Your search keyword '"Schwarte, Kathrin"' showing total 3 results

1. Association of FKBP5 genotype with depressive symptoms in patients with coronary heart disease: a prospective study.

Author

Brandt, Julia, Warnke, Katharina, Jörgens, Silke, Arolt, Volker, Beer, Katja, Domschke, Katharina, Haverkamp, Wilhelm, Kuhlmann, Stella L., Müller-Nordhorn, Jacqueline, Rieckmann, Nina, Schwarte, Kathrin, Ströhle, Andreas, Tschorn, Mira, Waltenberger, Johannes, and Grosse, Laura

Subjects

CORONARY disease, MENTAL depression, CARDIAC patients, SINGLE nucleotide polymorphisms, DYSLIPIDEMIA, GENOTYPES

Abstract

Depression and coronary heart disease (CHD) are prevalent and often co-occurring disorders. Both have been associated with a dysregulated stress system. As a central element of the stress system, the FKBP5 gene has been shown to be associated with depression. In a prospective design, this study aims to investigate the association of FKBP5 with depressive symptoms in CHD patients. N = 268 hospitalized CHD patients were included. Depressive symptoms were measured using the Hospital Anxiety and Depression Scale (HADS-D) at four time points (baseline, and after 1 month, 6 months, and 12 months). The functional FKBP5 single-nucleotide polymorphism (SNP) rs1360780 was selected for genotyping. Linear regression models showed that a higher number of FKBP5 C alleles was associated with more depressive symptoms in CHD patients both at baseline (p = 0.015) and at 12-months follow-up (p = 0.025) after adjustment for confounders. Further analyses revealed that this effect was driven by an interaction of FKBP5 genotype with patients' prior CHD course. Specifically, only in patients with a prior myocardial infarction or coronary revascularization, more depressive symptoms were associated with a higher number of C alleles (baseline: p = 0.046; 1-month: p = 0.026; 6-months: p = 0.028). Moreover, a higher number of C alleles was significantly related to a greater risk for dyslipidemia (p =.016). Our results point to a relevance of FKBP5 in the association of the two stress-related diseases depression and CHD. [ABSTRACT FROM AUTHOR]

Published

2020

2. The role of BDNF methylation and Val66Met in amygdala reactivity during emotion processing.

Author

Redlich, Ronny, Schneider, Ilona, Kerkenberg, Nicole, Opel, Nils, Bauhaus, Jonas, Enneking, Verena, Repple, Jonathan, Leehr, Elisabeth J., Grotegerd, Dominik, Kähler, Claas, Förster, Katharina, Dohm, Katharina, Meinert, Susanne, Hahn, Tim, Kugel, Harald, Schwarte, Kathrin, Schettler, Christiane, Domschke, Katharina, Arolt, Volker, and Heindel, Walter

Subjects

METHYLATION, BRAIN-derived neurotrophic factor, SINGLE nucleotide polymorphisms, PERSONALITY questionnaires, DNA methylation

Abstract

Epigenetic alterations of the brain‐derived neurotrophic factor (BDNF) gene have been associated with psychiatric disorders in humans and with differences in amygdala BDNF mRNA levels in rodents. This human study aimed to investigate the relationship between the functional BDNF‐Val66Met polymorphism, its surrounding DNA methylation in BDNF exon IX, amygdala reactivity to emotional faces, and personality traits. Healthy controls (HC, n = 189) underwent functional MRI during an emotional face‐matching task. Harm avoidance, novelty seeking and reward dependence were measured using the Tridimensional Personality Questionnaire (TPQ). Individual BDNF methylation profiles were ascertained and associated with several BDNF single nucleotide polymorphisms surrounding the BDNF‐Val66Met, amygdala reactivity, novelty seeking and harm avoidance. Higher BDNF methylation was associated with higher amygdala reactivity (x = 34, y = 0, z = −26, t(166) = 3.00, TFCE = 42.39, p(FWE) =.045), whereby the BDNF‐Val66Met genotype per se did not show any significant association with brain function. Furthermore, novelty seeking was negatively associated with BDNF methylation (r = −.19, p =.015) and amygdala reactivity (r = −.17, p =.028), while harm avoidance showed a trend for a positive association with BDNF methylation (r =.14, p =.066). The study provides first insights into the relationship among BDNF methylation, BDNF genotype, amygdala reactivity and personality traits in humans, highlighting the multidimensional relations among genetics, epigenetics, and neuronal functions. The present study suggests a possible involvement of epigenetic BDNF modifications in psychiatric disorders and related brain functions, whereby high BDNF methylation might reduce BDNF mRNA expression and upregulate amygdala reactivity. [ABSTRACT FROM AUTHOR]

Published

2020

3. Association of Adenosine Receptor Gene Polymorphisms and In Vivo Adenosine A1 Receptor Binding in The Human Brain.

Author

Hohoff, Christa, Garibotto, Valentina, Elmenhorst, David, Baffa, Anna, Kroll, Tina, Hoffmann, Alana, Schwarte, Kathrin, Zhang, Weiqi, Arolt, Volker, Deckert, Jürgen, and Bauer, Andreas

Subjects

ADENOSINES, RADIOLIGAND assay, BRAIN diseases, POSITRON emission tomography, SINGLE nucleotide polymorphisms, GENETICS

Abstract

Adenosine A1 receptors (A1ARs) and the interacting adenosine A2A receptors are implicated in neurological and psychiatric disorders. Variants within the corresponding genes ADORA1 and ADORA2A were shown associated with pathophysiologic alterations, particularly increased anxiety. It is unknown so far, if these variants might modulate the A1AR distribution and availability in different brain regions. In this pilot study, the influence of ADORA1 and ADORA2A variants on in vivo A1AR binding was assessed with the A1AR-selective positron emission tomography (PET) radioligand [18F]CPFPX in brains of healthy humans. Twenty-eight normal control subjects underwent PET procedures to calculate the binding potential BPND of [18F]CPFPX in cerebral regions and to assess ADORA1 and ADORA2A single nucleotide polymorphism (SNP) effects on regional BPND data. Our results revealed SNPs of both genes associated with [18F]CPFPX binding to the A1AR. The strongest effects that withstood even Bonferroni correction of multiple SNP testing were found in non-smoking subjects (N=22) for ADORA2A SNPs rs2236624 and rs5751876 (corr. Pall<0.05). SNP alleles previously identified at risk for increased anxiety like the rs5751876 T-allele corresponded to consistently higher A1AR availability in all brain regions. Our data indicate for the first time that variation of A1AR availability was associated with ADORA SNPs. The finding of increased A1AR availability in regions of the fear network, particularly in ADORA2A risk allele carriers, strongly warrants evaluation and replication in further studies including individuals with increased anxiety. [ABSTRACT FROM AUTHOR]

Published

2014