Familial risk of Behçet’s disease among first-degree relatives: a population-based aggregation study in Korea

Author:

Ahn Hyeong Sik1ORCID,Kim Hyun Jung1,Kazmi Sayada Zartasha1,Kang Taeuk2,Jun Jae-Bum3,Kang Min Ji4,Kim Kyoung-Beom4,Kee Sun-Ho5,Kim Dong-Sook6,Hann Hoo Jae7

Affiliation:

1. Department of Preventive Medicine, College of Medicine, Korea University, Seoul, Korea

2. Korean Research-based Industry Association (KRPIA), Seoul, Korea

3. Department of Rheumatology, Hanyang University Hospital for Rheumatic Diseases, Seoul, Korea

4. Department Public Health, Graduate School, Korea University, Seoul, Korea

5. Department of Microbiology, College of Medicine, Korea University, Seoul, Korea

6. Health Insurance Review and Assessment service (HIRA), Seoul, Korea

7. Medical Research Institute, School of Medicine, Ewha Woman’s University, Seoul, Korea

Abstract

Abstract Objective Previous studies have indicated that Behçet’s disease (BD) has a genetic component, however population-level familial risk estimates are unavailable. We quantified the familial incidence and risk of BD in first-degree relatives (FDR) according to age, sex and type of family relationship. Methods Using the Korean National Health Insurance database, which has full population coverage and confirmed FDR information, we constructed a cohort of 21 940 795 individuals comprising 12 million families, which were followed for a familial occurrence of BD from 2002 to 2017. Age- and sex-adjusted incidence risk ratios for BD were calculated in individuals with affected FDR compared with those without affected FDR. Results Among the total study population, 53 687 individuals had affected FDR, of whom 284 familial cases developed BD with an incidence of 3.57/104 person-years. The familial risk (incidence) for BD was increased to 13.1-fold (2.71/104 person-years) in individuals with an affected father, 13.9-fold (3.11/104 person-years) with affected mother, 15.2-fold (4.9/104 person-years) with an affected sibling and the highest risk was 165-fold (46/104 person-years) with an affected twin. Familial risks showed age dependence, being higher in younger age groups. The sex-specific familial risk was similar in males and females. Conclusion This study provides quantified estimates of familial incidence and risk in FDR of BD patients in an entire population. Familial risks were higher within generation (sibling–sibling) vs between generations (parent–offspring). This implicates complex interactions between genetic factors and shared childhood environmental exposures in the pathogenesis of BD.

Publisher

Oxford University Press (OUP)

Subject

Pharmacology (medical),Rheumatology

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