Genome‐Wide Associations of Cognitive Domains and their Correlation with Polygenic Risk Scores for Antidepressant Response in Late‐Life Depression

多基因风险评分 萧条(经济学) 抗抑郁药 相关性 全基因组关联研究 认知 临床心理学 医学 心理学 精神科 生物 遗传学 基因 单核苷酸多态性 基因型 焦虑 几何学 数学 宏观经济学 经济
作者
Samar S. M. Elsheikh,Victoria S. Marshe,Małgorzata Maciukiewicz,Farhana Islam,Xiaoyu Men,Vanessa Goncalves,Daniel Felsky,James L. Kennedy,Benoit H. Mulsant,Charles F. Reynolds,Eric J. Lenze,Daniel Mueller
出处
期刊:Alzheimers & Dementia [Wiley]
卷期号:20 (S8)
标识
DOI:10.1002/alz.095772
摘要

Abstract Background Late‐life depression (LLD) often coincides with cognitive decline, impacting antidepressant treatment outcomes. Investigating the genetic profile of cognitive function and its association with antidepressant response in individuals with LLD is crucial. Method In the Incomplete Response in Late‐Life Depression: Getting to Remission (IRL‐GRey) study, 307 older adults with major depressive disorder underwent 12‐week venlafaxine treatment. A genome‐wide association study (GWAS) of five cognitive domains using the Repeatable Battery for the Assessment of Neuropsychological Status (RBANS) was conducted. Functional annotations were performed using FUMA. Polygenic risk scores (PRSs) for antidepressant non‐remission and symptom improvement were using PRSice v2. Associations between PRSs and cognitive domains were analyzed, adjusting for age, sex, and genomic principal components. Bonferroni correction and permutation tests were applied to address multiple testing issues. Result Out of the five cognitive domains, significant SNPs were identified for the attention domain (lead SNP rs67854110, beta = ‐9.91, CI = [‐13.12, ‐6.70], P = 4.4e −09 ). Top suggestive genes associated with language showed differential expression in the hypothalamus, cortex, and nucleus accumbens (P bon = 0.001). The language gene set analysis exhibited significant enrichment with the GWAS Catalog set response to cognitive‐behavioral therapy in depression (P = 9.24e −11 ). Additionally, the top SNP associated with delayed memory (rs13087568, beta = ‐8.24, CI = [‐11.36, ‐5.11], P = 4.5e −07 ) was previously linked to depressive symptoms by other studies. Polygenic risk scores (PRS) for non‐remission negatively correlated with attention (P Threshold = 0.0001, N SNPS = 39, OR = 0.105 [0.016, 0.686], P = 0.019), immediate memory (P Threshold = 0.001, N SNPS = 320, OR = 0.074 [0.011, 0.490], P = 0.0072), and delayed memory (P Threshold = 0.01, N SNPS = 2449, OR = 0.107 [0.021, 0.540], P = 0.0074). PRS for symptom improvement showed a positive correlation with delayed memory (PThreshold = 0.001, N SNPS = 385, OR = 5.329 [1.056, 26.885], P = 0.044). However, none of the PRS associations survived the Bonferroni threshold. Conclusion These findings suggest a genetic link between cognitive domains and antidepressant response in LLD, reinforcing previous associations. Understanding genetic contributions to cognitive decline in older adults with depression could aid in early identification and interventions to prevent dementia.

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