Department of Orthopedic Surgery, Leiden University Medical Center, 2333 ZA Leiden, The Netherlands.
Department of Clinical Epidemiology, Aarhus University, 8200 Aarhus N, Denmark.
J Clin Endocrinol Metab. 2024 May 17;109(6):1423-1432. doi: 10.1210/clinem/dgad744.
Fibrous dysplasia/McCune-Albright syndrome (FD/MAS) is a rare genetic disorder. Incidence and prevalence are not well-studied. Epidemiological research is complicated by the rarity of FD/MAS, absence of registries, heterogeneous presentation, and possibly asymptomatic phenotype. FD/MAS may present with FGF23-mediated hypophosphatemia, of which the epidemiology is also unclear.
Evaluate incidence and prevalence of FD/MAS and FD/MAS-related hypophosphatemia.
This cohort study based on the nationwide Danish National Patient Registry from 1995-2018, included patients identified by ICD-10 codes M85.0 (monostotic FD [MFD]) and Q78.1 (polyostotic FD [PFD]/MAS). Incidence rates and prevalence were calculated and stratified by sex, age, calendar period, and diagnosis code. Cases were screened for FD-associated hypophosphatemia by diagnosis code E.83 (disorder of mineral metabolism) and dispatched vitamin D analogues.
A total of 408 patients were identified, 269 with MFD (66%), 139 with PFD/MAS (34%), comparable between sexes. Incidence of FD/MAS demonstrated increasing secular trend with a rate of 3.6 per 1 000 000 person-years (95% CI: 2.9, 4.5) in 2015-2018. Incidence peaked between age 11 and 20. Prevalence of FD/MAS increased over time to 61.0 (95% CI: 54.6, 67.4) per 1 000 000 persons in 2018. The incidence rate of MFD was 1.5-fold that of PFD/MAS in the first decade, rising to 2.5-fold in the last decade. No FD/MAS cases were registered with diagnosis code or treatment for hypophosphatemia.
FD/MAS is rare, diagnosis peaks during adolescence without sex predominance, and MFD is most prevalent. Hypophosphatemia may be underdiagnosed and undertreated, or it may be underregistered, comparing this study to literature.
纤维结构不良/麦卡恩-阿尔布赖特综合征(FD/MAS)是一种罕见的遗传性疾病。其发病率和患病率尚未得到充分研究。由于 FD/MAS 罕见、缺乏登记、表现多样且可能为无症状表型,因此流行病学研究较为复杂。FD/MAS 可表现为成纤维细胞生长因子 23 介导的低磷血症,其流行病学也不清楚。
评估 FD/MAS 和 FD/MAS 相关低磷血症的发病率和患病率。
本队列研究基于 1995 年至 2018 年全国丹麦国家患者登记处的数据,通过 ICD-10 编码 M85.0(单发性 FD [MFD])和 Q78.1(多发性 FD [PFD]/MAS)识别患者。计算发病率和患病率,并按性别、年龄、日历时间和诊断代码进行分层。通过诊断代码 E.83(矿物质代谢障碍)和维生素 D 类似物的处方筛选 FD 相关低磷血症病例。
共确定了 408 例患者,其中 269 例为 MFD(66%),139 例为 PFD/MAS(34%),性别间无差异。FD/MAS 的发病率呈明显的时间趋势,2015 年至 2018 年的发病率为 3.6/100 万人口(95%CI:2.9,4.5)。发病率在 11 至 20 岁之间达到高峰。FD/MAS 的患病率随时间推移而增加,2018 年达到 61.0(95%CI:54.6,67.4)/100 万人口。在第一个十年中,MFD 的发病率是 PFD/MAS 的 1.5 倍,在最后十年中上升至 2.5 倍。没有 FD/MAS 病例以诊断代码或低磷血症治疗进行登记。
FD/MAS 较为罕见,诊断高峰在青春期,无性别优势,MFD 最常见。与文献相比,低磷血症可能诊断不足和治疗不足,或者登记不足。
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