St John's Institute of Dermatology, King's College London, London, United Kingdom.
Department of Dermatology and Venereology, Faculty of Medicine, Public Health, and Nursing, Universitas Gadjah Mada, Sleman, Special Region of Yogyakarta, Indonesia.
JAMA Dermatol. 2024 Jul 1;160(7):732-735. doi: 10.1001/jamadermatol.2024.1315.
Frontal fibrosing alopecia (FFA) is an increasingly prevalent form of follicular lichen planus, causing irreversible hair loss predominantly in postmenopausal individuals. An earlier genome-wide meta-analysis of female FFA identified risk loci in genes implicated in self-antigen presentation and T-cell homeostasis, including HLA-B*07:02, ST3GAL1, and SEMA4B. However, CYP1B1, which is important for hormone metabolism, was also implicated with the substitution of serine for asparagine at position 453 (c.1358A>G, p.Asn453Ser) exhibiting a protective effect against FFA. Increasing understanding of genetic and environmental variables and their interactions will improve understanding of disease pathogenesis and has the potential to inform risk mitigation strategies.
To investigate whether oral contraceptive pill (OCP) use modulates the protective effect of the common missense variant in CYP1B1 (c.1358A>G, p.Asn453Ser) on FFA risk.
DESIGN, SETTING, AND PARTICIPANTS: This gene-environment interaction study using a case-control design enrolled female patients with FFA from UK-based dermatology clinics. The patients were matched with unrelated age- and ancestry-matched female control individuals derived from UK Biobank in a 1:66 ratio, determined by the first 4 principal components from genome-wide genotypes. Data were collected from July 2015 to September 2017, and analyzed from October 2022 to December 2023.
The main outcomes were the modulatory effect of OCP use on the contribution of the CYP1B1 missense variant to female FFA risk and a formal gene-environment interaction test evaluated by a logistic regression model with a multiplicative interaction term, under the assumptions of an additive genetic model interaction term, under the assumptions of an additive genetic model.
Of the 489 female patients with FFA, the mean (SD) age was 65.8 (9.7) years, and 370 (75.7%) had a history of OCP use. Of the 34 254 age- and ancestry-matched control individuals, the mean (SD) age was 65.0 (8.4) years, and previous OCP use was reported in 31 177 (91.0%). An association between female FFA and the CYP1B1 risk allele was observed in individuals who reported OCP use (odds ratio, 1.90 [95% CI, 1.50-2.40]; P = 8.41 × 10-8) but not in those with no documented exposure to OCPs (odds ratio, 1.16 [95% CI, 0.82-1.64]; P = .39). A full gene-environment interaction model demonstrated a significant additive statistical interaction between c.1358A, p.453Asn, and history of OCP use on FFA risk (OR for interaction, 1.63 [95% CI, 1.07-2.46]; P = .02).
This gene-environment interaction analysis suggests that the protective effect of the CYP1B1 missense variant on FFA risk might be mediated by exposure to OCPs. The allele that encodes an asparagine at position 453 of CYP1B1 was associated with increased odds of FFA only in participants with OCP history.
额部纤维性脱发(FFA)是一种越来越常见的滤泡性扁平苔藓形式,主要导致绝经后个体不可逆的脱发。对女性 FFA 的早期全基因组荟萃分析确定了风险基因座,这些基因座涉及自身抗原呈递和 T 细胞稳态,包括 HLA-B*07:02、ST3GAL1 和 SEMA4B。然而,CYP1B1 对于激素代谢也很重要,其第 453 位的丝氨酸被天冬酰胺取代(c.1358A>G,p.Asn453Ser),这与 FFA 风险呈保护作用。越来越多地了解遗传和环境变量及其相互作用将有助于更好地理解疾病发病机制,并有可能为风险缓解策略提供信息。
研究口服避孕药(OCP)的使用是否会调节 CYP1B1 常见错义变体(c.1358A>G,p.Asn453Ser)对 FFA 风险的保护作用。
设计、地点和参与者:本项病例对照研究采用基因-环境相互作用设计,招募了来自英国皮肤科诊所的女性 FFA 患者。患者与来自英国生物库的年龄和祖源相匹配的女性对照个体以 1:66 的比例相匹配,这是通过全基因组基因型的前 4 个主成分确定的。数据于 2015 年 7 月至 2017 年 9 月收集,2023 年 10 月至 12 月分析。
主要结果是 OCP 使用对 CYP1B1 错义变体对女性 FFA 风险的贡献的调节作用,以及通过具有乘法交互项的逻辑回归模型评估的正式基因-环境相互作用检验,假设遗传模型交互项为加性。
在 489 名患有 FFA 的女性患者中,平均(标准差)年龄为 65.8(9.7)岁,370 名(75.7%)有 OCP 使用史。在 34254 名年龄和祖源匹配的对照个体中,平均(标准差)年龄为 65.0(8.4)岁,31177 名(91.0%)报告有 OCP 使用史。在有 OCP 使用史的个体中,女性 FFA 与 CYP1B1 风险等位基因相关(优势比,1.90[95%CI,1.50-2.40];P=8.41×10-8),但在无 OCP 暴露史的个体中则没有(优势比,1.16[95%CI,0.82-1.64];P=0.39)。全基因-环境相互作用模型表明,c.1358A、p.453Asn 和 OCP 使用史与 FFA 风险之间存在显著的加性统计相互作用(交互作用的优势比,1.63[95%CI,1.07-2.46];P=0.02)。
这项基因-环境相互作用分析表明,CYP1B1 错义变体对 FFA 风险的保护作用可能是由 OCP 暴露介导的。编码 CYP1B1 第 453 位天冬酰胺的等位基因与 OCP 史参与者的 FFA 发病几率增加相关。
