前额纤维性秃发中ERAP1与4种主要组织相容性复合体I类等位基因的上位性:一项全基因组关联研究的荟萃分析
Epistasis of ERAP1 With 4 Major Histocompatibility Complex Class I Alleles in Frontal Fibrosing Alopecia: A Genome-Wide Association Study Meta-Analysis.
作者信息
Rayinda Tuntas, Dand Nick, McSweeney Sheila M, Christou Evangelos, Ung Chuin Ying, Stefanato Catherine M, Fenton David A, Harries Matthew, Palamaras Ioulios, Tidman Alice, Holmes Susan, Koutalopoulou Anastasia, Ardern-Jones Michael, Kaur Manjit, Papanikou Sofia, Chasapi Vasiliki, Vañó-Galvan Sergio, Saceda-Corralo David, Melián-Olivera Ana, Azcarraga-Llobet Carlos, Lobato-Berezo Alejandro, Bustamante Mariona, Sunyer Jordi, Starace Michela Valeria Rita, Piraccini Bianca Maria, Wiss Isabel Pupo, Senna Maryanne Makredes, Singh Rashmi, Hillmann Kathrin, Kanti-Schmidt Varvara, Blume-Peytavi Ulrike, McGrath John A, Simpson Michael A, Tziotzios Christos
机构信息
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, Yogyakarta, Indonesia.
出版信息
JAMA Dermatol. 2025 Mar 1;161(3):310-314. doi: 10.1001/jamadermatol.2024.6434.
IMPORTANCE
Frontal fibrosing alopecia (FFA) is an inflammatory and scarring form of hair loss of increasing prevalence that most commonly affects women. An improved understanding of the genetic basis of FFA will support the identification of pathogenic mechanisms and therapeutic targets.
OBJECTIVE
To identify novel genomic loci at which common genetic variation affects FFA susceptibility and assess nonadditive effects on genetic risk between susceptibility loci.
DESIGN, SETTING, AND PARTICIPANTS: Four genome-wide association studies were combined using an SE-weighted meta-analysis. Within the major histocompatibility complex (MHC) locus, stepwise conditional analysis was undertaken to determine independently associated classical MHC class I alleles. Statistical tests for epistatic interaction were performed between risk alleles at the MHC and endoplasmic reticulum aminopeptidase 1 (ERAP1) loci.
MAIN OUTCOMES AND MEASURES
Genome-wide significant locus associated with FFA and nonadditive effects on genetic risk between susceptibility loci.
RESULTS
Of 6668 included patients, there were 1585 European female individuals with FFA and 5083 controls. Genome-wide significant associations were identified at 4 genomic loci, including a novel susceptibility locus at 5q15, and the association signal could be fine-mapped to a single nucleotide substitution (rs10045403) in the 5' untranslated region of ERAP1 (rs10045403; odds ratio, 1.30; 95% CI, 1.19-1.43; P = 3.6 × 10-8). Within the MHC, FFA risk was statistically independently associated with HLA-A11:01, HLA-A33:01, HLA-B07:02, and HLA-B35:01. FFA risk was affected by genetic variation at the ERAP1 locus only in individuals who carried at least 1 of the MHC class I risk alleles.
CONCLUSIONS AND RELEVANCE
In this genome-wide meta-analysis, a supra-additive effect of genetic variation was found that affected peptide trimming and antigen presentation on FFA susceptibility. Patients with FFA may benefit from emerging therapeutic approaches that modulate ERAP-mediated processes.
重要性
额部纤维性秃发(FFA)是一种炎症性瘢痕性脱发,其患病率不断上升,最常影响女性。更好地理解FFA的遗传基础将有助于确定致病机制和治疗靶点。
目的
确定常见基因变异影响FFA易感性的新基因组位点,并评估易感位点之间对遗传风险的非加性效应。
设计、背景和参与者:使用SE加权荟萃分析合并了四项全基因组关联研究。在主要组织相容性复合体(MHC)位点内,进行逐步条件分析以确定独立相关的经典MHC I类等位基因。对MHC和内质网氨肽酶1(ERAP1)位点的风险等位基因之间进行上位性相互作用的统计检验。
主要结局和指标
与FFA相关的全基因组显著位点以及易感位点之间对遗传风险的非加性效应。
结果
在纳入的6668例患者中,有1585例欧洲女性FFA患者和5083例对照。在4个基因组位点发现了全基因组显著关联,包括5q15处的一个新的易感位点,并且关联信号可精细定位到ERAP1 5'非翻译区的一个单核苷酸替换(rs10045403;比值比,1.30;95%CI,1.19 - 1.43;P = 3.6 × 10⁻⁸)。在MHC内,FFA风险与HLA - A11:01、HLA - A33:01、HLA - B07:02和HLA - B35:01在统计学上独立相关。仅在携带至少1个MHC I类风险等位基因的个体中,ERAP1位点的基因变异会影响FFA风险。
结论和相关性
在这项全基因组荟萃分析中,发现了基因变异的超加性效应,其影响肽修剪和抗原呈递对FFA易感性的作用。FFA患者可能受益于调节ERAP介导过程的新兴治疗方法。
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