Family-based and association studies of monoamine oxidase A and attention deficit hyperactivity disorder (ADHD): preferential transmission of the long promoter-region repeat and its association with impaired performance on a continuous performance test (TOVA)

Manor, Iris; Tyano, Samuel; Mel, Elena Prado; Eisenberg, Jacques; Bachner‐Melman, Rachel; Kotler, Moshe; Ebstein, Richard P.

doi:10.1038/sj.mp.4001037

Cited by 118 publications

(104 citation statements)

References 62 publications

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“…This finding is not inconsistent with previously published results of a significant main effect of the high-activity MAOA genotype on increasing risk for antisocial behavior and ADHD. [59][60][61] Moreover, closer inspection of other G Â E studies involving the MAOA polymorphism reveals similar findings, albeit at marginally significant levels. 3,6,7 For instance, Foley et al 6 found a nonsignificant trend (P < 0.14) for the high-activity MAOA allele increasing risk for conduct disorder; after adjusting for the interaction between the MAOA polymorphism and maltreatment, the main effect became significant (P = 0.04).…”

Section: Discussionsupporting

confidence: 58%

MAOA, maltreatment, and gene–environment interaction predicting children's mental health: new evidence and a meta-analysis

et al. 2006

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Previous research on adults has shown that a functional polymorphism in the promoter region of the monoamine oxidase A (MAOA) gene moderates the impact of childhood maltreatment on risk for developing antisocial behavior. Thus far, attempts to replicate this finding have been mixed. The current study (i) presents new data investigating this finding in a sample of 975 seven-year-old boys, and (ii) evaluates the extant data by conducting a meta-analysis of published findings. We replicated the original finding by showing that the MAOA polymorphism moderates the development of psychopathology after exposure to physical abuse, we extended the finding to childhood closer in time to the maltreatment experience, and we ruledout the possibility of a spurious finding by accounting for passive and evocative geneenvironment correlation. Moreover, meta-analysis demonstrated that across studies, the association between maltreatment and mental health problems is significantly stronger in the group of males with the genotype conferring low vs high MAOA activity. These findings provide the strongest evidence to date suggesting that the MAOA gene influences vulnerability to environmental stress, and that this biological process can be initiated early in life. Molecular Psychiatry (2006) 11, 903-913.

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Section: Discussionsupporting

confidence: 58%

MAOA, maltreatment, and gene–environment interaction predicting children's mental health: new evidence and a meta-analysis

et al. 2006

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“…A high rate of similarity between the carrier state of the parents and their children was also observed by others, (28) but inheritance of risk alleles for ADHD is a complex process as there seems to be a preferential transmission of paternal over maternal alleles (28,29).…”

Section: Discussionsupporting

confidence: 67%

ADHD risk alleles associated with opiate addiction: study of addicted parents and their children

et al. 2016

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Background: Polymorphisms in genes such as DAT1, 5HTTLPR, D4DR4, and MAO-A have been linked to attention deficit hyperactivity disorder (ADHD) and susceptibility for opiate addiction. We investigated in opiate-addicted parents and their children the rate of ADHD and genetic markers that could predict susceptibility to ADHD and/or opiate addiction. Methods: We studied 64 heroin-addicted, methadone-maintained parents, and their 94 children who had or had not been exposed prenatally to opiates. DNA extracted from mouthwash was assessed for genetic polymorphism for six polymorphic sites of four different genes. Study subjects also filled a variety of questionnaires assessing the rate of ADHD in the parents and children and the children's intelligence quotient. results: Children of opiate-dependent mothers had a higher rate of ADHD compared to those of the opiate-dependent fathers. Opiate-dependent parents have a high risk of being carriers of most risk alleles examined except DRD4EX3 (allele 7). There was no difference whether the addicted parents had or did not have ADHD. conclusions: Serotonergic and dopaminergic risk alleles seem to be mainly related to opiate dependence with no effect on the occurrence of ADHD. People carrying those polymorphisms are susceptible to opioid addiction and not necessarily to ADHD.

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“…30 Dysregulation of monoamine pathways has long been implicated as one of the mechanisms involved in the etiology of ADHD. Several groups [31][32][33][34][35][36] have set out to test whether MAOA confers risk for ADHD, however, definite conclusion has not yet been received. Our data may serve as a support for previous positive reports of linkage/association for MAOA, especially in Chinese Han population.…”

Section: Discussionmentioning

confidence: 99%

A high-density single-nucleotide polymorphism screen of 23 candidate genes in attention deficit hyperactivity disorder: suggesting multiple susceptibility genes among Chinese Han population

et al. 2008

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Attention deficit hyperactivity disorder (ADHD) is a common childhood-onset behavioral disorder with a definite genetic component. The search for genes predisposing to ADHD has focused on genes involved in the regulation of monoamine systems. In this study, we emphasized genes that underlie various aspects of dopamine, norepinephrine and serotonin neurotransmissions and performed a comprehensive association analysis by screening with 245 single-nucleotide polymorphisms (SNPs) of 23 candidate genes in a sample of Chinese Han descent. A total of 182 DSM-IV ADHD children and 184 healthy controls were genotyped and analyzed with an average density of one SNP every 6.1 kb. Both single-SNP and multimarker haplotype analyses were implemented to exploit association signal for ADHD and its diagnostic subtypes. Empirical P-values were derived on the basis of 5000 permutations to evaluate gene-wide statistical significance. MAOA yielded highly suggestive evidence of association (empirical P < 0.01, OR = 1.94) with ADHD. For inattentive ADHD, MAOA, DDC and SYP showed suggestive evidence of association (empirical P < 0.05). ADRA2C achieved suggestive significance (empirical P < 0.05) for ADHD combined type. Additionally, for six genes (SNAP25, NET1, DBH, CHRNA4, DRD3 and SYT1) we detected one or more SNPs with nominal P-valuesp0.05. This study has identified several genes as promising susceptibility loci for ADHD. Replication efforts and further investigations remain necessary to provide definite proof of association.

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Family-based and association studies of monoamine oxidase A and attention deficit hyperactivity disorder (ADHD): preferential transmission of the long promoter-region repeat and its association with impaired performance on a continuous performance test (TOVA)

Cited by 118 publications

References 62 publications

MAOA, maltreatment, and gene–environment interaction predicting children's mental health: new evidence and a meta-analysis

MAOA, maltreatment, and gene–environment interaction predicting children's mental health: new evidence and a meta-analysis

ADHD risk alleles associated with opiate addiction: study of addicted parents and their children

A high-density single-nucleotide polymorphism screen of 23 candidate genes in attention deficit hyperactivity disorder: suggesting multiple susceptibility genes among Chinese Han population

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