治疗方案:试验注册:ClinicalTrials.gov 注册号:NCT03623633:试验注册:ClinicalTrials.gov 注册号:NCT03623633。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

One versus 2 years of alendronate following denosumab: the CARD extension.

One versus 2 years of alendronate following denosumab: the CARD extension.

When denosumab is discontinued, antiresorptive therapy is critical to reduce high-turnover bone loss. The ideal duration of antiresorptive therapy after denosumab is uncertain. This study demonstrates that both 1 and 2 years of alendronate maintained bone density gains achieved with 1 year of denosumab.

Background: When denosumab is discontinued, antiresorptive therapy is critical to attenuate high-turnover bone loss. The ideal choice and duration of antiresorptive therapy are not yet defined, however. In the Comparison of Alendronate or Raloxifene following Denosumab (CARD) study, we demonstrated that 12 months of alendronate was better able to maintain the bone mineral density (BMD) gains achieved with 12 months of denosumab versus 12 months of raloxifene. In this extension, we wished to determine if 12 months of alendronate would be sufficient in maintaining these denosumab-induced BMD gains.

Methods: In the CARD study, postmenopausal osteoporotic women aged 60-79 at high fracture risk received 12 months of denosumab 60-mg SC every 6 months followed by 12 months of either alendronate 70 mg weekly (N = 26) or raloxifene (N = 25). All subjects in the alendronate arm were then offered participation in a 1-year extension in which they were randomized to continue alendronate for an additional 12 months (N = 10) or to receive calcium and vitamin D alone (N = 8). The primary outcome was change in spine BMD between months 24 and 36. Exploratory endpoints included changes in areal BMD (aBMD) at other anatomic sites as well as changes in serum bone turnover markers.

Results: The CARD study demonstrated the effectiveness of 12 months alendronate in preserving denosumab-induced BMD gains. In the extension, aBMD was maintained at the spine, total hip, and femoral neck in both those randomized to an additional year of alendronate and those randomized to calcium/vitamin D alone. We did, however, observe a transient comparative decrease between months 24-30 in the calcium/vitamin D group at the total hip (P = 0.008) and femoral neck (P = 0.040). At the end of 24 months of the CARD study, bone turnover markers serum c-telopeptide (CTX) and procollagen N-propeptide of type I collagen (PINP) were suppressed in both groups and then increased more between months 24-36 in the calcium/vitamin D group than the alendronate group (P = 0.051 for CTX, P = 0.030 for P1NP). Both CTX and PINP remained below the month 0 baseline in both groups (P < 0.05 for all comparisons).

Conclusions: With the limitations of our small sample size, these data suggest that both 1 and 2 years of alendronate effectively maintain BMD gains achieved with 1 year of denosumab and prevented any rebound in bone turnover marker levels above pre-denosumab baseline. This is the first randomized trial to assess minimum duration of bisphosphonate after short-term denosumab and may be helpful to guide clinical care. Similar studies performed after longer durations of denosumab would be helpful to further define optimal management.

Trial registration: ClinicalTrials.gov registration number: NCT03623633.

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来源期刊
Osteoporosis International
Osteoporosis International 医学-内分泌学与代谢
CiteScore
8.10
自引率
10.00%
发文量
224
审稿时长
3 months
期刊介绍: An international multi-disciplinary journal which is a joint initiative between the International Osteoporosis Foundation and the National Osteoporosis Foundation of the USA, Osteoporosis International provides a forum for the communication and exchange of current ideas concerning the diagnosis, prevention, treatment and management of osteoporosis and other metabolic bone diseases. It publishes: original papers - reporting progress and results in all areas of osteoporosis and its related fields; review articles - reflecting the present state of knowledge in special areas of summarizing limited themes in which discussion has led to clearly defined conclusions; educational articles - giving information on the progress of a topic of particular interest; case reports - of uncommon or interesting presentations of the condition. While focusing on clinical research, the Journal will also accept submissions on more basic aspects of research, where they are considered by the editors to be relevant to the human disease spectrum.
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