Single-Nucleotide Polymorphism of the FKBP5 Gene and Childhood Maltreatment as Predictors of Structural Changes in Brain Areas Involved in Emotional Processing in Depression

Tozzi, Leonardo; Carballedo, Angela; Wetterling, Friedrich; McCarthy, Hazel; O’Keane, Veronica; Gill, Michael; Morris, Derrek; Fahey, Ciara; Meaney, James; Frodl, Thomas

doi:10.1038/npp.2015.170

Cited by 88 publications

(56 citation statements)

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“…Our finding, however, was that of gene-environment interaction, and thus adds to the growing literature supporting the role of FKBP5 in susceptibility to maltreatment and childhood trauma. While most studies implicating FKBP5 in vulnerability to maltreatment were conducted in adults (Bevilacqua et al, 2012;Fani et al, 2014;Buchmann et al, 2014;Tozzi et al, 2015), the present study suggests that this susceptibility may emerge early in life. The FKBP5 gene is differentially methylated in maltreated as opposed to non-maltreated children (Weder et al, 2014), this methylation is allele-specific (Klengel et al, 2013) which suggests that the underlying mechanism of this gene-environment interaction is epigenetic.…”

Section: Discussionmentioning

confidence: 60%

FKBP5 interacts with maltreatment in children with extreme, pervasive, and persistent aggression

Bryushkova

Zai

Sheng

et al. 2016

Psychiatry Research

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Section: Discussionmentioning

confidence: 60%

FKBP5 interacts with maltreatment in children with extreme, pervasive, and persistent aggression

Bryushkova

Zai

Sheng

et al. 2016

Psychiatry Research

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“…In this systematic review, neuroimaging alteration in MDD was found to be associated with FK506‐binding protein 51 (FKBP5) and corticotropin‐releasing hormone receptor 1 (CRHR1) genes . The dysfunction of glucocorticoid receptor and endogenous glucocorticoid levels impair the HPA axis feedback inhibition in depressed patients.…”

Section: Discussionmentioning

confidence: 99%

“…70,71 MDD patients with an MAOA H-allele showed significantly lower amygdalaprefrontal connectivity, 72 but not in those with 5-HTTLPR genetic variants. 70,73 Other studies have reported significant genotype-diagnosis interaction effects on emotional regulation systems for FKBP5, 74 CACNA1C, 75 CRHR1, 64 and BICCI 39 genes. The remaining studies showed decreased activation of the striatum with a PCLO risk allele, decreased activation of right frontal middle gyrus in a 5-HT2A T-allele, or decreased connectivity of amygdala-prefrontal circuitry with the MAOA H-allele.…”

Section: Genetic-neuroimaging Association Using Task-fmrimentioning

confidence: 98%

“…In this systematic review, neuroimaging alteration in MDD was found to be associated with FK506-binding protein 51 (FKBP5) and corticotropin-releasing hormone receptor 1 (CRHR1) genes. 64,74 The dysfunction of glucocorticoid receptor and endogenous glucocorticoid levels impair the HPA axis feedback inhibition in depressed patients. Abnormal glucocorticoid levels can inhibit neural proliferation and encourage dendritic atrophy, which in turn causes brain structural and functional alterations.…”

Section: Association Of Hpa Axis-related Genes With Neuroimagingmentioning

confidence: 99%

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Neuroimaging genomic studies in major depressive disorder: A systematic review

2018

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Genetic-neuroimaging studies could identify new potential endophenotypes of major depressive disorder (MDD). Morphological and functional alterations may be attributable to genetic factors that regulate neurogenesis and neurodegeneration. Given that the association between gene polymorphisms and brain morphology or function has varied across studies, this systematic review aims at evaluating and summarizing all available genetic-neuroimaging studies. Twenty-eight gene variants were evaluated in 64 studies by structural or functional magnetic resonance imaging. Significant genetic-neuroimaging associations were found in monoaminergic genes, BDNF genes, glutamatergic genes, HPA axis genes, and the other common genes, which were consistent with common hypotheses of the pathogenesis of MDD.

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“…Initial studies that combined a candidate gene approach with neuroimaging reported that specific single-nucleotide polymorphisms (SNPs) of genes associated with neuroplasticity and stress reactivity, including brain derived neurotrophic factor, glucocorticoid and oxytocin receptor sensitivity, confer greater sensitivity to the detrimental impact of ELS, e.g. pronounced reductions of limbic volumes (Dannlowski et al 2016;Tozzi et al 2016;van Velzen et al 2016). Interestingly, two initial studies reported that specific allelic combinations associated with differences in central dopamine and serotonergic functioning exhibited ELS-associated changes in hippocampal and amygdala activation that may reflect improved threat learning and implicit emotion regulation following early aversive experiences (Hermann et al 2012;van Rooij et al 2017).…”

Section: Introductionmentioning

confidence: 99%

Serotonin and early life stress interact to shape brain architecture and anxious avoidant behavior – a TPH2 imaging genetics approach

Liu¹,

Lei²,

Li³

et al. 2019

Preprint

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Serotonin regulates developmental and experience-dependent neuroplasticity in limbicprefrontal systems engaged in emotional reactivity and regulation. Tryptophan hydroxylase 2 (TPH2) regulates central serotonergic biosynthesis rates and transgenic animal models suggest that TPH2-associated changes in serotonergic signaling mediate the impact of early life stress (ELS) shaping a phenotype characterized by anxious avoidance. The present study employed an imaging genomics approach that capitalized on individual differences in a TPH2 polymorphism (703G/T; rs4570625) to determine whether differences in serotonergic signaling modulate the effects of ELS on brain structure and function and punishment sensitivity in humans (n = 252). Higher ELS exposure was associated with increased gray matter volumes in a circuitry spanning thalamic-limbic-prefrontal regions and decreased intrinsic communication in limbic-prefrontal circuits selectively in TT carriers. On the phenotype level, the genotype moderated the association between higher ELS exposure and higher punishment sensitivity. In TT carriers, the association between higher ELS exposure and punishment sensitivity was critically mediated by increased thalamic-limbic-prefrontal volumes. The present findings suggest that ELS shapes the neural organization of the thalamic-limbic-prefrontal circuits in interaction with individual variations in TPH2 to promote a phenotype characterized by facilitated threat avoidance, thus promoting early adaptation to an adverse environment.

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Single-Nucleotide Polymorphism of the FKBP5 Gene and Childhood Maltreatment as Predictors of Structural Changes in Brain Areas Involved in Emotional Processing in Depression

Cited by 88 publications

References 50 publications

FKBP5 interacts with maltreatment in children with extreme, pervasive, and persistent aggression

FKBP5 interacts with maltreatment in children with extreme, pervasive, and persistent aggression

Neuroimaging genomic studies in major depressive disorder: A systematic review

Serotonin and early life stress interact to shape brain architecture and anxious avoidant behavior – a TPH2 imaging genetics approach

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