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地舒单抗治疗持续时间和唑来膦酸在停药后维持骨密度的疗效。

The Duration of Denosumab Treatment and the Efficacy of Zoledronate to Preserve Bone Mineral Density After Its Discontinuation.

机构信息

Department of Endocrinology and Diabetes and Department of Medical Research, 251 Hellenic Air Force & VA General Hospital, 11525, Athens,Greece.

Center for Bone Quality, Department of Internal Medicine, section Endocrinology, Leiden University Medical Center, 9600 2300 RC, Leiden,The Netherlands.

出版信息

J Clin Endocrinol Metab. 2021 Sep 27;106(10):e4155-e4162. doi: 10.1210/clinem/dgab321.

Abstract

CONTEXT

Zoledronate is used to prevent bone loss following denosumab discontinuation but its efficacy differs among studies.

OBJECTIVE

To test if the duration of denosumab treatment affects the efficacy of subsequent zoledronate infusion.

METHODS

This multicenter, prospective cohort study, conducted at 2 Greek and 1 Dutch bone centers, included 47 postmenopausal women (n = 47) who received a single zoledronate infusion 6 months after the last denosumab injection and then were followed for 1 year. Twenty-seven women received ≤ 6 denosumab injections (≤ 6 Group) and 20 received > 6 denosumab injections (> 6 Group). The main outcome measure was changes in lumbar spine (LS) bone mineral density (BMD).

RESULTS

At 12 months LS-BMD values were maintained in the ≤ 6 Group (0.98 ± 0.10 to 0.99 ± 0.9 g/cm2, P = 0.409) but decreased significantly in the > 6 Group (1.0 ± 0.11 to 0.93 ± 0.12 g/cm2, P < 0.001). The percent change of LS-BMD of the ≤ 6 Group (+1.0%) was significantly different (P < 0.001) from the change of the > 6 Group (-7.0%). In the whole cohort, the duration of denosumab treatment was negatively correlated with the percentage change of LS-BMD (rs = -0.669, P < 0.001) but not with the change of femoral neck (FN)-BMD. Bone turnover markers increased in all patients 6 months following zoledronate administration with no difference between the 2 groups.

CONCLUSION

The duration of denosumab treatment significantly affects the efficacy of subsequent zoledronate infusion to maintain BMD gains. Frequent follow-up of patients treated with denosumab longer than 3 years is advisable as additional therapeutic interventions may be needed.

摘要

背景

唑来膦酸用于预防地舒单抗停药后的骨质流失,但不同研究的疗效不同。

目的

检测地舒单抗治疗持续时间对后续唑来膦酸输注疗效的影响。

方法

这项多中心前瞻性队列研究在希腊的 2 家和荷兰的 1 家骨科中心进行,共纳入 47 名绝经后女性(n=47),她们在最后一次地舒单抗注射后 6 个月接受单次唑来膦酸输注,然后随访 1 年。27 名女性接受≤6 次地舒单抗注射(≤6 组),20 名女性接受>6 次地舒单抗注射(>6 组)。主要结局测量指标为腰椎(LS)骨密度(BMD)变化。

结果

在 12 个月时,≤6 组 LS-BMD 值保持稳定(0.98±0.10 至 0.99±0.9 g/cm2,P=0.409),但>6 组显著下降(1.0±0.11 至 0.93±0.12 g/cm2,P<0.001)。≤6 组 LS-BMD 的百分变化(+1.0%)与>6 组的变化(-7.0%)显著不同(P<0.001)。在整个队列中,地舒单抗治疗持续时间与 LS-BMD 百分变化呈负相关(rs=-0.669,P<0.001),但与股骨颈(FN)-BMD 的变化无关。所有患者在唑来膦酸给药后 6 个月时骨转换标志物均增加,两组之间无差异。

结论

地舒单抗治疗持续时间显著影响后续唑来膦酸输注维持 BMD 获益的疗效。对于接受地舒单抗治疗超过 3 年的患者,应进行频繁随访,可能需要额外的治疗干预。

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