Genetic Pleiotropy Between Mood Disorders, Metabolic, and Endocrine Traits in a Multigenerational Pedigree

Overview

Journal Transl Psychiatry

Specialties Psychiatry
Public Health

Date 2018 Oct 14

PMID 30315151

Citations 8

Authors

Rachel L Kember

Liping Hou

Xiao Ji

Lars H Andersen

Arpita Ghorai

Lisa N Estrella

Laura Almasy

Francis J McMahon

Christopher Brown

Maja Bucan

Affiliations

Soon will be listed here.

Abstract

Bipolar disorder (BD) is a mental disorder characterized by alternating periods of depression and mania. Individuals with BD have higher levels of early mortality than the general population, and a substantial proportion of this is due to increased risk for comorbid diseases. To identify the molecular events that underlie BD and related medical comorbidities, we generated imputed whole-genome sequence data using a population-specific reference panel for an extended multigenerational Old Order Amish pedigree (n = 394), segregating BD and related disorders. First, we investigated all putative disease-causing variants at known Mendelian disease loci present in this pedigree. Second, we performed genomic profiling using polygenic risk scores (PRS) to establish each individual's risk for several complex diseases. We identified a set of Mendelian variants that co-occur in individuals with BD more frequently than their unaffected family members, including the R3527Q mutation in APOB associated with hypercholesterolemia. Using PRS, we demonstrated that BD individuals from this pedigree were enriched for the same common risk alleles for BD as the general population (β = 0.416, p = 6 × 10). Furthermore, we find evidence for a common genetic etiology between BD risk and polygenic risk for clinical autoimmune thyroid disease (p = 1 × 10), diabetes (p = 1 × 10), and lipid traits such as triglyceride levels (p = 3 × 10) in the pedigree. We identify genomic regions that contribute to the differences between BD individuals and unaffected family members by calculating local genetic risk for independent LD blocks. Our findings provide evidence for the extensive genetic pleiotropy that can drive epidemiological findings of comorbidities between diseases and other complex traits.

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