Genome-wide association study in Turkish and Iranian populations identify rare familial Mediterranean fever gene (MEFV) polymorphisms associated with ankylosing spondylitis
Li, Zhixiu, Akar, Servet, Yarkan, Handan, Lee, Sau Kuen, Cetin, Pınar, Can, Gercek, Kenar, Gokce, Capa, Fernur, Pamuk, Omer Nuri, Pehlivan, Yavuz, Cremin, Katie, de Guzman, Erika, Harris, Jessica, Wheeler, Lawrie, Jamshidi, Ahmadreza, Vojdanian, Mahdi, Farhadi, Elham, Ahmadzadeh, Nooshin, Yüce, Zeynep, Dalkılıc, Ediz, Solmaz, Dilek, Akın, Berrin, Donmez, Salim, Sarı, İsmail, Leo, Paul J., Kenna, Tony J., Onen, Fatos, Mahmoudi, Mahdi, Brown, Matthew A., & Akkoc, Nurullah (2019) Genome-wide association study in Turkish and Iranian populations identify rare familial Mediterranean fever gene (MEFV) polymorphisms associated with ankylosing spondylitis. PLoS Genetics, 15(4), Article number: e1008038.
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Description
Ankylosing spondylitis (AS) is a highly heritable immune-mediated arthritis common in Turkish and Iranian populations. Familial Mediterranean Fever (FMF) is an autosomal recessive autoinflammatory disease most common in people of Mediterranean origin. MEFV, an FMF-associated gene, is also a candidate gene for AS. We aimed to identify AS susceptibility loci and also examine the association between MEFV and AS in Turkish and Iranian cohorts. We performed genome-wide association studies in 1001 Turkish AS patients and 1011 Turkish controls, and 479 Iranian AS patients and 830 Iranian controls. Serum IL-1β, IL-17 and IL-23 cytokine levels were quantified in Turkish samples. An association of major effect was observed with a novel rare coding variant in MEFV in the Turkish cohort (rs61752717, M694V, OR = 5.3, P = 7.63×10−12), Iranian cohort (OR = 2.9, P = 0.042), and combined dataset (OR = 5.1, P = 1.65×10−13). 99.6% of Turkish AS cases, and 96% of those carrying MEFV rs61752717 variants, did not have FMF. In Turkish subjects, the association of rs61752717 was particularly strong in HLA-B27-negative cases (OR = 7.8, P = 8.93×10−15), but also positive in HLA-B27-positive cases (OR = 4.3, P = 7.69×10−8). Serum IL-1β, IL-17 and IL-23 levels were higher in AS cases than controls. Among AS cases, serum IL-1β and IL-23 levels were increased in MEFV 694V carriers compared with non-carriers. Our data suggest that FMF and AS have overlapping aetiopathogenic mechanisms. Functionally important MEFV mutations, such as M694V, lead to dysregulated inflammasome function and excessive IL-1β function. As IL-1 inhibition is effective in FMF, AS cases carrying FMF-associated MEFV variants may benefit from such therapy.
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| ID Code: | 133127 | ||||||||||||
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| Item Type: | Contribution to Journal (Journal Article) | ||||||||||||
| Refereed: | Yes | ||||||||||||
| ORCID iD: |
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| Measurements or Duration: | 18 pages | ||||||||||||
| DOI: | 10.1371/journal.pgen.1008038 | ||||||||||||
| ISSN: | 1553-7404 | ||||||||||||
| Pure ID: | 33498646 | ||||||||||||
| Divisions: | Past > Institutes > Institute of Health and Biomedical Innovation | ||||||||||||
| Funding Information: | Funding was received for this study from Pfizer Inc. MAB was funded by a National Health and Medical Research Council (Australia) Senior Principal Research Fellowship. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. The authors would like to thank the AS patients and healthy controls who participated in this study for their contribution. We also thank Professor Arzu Sayıner and Professor Yusuf Baran, who kindly allowed use of their lab for sample preparation, and Miray Ünlü and Filiz Alkan, who performed DNA extraction and quantification. We are very grateful to Professor Francesco Ciccia for his helpful advice and comments about the study. We thank Dr David Pennisi for assistance with manuscript preparation. | ||||||||||||
| Copyright Owner: | Consult author(s) regarding copyright matters | ||||||||||||
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| Deposited On: | 27 Sep 2019 09:41 | ||||||||||||
| Last Modified: | 29 Nov 2025 01:59 |
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