早发性卵巢功能不全/早绝经女性的骨骼健康：23 年的纵向分析。

Bone health in women with premature ovarian insufficiency/early menopause: a 23-year longitudinal analysis.

机构信息

Monash Centre for Health Research and Implementation, Monash University, Melbourne, VIC, Australia.

Department of Endocrinology, Monash Health, Melbourne, VIC, Australia.

出版信息

Hum Reprod. 2024 May 2;39(5):1013-1022. doi: 10.1093/humrep/deae037.

STUDY QUESTION

What is the frequency of, and predictors for, osteoporosis, fractures, and osteoporosis management (investigation, treatment) in women with premature ovarian insufficiency (POI; menopause <40 years) and early menopause (EM; menopause 40-44years)?

SUMMARY ANSWER

Over the 23-year follow-up duration, at a mean age of 68 years, women with POI/EM had higher osteoporosis/fracture risk and prevalence, higher osteoporosis screening and anti-osteoporosis medication use compared to women with usual age menopause; increasing age was predictive of increased risk of osteoporosis/fracture and menopause hormone therapy (MHT) prior to or at study entry (aged 45-50 years) was protective.

WHAT IS KNOWN ALREADY

Women with POI/EM have increased risk of osteoporosis and fractures with limited data regarding risk factors for reduced bone density and fractures. Clinical guidelines recommend screening with dual X-ray absorptiometry (DXA) and treatment with MHT for most women with POI/EM to reduce osteoporosis and fracture risk; however, studies indicate gaps in osteoporosis knowledge, guideline uptake, and management adherence by clinicians and women.

STUDY DESIGN, SIZE, DURATION: The Australian Longitudinal Study on Women's Health is a prospective longitudinal study of Australian women. This study uses the cohort of women born between 1946 and 1951, surveyed nine times between 1996 and 2019. Data from the Australian administrative health records, including hospital admissions data (fractures, osteoporosis), Medicare Benefits Schedule (DXA), and the Pharmaceutical Benefits Scheme (PBS; MHT, anti-osteoporosis medication, available only from 2002) were linked to survey data.

PARTICIPANTS/MATERIALS, SETTING, METHODS: Survey respondents with self-reported age of menopause were included. POI/EM was defined as menopause <45 years. T-test or chi-square were used for comparisons at baseline (P < 0.05 indicates significance). Generalized estimating equations for panel data explored predictors for the longitudinal outcomes of osteoporosis, fractures, DXA rates, MHT use, and anti-osteoporosis medication (in women with osteoporosis/fracture, from Survey 4 onwards only). Univariable regression was performed, and variables retained where P < 0.2, to form the multivariable model, and bootstrapping with 100 repetitions at 95% sampling of the original dataset to ensure robustness of results.

MAIN RESULTS AND THE ROLE OF CHANCE

Eight thousand six hundred and three women were included: 610 (7.1%) with POI/EM. Mean (SD) baseline age was 47.6 (1.45) years in the entire cohort and mean (SD) age of menopause was 38.2 (7.95) and 51.3 (3.04) years in women with POI/EM and usual age menopause, respectively (P < 0.001). Over the 23 years, of women with POI/EM, 303 (49.7%) had osteoporosis/fractures, 421 (69.0%) had DXA screening, 474 ever used MHT (77.7%), and 116 (39.1%) of those with osteoporosis/fractures used anti-osteoporosis medication. Of women with usual age menopause, 2929 (36.6%) had osteoporosis/fractures, 4920 (61.6%) had DXA screening, 4014 (50.2%) used MHT, and 964 (33.0%) of those with osteoporosis/fractures used anti-osteoporosis medication. Compared to women with menopause at age ≥45 years and after adjusting for other risk factors, women with POI/EM had increased risk of osteoporosis (odds ratio [OR] 1.37; 95% CI 1.07-1.77), fractures (OR 1.45; 1.15-1.81), DXA testing (OR 1.64; 1.42-1.90), MHT use (OR 6.87; 5.68-8.30), and anti-osteoporosis medication use (OR 1.50; 1.14-1.98). In women with POI/EM women, increasing age was associated with greater risk of osteoporosis/fracture (OR 1.09; 1.08-1.11), and MHT prior to or at study entry (aged 45-50 years), was protective (OR 0.65, 0.45-0.96). In women with POI/EM, age (OR 1.11; 1.10-1.12), fractures (OR 1.80, 1.38-2.34), current smoking (OR 0.60; 0.43-0.86), and inner (OR 0.68; 0.53-0.88) or outer regional (OR 0.63; 0.46-0.87) residential location were associated with DXA screening. In women with POI/EM, increasing age (OR 1.02; 1.01-1.02), and currently consuming alcohol (OR 1.17; 1.06-1.28), was associated with having ever used MHT. In the 299 women with POI/EM and osteoporosis/fractures, only 39.1% ever received treatment with an anti-osteoporosis medication. Increasing age (OR 1.07; 1.04-1.09) and lower BMI (OR 0.95; 0.92-0.98) were associated with greater likelihood of treatment with anti-osteoporosis medication.

LIMITATIONS, REASONS FOR CAUTION: Survey data including age of menopause were self-reported by participants; fracture questions were not included in the 2001 survey, and location or level of trauma of self-reported fractures was not asked. Additional risk/protective factors such as vitamin D status, calcium intake, and exercise were not able to be included. Due to sample size, POI and EM were combined for all analyses, and we were unable to differentiate between causes of POI/EM. PBS data were only available from 2004, and hospital admissions data were state-based, with all of Australia were only available from 2007.

WIDER IMPLICATIONS OF THE FINDINGS

This study supports previous literature indicating increased risk of osteoporosis and fractures in women with POI, and adds evidence for women with POI/EM, where there was a relative paucity of data. This is the first study to analyse a variety of clinical and demographic risk factors for osteoporosis and fractures in women with POI/EM, as well as analysing investigation and treatment rates. In these women, using MHT prior to or at study entry, aged 45-50 years, was protective for osteoporosis/fractures; however, having ever used MHT was not, highlighting the importance of early treatment with MHT in these women to preserve bone strength. Although women with POI/EM and osteoporosis or fractures were more likely to use anti-osteoporosis medications than those with usual age menopause, overall treatment rates are low at <40%, demonstrating a significant treatment gap that should be addressed to reduce future fracture risk.

STUDY FUNDING/COMPETING INTEREST(S): This study was funded by The Australian NHMRC Centre of Research Excellence Women's Health in Reproductive Life (CRE-WHIRL, project number APP1171592). A.R.J. is the recipient of a National Health and Medical Research Council post-graduate research scholarship (grant number 1169192). P.R.E. is supported by a National Health and Medical Research Council grant 1197958. P.R.E. reports grants paid to their institution from Amgen, Sanofi, and Alexion, honoraria from Amgen paid to their institution, and honoraria from Alexion and Kyowa-Kirin.

TRIAL REGISTRATION NUMBER

N/A.

研究问题

患有原发性卵巢功能不全（绝经年龄＜40 岁）和早发性卵巢功能不全（绝经年龄 40-44 岁）的女性骨质疏松症、骨折和骨质疏松症管理（调查、治疗）的频率及其预测因素是什么？

总结答案

在 23 年的随访期间，在平均 68 岁时，与绝经年龄≥45 岁且其他危险因素调整后相比，POI/EM 女性的骨质疏松/骨折风险和患病率更高，骨质疏松症筛查和抗骨质疏松症药物使用率更高；年龄增长与骨质疏松/骨折风险增加相关，绝经前或研究入组时（45-50 岁）使用激素替代疗法（HRT）具有保护作用。

已知信息

POI/EM 女性的骨质疏松症和骨折风险增加，关于降低骨密度和骨折风险的危险因素的资料有限。临床指南建议对大多数 POI/EM 女性进行双能 X 线吸收法（DXA）筛查和使用 HRT 治疗，以降低骨质疏松症和骨折风险；然而，研究表明，临床医生和女性在骨质疏松症知识、指南采用和管理依从性方面存在差距。

研究设计、规模、持续时间：澳大利亚女性健康纵向研究是一项对澳大利亚女性的前瞻性纵向研究。该研究使用了 1946 年至 1951 年出生的女性队列，于 1996 年至 2019 年进行了九次调查。澳大利亚行政健康记录中的数据，包括医院入院数据（骨折、骨质疏松症）、医疗保险福利计划（DXA）和药品福利计划（PBS；仅从 2002 年起可用于抗骨质疏松症药物）与调查数据相关联。

参与者/材料、设置、方法：纳入了有自我报告绝经年龄的调查参与者。POI/EM 定义为绝经年龄＜45 岁。T 检验或卡方检验用于比较基线时的差异（P＜0.05 表示差异显著）。面板数据的广义估计方程用于研究骨质疏松症、骨折、DXA 率、HRT 使用和骨质疏松症治疗（骨折/骨质疏松症女性从调查 4 开始）的纵向结局的预测因素。进行单变量回归，保留 P＜0.2 的变量，以形成多变量模型，并通过对原始数据集的 95%抽样进行 100 次 bootstrap 处理，以确保结果的稳健性。

主要结果和机会的作用

纳入了 8630 名女性：610 名（7.1%）患有 POI/EM。整个队列的平均（SD）基线年龄为 47.6（1.45）岁，POI/EM 女性的平均（SD）绝经年龄为 38.2（7.95）岁和 51.3（3.04）岁（P＜0.001）。在 23 年期间，POI/EM 女性中有 303 名（49.7%）患有骨质疏松症/骨折，421 名（69.0%）接受了 DXA 筛查，474 名女性曾使用 HRT（77.7%），303 名患有骨质疏松症/骨折的女性中有 116 名（39.1%）使用了抗骨质疏松症药物。在绝经年龄≥45 岁的女性中，2929 名（36.6%）患有骨质疏松症/骨折，4920 名（61.6%）接受了 DXA 筛查，4014 名（50.2%）使用了 HRT，303 名患有骨质疏松症/骨折的女性中有 964 名（33.0%）使用了抗骨质疏松症药物。与绝经年龄≥45 岁且其他危险因素调整后相比，POI/EM 女性的骨质疏松症（优势比[OR]1.37；95%置信区间[CI]1.07-1.77）、骨折（OR 1.45；1.15-1.81）、DXA 检测（OR 1.64；1.42-1.90）、HRT 使用（OR 6.87；5.68-8.30）和抗骨质疏松症药物使用（OR 1.50；1.14-1.98）的风险增加。在 POI/EM 女性中，年龄增长与骨质疏松/骨折风险增加相关（OR 1.09；1.08-1.11），绝经前或研究入组时（45-50 岁）使用 HRT 具有保护作用（OR 0.65，0.45-0.96）。在 POI/EM 女性中，年龄（OR 1.11；1.10-1.12）、骨折（OR 1.80；1.38-2.34）、当前吸烟（OR 0.60；0.43-0.86）和内部（OR 0.68；0.53-0.88）或外部区域（OR 0.63；0.46-0.87）居住地点与 DXA 筛查相关。在 POI/EM 女性中，年龄增长（OR 1.02；1.01-1.02）和目前饮酒（OR 1.17；1.06-1.28）与使用 HRT 有关。在 299 名患有 POI/EM 和骨质疏松/骨折的女性中，只有 39.1%的人接受过抗骨质疏松症药物治疗。年龄增长（OR 1.07；1.04-1.09）和较低的 BMI（OR 0.95；0.92-0.98）与接受抗骨质疏松症药物治疗的可能性更大相关。

局限性、谨慎的原因：包括年龄的调查数据是由参与者自我报告的；骨折问题未包含在 2001 年的调查中，也没有询问自我报告的骨折的创伤部位或严重程度。无法包括其他风险/保护因素，如维生素 D 状态、钙摄入量和运动。由于样本量的限制，POI 和 EM 在所有分析中合并，我们无法区分 POI/EM 的原因。从 2004 年开始才有 PBS 数据，从 2007 年开始才有州级的医院入院数据，直到所有澳大利亚的医院入院数据才开始可用。

更广泛的影响

这项研究支持之前关于 POI 女性骨质疏松症和骨折风险增加的文献，并为 POI/EM 女性提供了证据，因为之前这方面的数据很少。这是第一项分析 POI/EM 女性各种临床和人口统计学骨质疏松症和骨折风险因素的研究，以及分析调查和治疗率的研究。在这些女性中，绝经前或研究入组时（45-50 岁）使用 HRT 具有保护作用，可预防骨质疏松/骨折；然而，曾使用 HRT 并不具有保护作用，这强调了在这些女性中早期使用 HRT 以保持骨强度的重要性。尽管 POI/EM 女性患有骨质疏松症或骨折的可能性比绝经年龄≥45 岁且其他危险因素调整后更高，但使用抗骨质疏松症药物的可能性仍然较低，<40%，这表明需要解决这一显著的治疗差距，以降低未来骨折风险。

研究资助/利益冲突：这项研究由澳大利亚国家卫生和医学研究委员会妇女生殖生活研究卓越中心（项目编号 APP1171592）资助。A.R.J. 是澳大利亚国家卫生和医学研究委员会研究生研究奖学金（赠款编号 1169192）的获得者。P.R.E. 得到了澳大利亚国家卫生和医学研究委员会 1197958 号赠款的支持。P.R.E. 报告说，他们的机构收到了 Amgen、Sanofi 和 Alexion 的拨款，他们的机构收到了 Amgen 的酬金，他们还从 Alexion 和 Kyowa-Kirin 获得了酬金。

试验注册号码

无。