Your search keyword '"Bettecken, T."' showing total 13 results

1. Next Generation Sequencing in der diagnostischen Praxis.

Author

Bettecken, T., Pfeufer, A., Sudbrak, R., Siddiqui, R., Franke, A., Wienker, T.F., and Krawczak, M.

Abstract

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Published

2014

2. Variants within the GABA transaminase (ABAT) gene region are associated with somatosensory evoked EEG potentials in families at high risk for affective disorders.

Author

Wegerer, M., Adena, S., Pfennig, A., Czamara, D., Sailer, U., Bettecken, T., Müller-Myhsok, B., Modell, S., and Ising, M.

Subjects

AFFECTIVE disorders, AMINOTRANSFERASES, MENTAL depression, ELECTROENCEPHALOGRAPHY, GENES, GENETIC polymorphisms, NEUROTRANSMITTERS, PSYCHOLOGICAL tests, REGRESSION analysis, SOMATOSENSORY evoked potentials, SYMPTOMS, DATA analysis software, DESCRIPTIVE statistics

Abstract

BackgroundDepression frequently co-occurs with somatization, and somatic complaints have been reported as a vulnerability marker for affective disorders observable before disease onset. Somatization is thought to result from an increased attention to somatic sensations, which should be reflected in long-latency somatosensory evoked electroencephalogram (EEG) potentials (SSEPs) at the physiological level. Previous studies revealed that SSEPs are altered in depressed patients and suggested late SSEP components as vulnerability markers for affective disorders. Neurotransmitters such as serotonin, γ-aminobutyric acid (GABA) and the neuropeptide substance P may play an important role for both affective disorders and somatosensory processing.MethodWe investigated the associations between SSEPs and polymorphisms within candidate genes of the serotonergic, GABAergic as well as the substance P system in subjects at high risk for affective disorders. The sample was composed of high-risk families participating in the Munich Vulnerability Study and genetic association analyses were calculated using qfam (family-based association tests for quantitative traits) implemented in PLINK 1.05.ResultsWe observed significant associations (false discovery rate <0.05) withstanding correction for multiple testing between late SSEP components (response strength 170–370 ms after stimulation) and four single nucleotide polymorphisms within the GABA transaminase (ABAT) gene region coding for a protein responsible for GABA degradation. No effects were found with the classical disease trait approach, suggesting SSEP marker specificity of the observed associations.ConclusionsOur findings point to a possible role of ABAT gene-regulated GABA catabolism for an altered processing of somatosensory stimuli as a potential vulnerability marker for affective disorders. [ABSTRACT FROM PUBLISHER]

Published

2013

3. Estimating the Age of the Most Common Italian GRN Mutation: Walking Back to Canossa Times.

Author

Benussi L, Rademakers R, Rutherford NJ, Wojtas A, Glionna M, Paterlini A, Albertini V, Bettecken T, Binetti G, and Ghidoni R

Published

2013

4. More CLEC16A gene variants associated with multiple sclerosis.

Author

Nischwitz, S., Cepok, S., Kroner, A., Wolf, C., Knop, M., Müller-Sarnowski, F., Pfister, H., Rieckmann, P., Hemmer, B., Ising, M., Uhr, M., Bettecken, T., Holsboer, F., Müller-Myhsok, B., and Weber, F.

Subjects

MULTIPLE sclerosis, NUCLEOTIDE sequence, GENETIC polymorphisms, INTRONS, GENE mapping, LINKAGE (Genetics), DNA replication

Abstract

Nischwitz S, Cepok S, Kroner A, Wolf C, Knop M, Müller-Sarnowski F, Pfister H, Rieckmann P, Hemmer B, Ising M, Uhr M, Bettecken T, Holsboer F, Müller-Myhsok B, Weber F. More CLEC16A gene variants associated with multiple sclerosis. Acta Neurol Scand: 2011: 123: 400-406. © 2010 John Wiley & Sons A/S. Recently, associations of several single-nucleotide polymorphisms (SNPs) within the CLEC16A gene with multiple sclerosis (MS), type-I diabetes, and primary adrenal insufficiency were reported. We performed linkage disequilibrium (LD) fine mapping with 31 SNPs from this gene, searching for the region of highest association with MS in a German sample consisting of 603 patients and 825 controls. Four SNPs located in intron 19 of the CLEC16A gene were found associated. We could replicate the finding for SNP rs725613 and were able to show for the first time the association of rs2041670, rs2080272 and rs998592 with MS. All described base polymorphisms are mapping to one LD block of approximately 50 kb within intron 19 of the CLEC16A gene, suggesting a pivotal role of this region for susceptibility of MS and possibly also for other autoimmune diseases. [ABSTRACT FROM AUTHOR]

Published

2011

5. Proteomic-based genotyping in a mouse model of trait anxiety exposes disease-relevant pathways.

Author

Ditzen, C., Varadarajulu, J., Czibere, L., Gonik, M., Targosz, B. S., Hambsch, B., Bettecken, T., Keßler, M. S., Frank, E., Bunck, M., Teplytska, L., Erhardt, A., Holsboer, F., Müller-Myhsok, B., Landgraf, R., and Turck, C. W.

Subjects

BIOMARKERS, ENOLASE, PHOSPHATASES, NUCLEOTIDES, AMINO acids

Abstract

In our biomarker identification efforts, we have reported earlier on a protein that differs in its electrophoretic mobility between mouse lines bred either for high or low trait anxiety. The altered electrophoretic behavior of enolase phosphatase (EP) is now identified to be caused by two single-nucleotide polymorphisms. In both cases, the genetic polymorphism introduces an amino acid change in the protein's sequence resulting in differential mobility on SDS gels. This was shown by recombinantly expressing the two EP isoforms. Functional studies indicate that the EP isoform from the high anxiety mouse line has a lower enzymatic activity than does its low anxiety mouse counterpart. EP is a member of the methionine salvage pathway that is responsible for the synthesis of S-adenosyl-L-methionine, a natural compound with potential antidepressant activities. In addition, it is linked to the polyamine pathway whose members have functions in anxiety/depression-related behaviors. In a freely-segregating F2 panel, both single-nucleotide polymorphisms were significantly associated with locomotion-independent trait anxiety, further supporting a functional role of EP for this phenotype. The study shows that proteomic analysis can reveal genotypic differences relevant for the phenotype. The identified protein alterations, in turn, can expose metabolic pathways pertinent to the behavioral phenotype. [ABSTRACT FROM AUTHOR]

Published

2010

6. The GABA transporter 1 (SLC6A1): a novel candidate gene for anxiety disorders.

Author

Thoeringer, C. K., Ripke, S., Unschuld, P. G., Lucae, S., Ising, M., Bettecken, T., Uhr, M., Keck, M. E., Mueller-Myhsok, B., Holsboer, F., Binder, E. B., and Erhardt, A.

Subjects

ANXIETY disorders, GABA, DISEASE susceptibility, GENES, PSYCHOLOGICAL stress

Abstract

Recent evidence suggests that the GABA transporter 1 (GAT-1; SLC6A1) plays a role in the pathophysiology and treatment of anxiety disorders. In order to understand the impact of genetic variation within SLC6A1 on pathological anxiety, we performed a case–control association study with anxiety disorder patients with and without syndromal panic attacks. Using the method of sequential addition of cases, we found that polymorphisms in the 5′ flanking region of SLC6A1 are highly associated with anxiety disorders when considering the severity of syndromal panic attacks as phenotype covariate. Analysing the effect size of the association, we observed a constant increase in the odds ratio for disease susceptibility with an increase in panic severity (OR ~ 2.5 in severely affected patients). Nominally significant association effects were observed considering the entire patient sample. These data indicate a high load of genetic variance within SLC6A1 on pathological anxiety and highlight GAT-1 as a promising target for treatment of anxiety disorders with panic symptoms. [ABSTRACT FROM AUTHOR]

Published

2009

7. IL2RA and IL7RA genes confer susceptibility for multiple sclerosis in two independent European populations.

Author

Weber, F., Fontaine, B., Cournu-Rebeix, I., Kroner, A., Knop, M., Lutz, S., Müller-Sarnowski, F., Uhr, M., Bettecken, T., Kohli, M., Ripke, S., Ising, M., Rieckmann, P., Brassat, D., Semana, G., Babron, M.-C., Mrejen, S., Gout, C., Lyon-Caen, O., and Yaouanq, J.

Subjects

MULTIPLE sclerosis diagnosis, GENETIC polymorphisms, INTERLEUKIN-2, LEUCOCYTES, IMMUNE response, SCIENTIFIC method

Abstract

Multiple sclerosis (MS) is the most common chronic inflammatory neurologic disorder diagnosed in young adults and, due to its chronic course, is responsible for a substantial economic burden. MS is considered to be a multifactorial disease in which both genetic and environmental factors intervene. The well-established human leukocyte antigen (HLA) association does not completely explain the genetic impact on disease susceptibility. However, identification and validation of non-HLA-genes conferring susceptibility to MS has proven to be difficult probably because of the small individual contribution of each of these genes. Recently, associations with two single nucleotide polymorphisms (SNPs) in the IL2RA gene (rs12722489, rs2104286) and one SNP in the IL7RA gene (rs6897932) have been reported by several groups. These three SNPs were genotyped in a French and a German population of MS patients using the hME assay by the matrix-assisted laser desorption/ionization time of flight technology (Sequenom, San Diego, CA, USA). We show that these SNPs do contribute to the risk of MS in these two unrelated European MS patient populations with odds ratios varying from 1.1 to 1.5. The discovery and validation of new genetic risk factors in independent populations may help toward the understanding of MS pathogenesis by providing valuable information on biological pathways to be investigated.Genes and Immunity (2008) 9, 259–263; doi:10.1038/gene.2008.14; published online 20 March 2008 [ABSTRACT FROM AUTHOR]

Published

2008

8. Family-based association study of serotonergic candidate genes and attention-deficit/hyperactivity disorder in a German sample.

Author

Heiser, P., Dempfle, A., Friedel, S., Konrad, K., Hinney, A., Kiefl, H., Walitza, S., Bettecken, T., Saar, K., Linder, M., Warnke, A., Herpertz-Dahlmann, B., Schäfer, H., Remschmidt, H., and Hebebrand, J.

Subjects

SEROTONIN, ATTENTION-deficit hyperactivity disorder, GENETIC polymorphisms, HETEROGENEITY, HUMAN genetic variation

Abstract

Alterations in the serotonergic pathway have been implicated in the pathogenesis of attention-deficit/hyperactivity disorder (ADHD). The aim of this study was to investigate seven genetic variants in three genes (serotonin transporter ( 5-HTT), serotonin receptor 1B ( 5-HTR1B) and serotonin receptor 2A ( 5-HTR2A)), which have previously been shown to be associated with ADHD. The polymorphisms under investigation were the 5-HTTLPR, the VNTR in intron 2 and the 3′UTR SNP in 5-HTT, the 5-HTR1B variations 861G>C and 102T>C, and the 5-HTR2A variations His452Tyr and 1438G>A. We genotyped these variants in a sample of 102 families with 229 children with ADHD according to DSM-IV criteria. Among the affected children, 69% fulfilled criteria for the combined type, 27% for the predominantly inattentive type, and 4% for the predominantly hyperactive-impulsive type. Associations were tested by the pedigree transmission disequilibrium test (PDT). All investigated polymorphisms in serotonergic candidate genes showed no association to ADHD in our sample. Earlier studies of these polymorphisms had also shown inconsistent results, with some studies reporting significant associations and others demonstrating no association. This discordance between studies may reflect variation in patient ascertainment criteria, genetic heterogeneity, too low statistical power for the expected effects or false positive results in the initial reports. We cannot rule out the possibility that other variations in the investigated genes contribute to the etiology of ADHD. [ABSTRACT FROM AUTHOR]

Published

2007

9. A 400-kb tandem duplication within the dystrophin gene leads to severe Becker muscular dystrophy.

Author

Gold, R., Kreß, W., Bettecken, T., Reichmann, H., and Müller, C.

Abstract

We describe a family with a large duplication of exons 2-16 of the dystrophin gene. It was characterized by immunocytochemistry, field-inversion gel electrophoresis and quantitative Southern blots. Our observations are of clinical interest in that they demonstrate an intermediate disease course despite a disrupted reading frame of dystrophin as postulated from exon-intron boundaries. We discuss possible mechanisms which may explain the unusual phenotype in our patient. [ABSTRACT FROM AUTHOR]

Published

1994

10. On the origin of deletions and point mutations in Duchenne muscular dystrophy: most deletions arise in oogenesis and most point mutations result from events in spermatogenesis.

Author

Grimm, T, Meng, G, Liechti-Gallati, S, Bettecken, T, Müller, C R, and Müller, B

Abstract

We present the results of a study of the rate and origin of mutations in Duchenne muscular dystrophy (DMD). Depending on the type of mutation (deletion/duplication or point mutation) present in the patient, there are widely varying ratios of male to female mutation rates. In deletions, the male mutation rate is only 30% of the female one. In non-deletional/non-duplicational mutations (presumably containing a high proportion of point mutations) the male mutation rate is at least 2.2 as high as the female one and probably much higher. Allowing for the presence of autosomal recessive phenocopies we find that k in non-deletional/non-duplicational mutations is 40.3. These findings mean that the vast majority of deletions arise in oogenesis, while most point mutations stem from spermatogenesis. Previous investigations have shown that in other diseases and genes, most notably haemophilia B and A, but also the ZFY and ZFX genes, the male mutation rate for point mutations tends to be higher than the female one. Our results can be seen as a confirmation of this for the special case of DMD. The influence on risk figures is considerable. As an example, the risk of the mother of an isolated case of DMD without an apparent structural anomaly of the gene of being a carrier increases from 67% to at least 76%. Given the estimate of 40.3 for k, allowing for the presence of autosomal recessive phenocopies mentioned above, it increases even further to 98%. However, as confidence intervals are still large, more data are needed to improve the estimates. Germinal mosaicism in this context is discussed. [ABSTRACT FROM PUBLISHER]

Published

1994

11. Evidence for associations between PDE4D polymorphisms and a subtype of neuroticism.

Author

Heck, A, Lieb, R, Unschuld, P G, Ellgas, A, Pfister, H, Lucae, S, Erhardt, A, Himmerich, H, Horstmann, S, Kloiber, S, Ripke, S, Müller-Myhsok, B, Bettecken, T, Uhr, M, Holsboer, F, and Ising, M

Subjects

LETTERS to the editor, NEUROSES

Abstract

A letter to the editor is presented in response to the article on the genome-wide analysis for extreme scores of the personality trait neuroticism by S. Shifman and colleagues.

Published

2008

12. Genetic markers within glutamate receptors associated with antidepressant treatment-emergent suicidal ideation.

Author

Menke A, Lucae S, Kloiber S, Horstmann S, Bettecken T, Uhr M, Ripke S, Ising M, Müller-Myhsok B, Holsboer F, and Binder EB

Published

2008

13. Frequency of CFTR gene mutations in males participating in an ICSI programme.

Author

Jakubiczka, S., Bettecken, Th., Stumm, M., Nickel, I., Musebeck, J., Krebs, P., Fischer, Ch., Kleinstein, J., Wieacke, P., Bettecken, T, Müsebeck, J, Fischer, C, and Wieacker, P

Abstract

A higher prevalence of cystic fibrosis transmembrane regulator (CFTR) gene mutations has been suggested both in men affected by congenital aplasia of the vas deferens, and in individuals presenting with reduced sperm quality. In this case, an increased risk for offspring being affected by cystic fibrosis (CF) can be expected in couples who are planning to undergo intracytoplasmic sperm injection (ICSI), since most of the male partners suffer from infertility. In order to determine the risk for these couples more precisely, we offered them a test for the most frequent CF mutations prevalent in the German population. The frequency of mutations within the CFTR gene in the female group was in the same range as expected for the general population (six out of 150). In 10 out of 207 males tested, infertility could be explained by exogenous factors not related to CFTR. Among the remaining 197 males with idiopathic infertility, we detected 13 heterozygotes for a mutation within the CFTR gene. This slightly, but significantly (P = 0.014), elevated rate could indicate that infertile males have, compared with the general population, an increased risk of being a carrier of a CFTR gene mutation. [ABSTRACT FROM AUTHOR]

Published

1999