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Genetic heterogeneity and subtypes of major depression

遗传力 遗传相关 遗传异质性 SNP公司 全基因组关联研究 相关性 萧条(经济学) 队列 医学 生物 遗传变异 遗传学 遗传关联 基因 单核苷酸多态性 表型 基因型 内科学 宏观经济学 数学 经济 几何学
作者
Thuy-Dung Nguyen,Arvid Harder,Ying Xiong,Kaarina Kowalec,Sara Hägg,Na Cai,Ralf Kuja‐Halkola,Christina Dalman,Patrick F. Sullivan,Yi Lu
标识
DOI:10.1101/2021.03.05.21252911
摘要

ABSTRACT Major depression (MD) is a heterogeneous disorder; however, the extent to which genetic factors distinguish MD patient subgroups (genetic heterogeneity) remains uncertain. This study sought evidence for genetic heterogeneity in MD. Using UK Biobank cohort, the authors defined 16 MD subtypes within eight comparison groups (vegetative symptoms, symptom severity, comorbid anxiety disorder, age at onset, recurrence, suicidality, impairment and postpartum depression; N∼3 000-47 000). To compare genetic component of these subtypes, subtype-specific genome-wide association studies were performed to estimate SNP-heritability, and genetic correlations within subtype comparison and with other related disorders or traits. The findings indicated that MD subtypes were divergent in their SNP-heritability, and genetic correlations both within subtype comparisons and with other related disorders/traits. Three subtype comparisons (vegetative symptoms, age at onset, and impairment) showed significant differences in SNP-heritability; while genetic correlations within subtype comparisons ranged from 0.55 to 0.86, suggesting genetic profiles are only partially shared among MD subtypes. Furthermore, subtypes that are more clinically challenging, e.g., early-onset, recurrent, suicidal, more severely impaired, had stronger genetic correlations with other psychiatric disorders. MD with atypical-like features showed a positive genetic correlation ( + 0.40) with BMI while a negative correlation (−0.09) was found in those without atypical-like features. Novel genomic loci with subtype-specific effects were identified. These results provide the most comprehensive evidence to date for genetic heterogeneity within MD, and suggest that the phenotypic complexity of MD can be effectively reduced by studying the subtypes which share partially distinct etiologies.
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