Abstract
Offspring of depressed parents are at risk for depression and recent evidence suggests that reduced positive affect (PA) may be a marker of risk. We investigated whether self-reports of PA and fMRI-measured striatal response to reward, a neural correlate of PA, are reduced in adolescent youth at high familial risk for depression (HR) relative to youth at low familial risk for depression (LR). Functional magnetic resonance imaging assessments were conducted with 14 HR and 12 LR youth. All youth completed an ecological momentary assessment protocol to measure PA in natural settings and a self-report measure of depression symptomatology. Analyses found that HR youth demonstrated lower striatal response than LR youth during both reward anticipation and outcome. However, after controlling for youth self-reports of depression, HR youth demonstrated lower striatal response than LR youth only during reward anticipation. No significant differences were found between HR and LR youth on subjective ratings of PA or depressive symptoms. Results are consistent with previous findings that reduced reward response is a marker of risk for depression, particularly during reward anticipation, even in the absence of (or accounting for) disrupted subjective mood. Further examinations of prospective associations between reward response and depression onset are needed.
Highlights
Offspring of depressed parents are at risk for developing depressive disorders (Lieb et al, 2002; Hammen et al., 2004; Klein et al, 2005; Goodman et al, 2011) and other functional impairments (Beardslee et al, 1998; Lewinsohn et al, 2005)
Arguments have been made that low levels of positive affect (PA) may serve as a vulnerability marker or endophenotype for depression (Meehl, 1975, 2001; Hasler et al, 2004)
Previous work using behavioral observations of young children have suggested that low levels of PA differentiates between youth at high- and low risk for unipolar depression (Durbin et al, 2005; Olino et al, 2011)
Summary
Offspring of depressed parents are at risk for developing depressive disorders As the high-risk girls in Gotlib et al had significantly higher (albeit sub-syndromal) levels of depressive symptoms than the low-risk girls, it is possible that current symptoms, rather than high-risk status, may have driven the results This seminal work examining differences between youth at high- and low-familial risk for depression has provided support for the hypothesis that reward-system alterations are present before the onset of depression. As youth at high-risk for depression often demonstrate higher levels of depressive symptoms than peers, it is important to consider state effects of youth symptoms on brain functioning This can provide additional leverage for understanding whether family history is directly or indirectly influencing youth outcomes. We hypothesize that offspring at high-risk for depression will demonstrate reduced PA and rewardrelated brain functioning relative to low-risk offspring and that these differences will persist after accounting for individual differences in subjective reports of depressive symptomatology
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