Genetic sharing and heritability of paediatric age of onset autoimmune diseases

Authors

Yun R. Li, The Children's Hospital of Philadelphia
Sihai D. Zhao, University of Illinois Urbana-Champaign
Jin Li, The Children's Hospital of Philadelphia
Jonathan P. Bradfield, The Children's Hospital of Philadelphia
Maede Mohebnasab, The Children's Hospital of Philadelphia
Laura Steel, The Children's Hospital of Philadelphia
Julie Kobie, University of Pennsylvania Perelman School of Medicine
Debra J. Abrams, The Children's Hospital of Philadelphia
Frank D. Mentch, The Children's Hospital of Philadelphia
Joseph T. Glessner, The Children's Hospital of Philadelphia
Yiran Guo, The Children's Hospital of Philadelphia
Zhi Wei, The Children's Hospital of Philadelphia
John J. Connolly, The Children's Hospital of Philadelphia
Christopher J. Cardinale, The Children's Hospital of Philadelphia
Marina Bakay, The Children's Hospital of Philadelphia
Dong Li, The Children's Hospital of Philadelphia
S. Melkorka Maggadottir, The Children's Hospital of Philadelphia
Kelly A. Thomas, The Children's Hospital of Philadelphia
Haijun Qui, The Children's Hospital of Philadelphia

Document Type

Article

Publication Date

10-9-2015

Abstract

Autoimmune diseases (AIDs) are polygenic diseases affecting 7-10% of the population in the Western Hemisphere with few effective therapies. Here, we quantify the heritability of paediatric AIDs (pAIDs), including JIA, SLE, CEL, T1D, UC, CD, PS, SPA and CVID, attributable to common genomic variations (SNP-h 2). SNP-h 2 estimates are most significant for T1D (0.863±s.e. 0.07) and JIA (0.727±s.e. 0.037), more modest for UC (0.386±s.e. 0.04) and CD (0.454±0.025), largely consistent with population estimates and are generally greater than that previously reported by adult GWAS. On pairwise analysis, we observed that the diseases UC-CD (0.69±s.e. 0.07) and JIA-CVID (0.343±s.e. 0.13) are the most strongly correlated. Variations across the MHC strongly contribute to SNP-h 2 in T1D and JIA, but does not significantly contribute to the pairwise rG. Together, our results partition contributions of shared versus disease-specific genomic variations to pAID heritability, identifying pAIDs with unexpected risk sharing, while recapitulating known associations between autoimmune diseases previously reported in adult cohorts.

Identifier

84944245664 (Scopus)

Publication Title

Nature Communications

External Full Text Location

https://doi.org/10.1038/ncomms9442

e-ISSN

20411723

PubMed ID

26450413

Volume

6

Grant

P30AR070549

Fund Ref

Juvenile Diabetes Research Foundation International

Recommended Citation

Li, Yun R.; Zhao, Sihai D.; Li, Jin; Bradfield, Jonathan P.; Mohebnasab, Maede; Steel, Laura; Kobie, Julie; Abrams, Debra J.; Mentch, Frank D.; Glessner, Joseph T.; Guo, Yiran; Wei, Zhi; Connolly, John J.; Cardinale, Christopher J.; Bakay, Marina; Li, Dong; Maggadottir, S. Melkorka; Thomas, Kelly A.; and Qui, Haijun, "Genetic sharing and heritability of paediatric age of onset autoimmune diseases" (2015). Faculty Publications. 6723.
https://digitalcommons.njit.edu/fac_pubs/6723