Are minor alleles more likely to be risk alleles?

Takashi Kido; Weronika Sikora-Wohlfeld; Minae Kawashima; Shinichi Kikuchi; Naoyuki Kamatani; Anil Patwardhan; Richard Chen; Marina Sirota; Keiichi Kodama; Dexter Hadley; Atul J. Butte

doi:10.1186/s12920-018-0322-5

BMC Medical Genomics (Jan 2018)

Are minor alleles more likely to be risk alleles?

Takashi Kido,
Weronika Sikora-Wohlfeld,
Minae Kawashima,
Shinichi Kikuchi,
Naoyuki Kamatani,
Anil Patwardhan,
Richard Chen,
Marina Sirota,
Keiichi Kodama,
Dexter Hadley,
Atul J. Butte

Affiliations

Takashi Kido: Rikengenesis Co., Ltd.
Weronika Sikora-Wohlfeld: Division of Systems Medicine, Department of Pediatrics, Stanford University
Minae Kawashima: Department of Human Genetics, Graduate School of Medicine, The University of Tokyo
Shinichi Kikuchi: AI System Department, DeNA, Inc.
Naoyuki Kamatani: StaGen Inc.
Anil Patwardhan: Personalis, Inc.
Richard Chen: Personalis, Inc.
Marina Sirota: Institute for Computational Health Sciences, University of California
Keiichi Kodama: Institute for Computational Health Sciences, University of California
Dexter Hadley: Institute for Computational Health Sciences, University of California
Atul J. Butte: Institute for Computational Health Sciences, University of California

DOI: https://doi.org/10.1186/s12920-018-0322-5
Journal volume & issue: Vol. 11, no. 1
pp. 1 – 11

Abstract

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Abstract Background Genome-wide association studies (GWASs) have revealed relationships between over 57,000 genetic variants and diseases. However, unlike Mendelian diseases, complex diseases arise from the interplay of multiple genetic and environmental factors. Natural selection has led to a high tendency of risk alleles to be enriched in minor alleles in Mendelian diseases. Therefore, an allele that was previously advantageous or neutral may later become harmful, making it a risk allele. Methods Using data in the NHGRI-EBI Catalog and the VARIMED database, we investigated whether (1) GWASs more easily detect risk alleles and (2) facilitate evolutionary insights by comparing risk allele frequencies of different diseases. We conducted computer simulations of P-values for association tests when major and minor alleles were risk alleles. We compared the expected proportion of SNVs whose risk alleles were minor alleles with the observed proportion. Results Our statistical results revealed that risk alleles were enriched in minor alleles, especially for variants with low minor allele frequencies (MAFs 50% risk alleles were minor alleles because of the larger difference in the power of GWASs to differentiate between minor and major alleles, especially with low MAFs or when the number of controls exceeds the number of cases. However, the observed ratios between minor and major alleles in low MAFs (< 0.1) were much larger than the expected ratios of GWAS’s power imbalance, especially for diseases whose average risk allele frequencies were low, such as myopia, sudden cardiac arrest, and systemic lupus erythematosus. Conclusions Minor alleles are more likely to be risk alleles in the published GWASs on complex diseases. One reason is that minor alleles are more easily detected as risk alleles in GWASs. Even when correcting for the GWAS’s power imbalance, minor alleles are more likely to be risk alleles, especially in some diseases whose average risk allele frequencies are low. These analyses serve as a starting point for future studies on quantifying the degree of negative natural selection in various complex diseases.

Published in BMC Medical Genomics

ISSN: 1755-8794 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine; Science: Biology (General): Genetics
Website: https://bmcmedgenomics.biomedcentral.com

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