Effect of monoamine oxidase B A644G variant on nicotine dependence and/or schizophrenia risk

Pehlıvan, Sacide; Aydin, Pınar; Uysal, Mehmet Atilla; Ciftci, Hayriye Senturk; Sever, Ulgen; Yavuz, F. K.

doi:10.1590/0101-60830000000186

Cited by 4 publications

(3 citation statements)

References 26 publications

(25 reference statements)

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“…In line with this finding, MAOB rs1799836 was not related to autism in children [ 62 , 63 ], severe agitation in patients with schizophrenia, CD, PTSD [ 23 , 30 ], anger-related traits and aggression in suicidal participants and controls [ 64 ], aggression determined using the Brown–Goodwin questionnaire [ 65 ], alcohol dependence [ 18 ], positive symptoms in schizophrenia [ 66 ], or negative emotionality in healthy subjects [ 67 ]. In contrast to our data, a moderate association of the G allele with higher scores on the Spontaneous Aggression subscale from the Freiburg Aggression Scale in alcohol-dependent patients [ 17 ], and the association with the development of schizophrenia in Han Chinese patients [ 68 ], but not in Turkish patients [ 69 ], was reported. MAOB rs1799836 might not be directly associated with CD or with delinquent behavior, but in a haplotype analysis with other polymorphisms, such as MAOA rs6323T [ 68 ] or MAOB rs1799836, rs10521432, rs6651806, and rs590551 [ 67 ], it might show significant association with altered behaviors.…”

Section: Discussioncontrasting

confidence: 99%

Detention in Juvenile Correctional Facilities Is Associated with Higher Platelet Monoamine Oxidase B Activity in Males

et al. 2020

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Juvenile delinquency is related to several biological factors, yet very few vulnerability biomarkers have been identified. Previous data suggest that the enzyme monoamine oxidase B (MAO-B) influences several personality traits linked to the propensity to engage in delinquent behavior. Building on this evidence, we assessed whether conduct disorder (CD), juvenile delinquency adjudications, or detention in a correctional facility were associated with either platelet MAO-B activity or the MAOB rs1799836 polymorphism. The study enrolled 289 medication-free male youths, including 182 individuals detained in a correctional facility (with or without a diagnosis of CD). Of the remaining 107 participants, 26 subjects had a diagnosis of CD, and 81 were mentally healthy controls. Platelet MAO-B activity was determined by spectrophotofluorometry, while MAOB rs1799836 was genotyped using qPCR. Platelet MAO-B activity, corrected for age and smoking, was significantly higher in juvenile detainees (p < 0.001), irrespective of CD diagnosis. MAOB rs1799836 was not associated with platelet MAO-B activity or with detention in a correctional facility, CD diagnosis, or delinquent behavior. These data suggest that detention in a juvenile correctional facility increases platelet MAO-B activity in male adolescents. Future studies are needed to determine the mechanisms and functional significance of MAO-B peripheral elevation in juvenile male detainees.

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Section: Discussioncontrasting

confidence: 99%

Detention in Juvenile Correctional Facilities Is Associated with Higher Platelet Monoamine Oxidase B Activity in Males

et al. 2020

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“…Regarding variations in the MAOB gene, the A allele of the MAOB rs1799836 polymorphism (A> G) is associated with a lower risk of heavy smoking in men 72 . However, this association is contradicted by other studies 66,105 . Interactions between this SNP with other polymorphisms seem to interfere with the risk of smoking 70,73 .…”

Section: Polymorphisms Of the Maoa And Maob Genesmentioning

confidence: 59%

Genetic variability in the neurobiology of nicotine dependence: effects on smoking behavior

et al. 2023

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Background: Smoking dependence is a chronic disease and a public health problem. The neurobiology of nicotine addiction can explain smoking behavior. This system has genetic variability that has been associated with vulnerability to dependence. Genetic variability in the neurobiology of smoking can help to understand why individuals exposed to drugs may or may not become addicted. Objective: This study aims to address genetic variability in the neurobiology of smoking addiction with a focus on polymorphic genes related to the nicotinic response and the dopaminergic reward pathway. Method: This work involved a search of the main scientific research on genetic variability in the neurobiology of smoking and its effects on smoking behavior. One hundred and five studies were selected, most of which highlighted polymorphisms in the genes of nicotinic receptors, dopamine receptors, and nicotine metabolism. Results: The majority of studies have focused on genes related to the activation of the dopaminergic reward system by nicotine. Combinations between different polymorphisms were also highlighted, showing that interactions can determine a genetic profile of predisposition to smoking addiction. Additionally, gender and ethnicity were identified as relevant factors. Conclusion: Knowledge of the genetic bases involved in the individual response to smoking can enable a better understanding of inter-individual differences in smoking behavior, and contribute to improving the treatment of addiction.

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“…Catecholamine neurotransmitters, such as dopamine, are found in the brain [ 186 ]. Parkinson's disease, schizophrenia, obsessive-compulsive disorder, bipolar disorder, and hyperactivity-hyperactivity disorder are only a few of the CNS illnesses where dopamine plays a major role [ 187 , 188 ]. D1 and D2 dopamine receptors are two subclasses of G protein-coupled receptors (GPCRs), which are responsible for the action of dopamine.…”

Section: Treatment Of Psychiatric Disordersmentioning

confidence: 99%

Insights into the Promising Prospect of G Protein and GPCR-Mediated Signaling in Neuropathophysiology and Its Therapeutic Regulation

Rahman

Islam

Mim

et al. 2022

Oxidative Medicine and Cellular Longevity

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G protein-coupled receptors (GPCRs) are intricately involved in the conversion of extracellular feedback to intracellular responses. These specialized receptors possess a crucial role in neurological and psychiatric disorders. Most nonsensory GPCRs are active in almost 90% of complex brain functions. At the time of receptor phosphorylation, a GPCR pathway is essentially activated through a G protein signaling mechanism via a G protein-coupled receptor kinase (GRK). Dopamine, an important neurotransmitter, is primarily involved in the pathophysiology of several CNS disorders; for instance, bipolar disorder, schizophrenia, Parkinson’s disease, and ADHD. Since dopamine, acetylcholine, and glutamate are potent neuropharmacological targets, dopamine itself has potential therapeutic effects in several CNS disorders. GPCRs essentially regulate brain functions by modulating downstream signaling pathways. GPR6, GPR52, and GPR8 are termed orphan GPCRs because they colocalize with dopamine D1 and D2 receptors in neurons of the basal ganglia, either alone or with both receptors. Among the orphan GPCRs, the GPR52 is recognized for being an effective psychiatric receptor. Various antipsychotics like aripiprazole and quetiapine mainly target GPCRs to exert their actions. One of the most important parts of signal transduction is the regulation of G protein signaling (RGS). These substances inhibit the activation of the G protein that initiates GPCR signaling. Developing a combination of RGS inhibitors with GPCR agonists may prove to have promising therapeutic potential. Indeed, several recent studies have suggested that GPCRs represent potentially valuable therapeutic targets for various psychiatric disorders. Molecular biology and genetically modified animal model studies recommend that these enriched GPCRs may also act as potential therapeutic psychoreceptors. Neurotransmitter and neuropeptide GPCR malfunction in the frontal cortex and limbic-related regions, including the hippocampus, hypothalamus, and brainstem, is likely responsible for the complex clinical picture that includes cognitive, perceptual, emotional, and motor symptoms. G protein and GPCR-mediated signaling play a critical role in developing new treatment options for mental health issues, and this study is aimed at offering a thorough picture of that involvement. For patients who are resistant to current therapies, the development of new drugs that target GPCR signaling cascades remains an interesting possibility. These discoveries might serve as a fresh foundation for the creation of creative methods for pharmacologically useful modulation of GPCR function.

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Effect of monoamine oxidase B A644G variant on nicotine dependence and/or schizophrenia risk

Cited by 4 publications

References 26 publications

Detention in Juvenile Correctional Facilities Is Associated with Higher Platelet Monoamine Oxidase B Activity in Males

Detention in Juvenile Correctional Facilities Is Associated with Higher Platelet Monoamine Oxidase B Activity in Males

Genetic variability in the neurobiology of nicotine dependence: effects on smoking behavior

Insights into the Promising Prospect of G Protein and GPCR-Mediated Signaling in Neuropathophysiology and Its Therapeutic Regulation

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