Polygenic Risk for Depression is Associated with the Severity and Rate of Change in Depressive Symptoms Across Adolescence

Kwong, Alex S. F.; Morris, Tim; Pearson, Rebecca; Timpson, Nicholas J.; Rice, Frances; Stergiakouli, Evie; Tilling, Kate

doi:10.1101/2019.12.31.19016212

Cited by 3 publications

(4 citation statements)

References 68 publications

(102 reference statements)

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“…We observed significant positive associations between depression PRS and phenotypic depression. This finding is consistent with previous work linking higher polygenic loading for MDD with elevated depressive symptoms during adolescence in European-ancestry populations (Kwong et al, 2019(Kwong et al, , 2020Rice et al, 2019). Notably, the depression PRS accounted for between 1.5%-2.5% of the variance in past year MDD and MDE, paralleling the amount of variance explained in European samples (1.5%-3.2%) (Howard et al, 2019).…”

Section: Discussionsupporting

confidence: 91%

“…Extant work has indicated that depression PRS were associated with childhood-persistent depression and early-adult onset depression in a predominantly European-ancestry sample (Kwong et al, 2019). Other work has shown that a depression PRS was associated with increasing and high depressive symptoms across childhood and adolescence (Lussier et al, 2020) and a steep increase in depressive symptoms in adolescence and young adulthood (Kwong et al, 2020) in Europeanancestry samples. Additional research has indicated that in a European-ancestry sample, depression PRS were associated with late adolescent depression, but not low or early-onset adolescent depression (Rice et al, 2019).…”

Section: Introductionmentioning

confidence: 99%

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Depression polygenic scores are associated with major depressive disorder diagnosis and depressive episode in Mexican adolescents

Rabinowitz

Campos

Benjet

et al. 2020

Preprint

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Objective. Large-scale genome-wide association studies have uncovered genetic variants associated with depression; however, most of this work has been limited to adults of European ancestry. We investigate the ability of depression polygenic risk scores (PRS) to predict both lifetime and past year major depressive disorder (MDD) diagnosis and the experience of a major depressive episode (MDE) in a sample of adolescents with admixed ancestry from Mexico City, and explore whether adverse life events moderate these relations. Methods. The study sample consisted of adolescents (N=1,152) aged 12-17 from Mexico City who were interviewed and genotyped as part of a general population survey on adolescent mental health. PRS for depression were derived using summary statistics from a large-scale discovery genome-wide association study (GWAS) conducted on depressive symptoms that included over 800,000 individuals of European ancestry (Howard et al., 2019). Results. Higher depression PRS were associated with a higher likelihood of both past year MDD and MDE and lifetime MDE, accounting for 1.5%-2.5% of the variance in these outcomes. Adversity did not moderate the relationship between depression PRS and lifetime or past year MDD or MDE. Limitations. This study is cross-sectional. As such, a few participants might have experience MDD/MDE after the interview. In addition, our sample comprised only Mexican youth and thus it may not generalize to other populations. Conclusions. Our results indicate that depression PRS derived from a European ancestry GWAS are associated with MDD and MDE risk among Mexican adolescents and have the potential to aid in the identification of youth who may be genetically prone to developing depressive symptoms.

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Section: Discussionsupporting

confidence: 91%

Section: Introductionmentioning

confidence: 99%

Depression polygenic scores are associated with major depressive disorder diagnosis and depressive episode in Mexican adolescents

Rabinowitz

Campos

Benjet

et al. 2020

Preprint

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“…At ages 9 to 12 girls and caregivers were asked about depression symptoms in the past month, and at ages 13 and older were asked about symptoms in the past month and past year. Participants were classified as having had MDD if they met DSM-IV criteria at any study visit by combined parent and child report (n=58; n=31 met criteria at ages 9-14; n=27 met criteria at ages [16][17][18][19][20]. Participants with MDD did not differ from those without MDD on sociodemographic variables (race, pubertal timing or tempo, and financial strain), age, or the number of fMRI scans (Table 1).…”

Section: Assessment Of Depressionmentioning

confidence: 99%

“…The peak incidence for MDD occurs during adolescence [16][17][18] , especially for girls 19 . Adolescence is also a developmental period in which reward-related activation, particularly of the VS, changes and peaks [20][21][22] .…”

Section: Introductionmentioning

confidence: 99%

Accelerated neurodevelopment of reward anticipation processing in adolescent girls with depression

Baranger,

Lindenmuth,

Yoon

et al. 2023

Preprint

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Objective To test the hypothesis that depression is associated with differential neurodevelopment of reward circuitry in adolescence. Methods Adolescent girls (N=183, 58 with MDD in early or late adolescence) underwent MRI scans from ages 16-20 (1-4 scans/participant, 477 scans total) and completed a card-guessing fMRI task with monetary rewards. Mixed-effect models tested the effect of age and the moderating effect of MDD on whole-brain regional activation during reward anticipation. Results Eighty of 414 regions showed age effects (pFDR<0.05), consisting primarily of increasing activation with increasing age. Most significant regions were in dorsal attention, salience, and somatomotor networks, and also included the bilateral putamen, pallidum, and right nucleus accumbens. MDD moderated age effects in 40 regions (pFDR<0.05), including the right putamen, medial orbitofrontal cortex, and amygdala, and regions in control and dorsal attention networks. MDD x linear and quadratic age effects were negative, suggesting that MDD was associated with accelerated neurodevelopment. Conclusions Theories of reward processing's contribution to adolescent risk for depression focus primarily on core reward regions, yet a host of regions beyond these continue to develop during late adolescence. Findings demonstrate differing regional patterns of age-related changes in relation to MDD in girls, suggesting that depression involves disruption of a wide range of regions during reward anticipation processing across adolescence. Childhood and adolescent MDD is associated with accelerated neurodevelopment of attention and cognitive control regions during reward anticipation processing, which may have consequences both for cognitive function and the emergence of reward-system-specific disruptions.

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Early-life inflammatory markers and subsequent episodes of depression and psychotic experiences in the ALSPAC birth cohort

Edmondson-Stait

Shen

Adams

et al. 2022

Preprint

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Background Inflammation is implicated in depression and psychosis, including association of childhood inflammatory markers on the subsequent risk of developing symptoms. However, it is unknown whether early-life inflammatory markers are associated with the number of depressive and psychotic symptoms from childhood to adulthood. Methods Using the prospective Avon Longitudinal Study of Children and Parents birth cohort (N=up-to 6,401), we have examined longitudinal associations of early-life inflammation [exposures: interleukin-6 (IL-6), C-reactive protein (CRP) levels at age 9y; IL-6 and CRP DNA-methylation (DNAm) scores at birth and age 7y; and IL-6 and CRP polygenic risk scores (PRSs)] with the number of depressive episodes and psychotic experiences (PEs) between ages 10-28 years. Psychiatric outcomes were assessed using the Short Mood and Feelings Questionnaire and Psychotic Like Symptoms Questionnaires, respectively. Exposure-outcome associations were tested using negative binomial models, which were adjusted for metabolic and sociodemographic factors. Results Serum IL-6 levels at age 9y were associated with the total number of depressive episodes between 10-28y (n=4,262; β=0.086; 95%CI:0.036-0.137; pFDR=0.009). CRP DNAm score at birth was associated with total number of PEs, size but this association did not survive correction for multiple testing (n=822; β=0.204; 95%CI:0.024-0.388; p uncorrected=0.027; pFDR=0.252). Other immune measures were not associated with depression or PEs. Conclusions Early-life inflammatory markers are associated with the burden of depressive episodes and of PEs subsequently from childhood to adulthood. These findings support a potential role of early-life inflammation in the aetiology of depression and psychosis and highlight inflammation as a potential target for treatment and prevention.

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Polygenic Risk for Depression is Associated with the Severity and Rate of Change in Depressive Symptoms Across Adolescence

Cited by 3 publications

References 68 publications

Depression polygenic scores are associated with major depressive disorder diagnosis and depressive episode in Mexican adolescents

Depression polygenic scores are associated with major depressive disorder diagnosis and depressive episode in Mexican adolescents

Accelerated neurodevelopment of reward anticipation processing in adolescent girls with depression

Early-life inflammatory markers and subsequent episodes of depression and psychotic experiences in the ALSPAC birth cohort

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