Abstract
Children of alcoholics have increased risk for substance abuse problems. Self-medication of negative affect may be one developmental path to future substance abuse. Because the 146 young (adolescent) children of alcoholics in the current sample had not used enough abused substances to study substance use directly, the relation of substance abuse risk markers to negative affect was assessed. Because the D 2 dopamine receptor (DRD2) A 1 allele has been associated with alcoholism and other substance use disorders, negative affect, measured by the Beck Depression Inventory (BDI), was determined in four groups of children: boys and girls with the A 1 + allele (A 1A 1 and A 1A 2 genotypes) and with the A 1 − allele (A 2A 2 genotype). The other risk markers were stress, low amplitude of the P300 evoked potential, poor visuospatial functioning, novelty seeking (NS), and harm avoidance (HA). Stress was correlated with BDI scores in all groups. In contrast, low P300 was associated with BDI scores only in boys with the A 1 + allele ( P = .04), NS was associated with BDI scores only in girls with the A 1 + allele ( P = .02), and HA was associated with BDI scores only in boys with the A 1 − allele ( P = .01). In addition, boys with the A 1 + allele had lower BDI ( P = .05) and HA ( P = .005) scores than the respective scores for boys with the A 1 − allele. Girls with the A 1 − allele had lower HA scores compared with scores for boys with the A 1 − allele ( P = .02). Girls with the A 1 + allele had lower visuospatial functioning than that of boys with the A 1 + allele ( P<.001). Results indicate that both sex and DRD2 genotype modify associations between negative affect and other substance abuse risk markers.
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