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激素避孕与骨代谢:对青春期后及育龄期女性研究的系统评价和荟萃分析的新证据

Hormonal Contraception and Bone Metabolism: Emerging Evidence from a Systematic Review and Meta-Analysis of Studies on Post-Pubertal and Reproductive-Age Women.

作者信息

Tassi Alice, Londero Ambrogio P, Xholli Anjeza, Lanzolla Giulia, Bertozzi Serena, Savelli Luca, Prefumo Federico, Cagnacci Angelo

机构信息

Obstetrics and Gynecology Unit, Morgagni-Pierantoni Hospital, 47121 Forlì, Italy.

Department of Neuroscience, Rehabilitation, Ophthalmology, Genetics, Maternal and Infant Health, University of Genoa, 16132 Genova, Italy.

出版信息

Pharmaceuticals (Basel). 2025 Jan 8;18(1):61. doi: 10.3390/ph18010061.

Abstract

BACKGROUND/OBJECTIVES: This study aims to assess the effects of combined hormonal contraceptives (CHCs) on bone metabolism markers. It primarily measures osteocalcin and additionally examines other bone health markers, seeking to determine their responses to estrogen-progestogen treatments.

METHODS

This study involved a comprehensive evaluation of the pertinent literature and a meta-analysis explicitly conducted on data describing women of reproductive age. The analysis encompassed accessible papers ranging to December 2024 (i.e., those listed in PubMed/Medline, Embase, Scopus, the Cochrane Database, International Clinical Trials Registry, and ClinicalTrials.gov). We examined published randomized controlled trials (RCTs) and prospective studies. The quality of the studies was assessed using the Cochrane tool for RCTs and the Newcastle-Ottawa Scale for prospective studies. The selected indicators for primary and secondary outcomes were ascertained by standardized mean change (SMC), displaying the difference between conditions before and after treatment. Trends were evaluated using meta-regressions.

RESULTS

Ultimately, 34 articles out of 1924 identified items met the inclusion criteria, covering 33 unique studies. In EE/E4 combinations, osteocalcin dropped significantly (SMC -0.54 (CI.95 -0.64/-0.43) and -0.43 (CI.95 -0.76/-0.10)). Similar effects were observed for other bone-formation and reabsorption markers, with less significant reductions observed in E2-containing CHC (e.g., alkaline phosphatase (bone) EE combinations, SMC -0.39 (CI.95 -0.67/-0.11); P1NP E2 combination, 0.12 (CI.95 -0.10/0.33); and EE combinations, -0.55 (CI.95 -0.83/-0.26)). The reduction patterns also exhibited differences according to the women's age (e.g., osteocalcin in EE combinations ≤21, SMC -0.63 (CI.95 -0.77/-0.49) and >21, SMC -0.42 (CI.95 -0.61/-0.24); alkaline phosphatase (bone) EE combinations ≤21, SMC -0.55 (CI.95 -0.86/-0.24) and >21, SMC -0.06 (CI.95 -0.47/0.35)). This analysis found that CHC maintains or reduces bone turnover in childbearing women, with effects varying by age and hormone combination. Moreover, bone-formation and reabsorption markers correlated positively to pro-androgenic progestins ( < 0.05). Thus, estrogen-progestogen combinations reduce bone turnover less when weak estrogens and a pro-androgenic or neutral progestin are present.

CONCLUSIONS

This study found that CHCs reduce bone turnover, with natural estrogens and androgenic progestins appearing to be more beneficial than EE and anti-androgenic types. These findings would potentially influence decisions relevant to CHC prescriptions during a woman's reproductive phases, emphasizing the need for additional research to tailor CHC usage to bone health.

摘要

背景/目的:本研究旨在评估复方激素避孕药(CHC)对骨代谢标志物的影响。主要测量骨钙素,并额外检测其他骨骼健康标志物,以确定它们对雌激素 - 孕激素治疗的反应。

方法

本研究对相关文献进行了全面评估,并对描述育龄女性的数据进行了明确的荟萃分析。分析涵盖了截至2024年12月可获取的论文(即那些列于PubMed/Medline、Embase、Scopus、Cochrane数据库、国际临床试验注册中心和ClinicalTrials.gov中的论文)。我们审查了已发表的随机对照试验(RCT)和前瞻性研究。使用Cochrane工具评估RCT的研究质量,使用纽卡斯尔 - 渥太华量表评估前瞻性研究的质量。通过标准化平均变化(SMC)确定主要和次要结局的选定指标,显示治疗前后状况的差异。使用荟萃回归评估趋势。

结果

最终,在1924篇识别出的文章中,有34篇符合纳入标准,涵盖33项独特的研究。在炔雌醇/雌四醇(EE/E4)组合中,骨钙素显著下降(SMC -0.54(CI.95 -0.64/-0.43)和 -0.43(CI.95 -0.76/-0.10))。其他骨形成和重吸收标志物也观察到类似效果,含雌二醇(E2)的CHC中观察到的下降不太显著(例如,骨碱性磷酸酶EE组合,SMC -0.39(CI.95 -0.67/-0.11);I型前胶原氨基端前肽E2组合,0.12(CI.95 -0.10/0.33);以及EE组合,-0.55(CI.95 -0.83/-0.26))。根据女性年龄,下降模式也存在差异(例如,EE组合中≤21岁女性的骨钙素,SMC -0.63(CI.95 -0.77/-0.49),>21岁女性的骨钙素,SMC -0.42(CI.95 -0.61/-0.24);骨碱性磷酸酶EE组合中≤21岁女性,SMC -0.55(CI.95 -0.86/-0.24),>21岁女性,SMC -0.06(CI.95 -0.47/0.35))。该分析发现,CHC可维持或降低育龄女性的骨转换,其效果因年龄和激素组合而异。此外,骨形成和重吸收标志物与促雄激素孕激素呈正相关(<0.05)。因此,当存在弱雌激素和促雄激素或中性孕激素时,雌激素 - 孕激素组合对骨转换的降低作用较小。

结论

本研究发现,CHC可降低骨转换,天然雌激素和雄激素类孕激素似乎比炔雌醇和抗雄激素类更有益。这些发现可能会影响女性生殖阶段CHC处方相关的决策,强调需要进行更多研究以根据骨骼健康调整CHC的使用。

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