Your search keyword '"Lascorz, J."' showing total 3 results

1. Characterisation of psoriasis susceptibility locus 6 (PSORS6) in patients with early onset psoriasis and evidence for interaction with PSORS1.

Author

Hüffmeier, U., Lascorz, J., Becker, T., Schürmeier-Horst, F., Magener, A., Ekici, A. B., Endele, S., Thiel, C. T., Toma-Uszynski, S., Mössner, R., Reich, K., Kurrat, W., Wienker, T. F., Traupe, H., and Reis, A.

Subjects

PSORIASIS, SKIN diseases, LINKAGE disequilibrium, MICROSATELLITE repeats, IMMUNOHISTOCHEMISTRY, LOCUS (Genetics)

Abstract

Background: Psoriasis is a genetically complex, chronic inflammatory skin disease. The authors have previously identified a susceptibility locus on chromosome 19p13 (PSORS6). Methods and results: In a follow-up linkage disequilibrium (LD) study in an independent family based cohort, the authors found evidence for association to a newly discovered microsatellite at this locus (D19SPS21, p<5.3 x 10-5). An LD based association scan in 300 trios revealed association to several single, single nucleotide polymorphisms (SNPs) in one LD block. When the authors stratified this cohort for carrying the PSORS1 risk allele at the HLA-C locus, evidence for association became much stronger at single SNP and haplotype levels (p values between 1.0 x 10-4 and 8.0 x 10-4). In a replication study of 1114 patients and 937 control individuals, evidence for association was also observed after stratification to the PSORS1 risk allele. In both study groups, logistic regression showed evidence for interaction between the risk alleles at PSORS1 and PSORS6. Best p values for rs12459358 in both study groups remained significant after correction for multiple testing. The associated LD block did not comprise any known genes. Interestingly, an adjacent gene, MUC16, coding for a large glycosylated protein expressed in epithelia and of unknown function, could be shown to be also expressed in tissues relevant for pathogenesis of psoriasis such as skin and thymus. Immunohistochemical analyses of skin revealed focal staining for MUC16 in suprabasal epidermal cells. Further functional studies are required to clarify its potential role in psoriasis and identify the causal variant(s) at this locus. [ABSTRACT FROM AUTHOR]

Published

2009

2. Systematic assessment of atypical deletions reveals genotype-phenotype correlation in 22q11.2.

Author

Rauch, A., Zink, S., Zweier, C., Thiel, C. T., Koch, A., Rauch, R., Lascorz, J., Hüffmeier, U., Weyand, M., Singer, H., and Hofbeck, M.

Subjects

GENETIC research, GENETIC polymorphisms, CONGENITAL heart disease, INTELLECTUAL disabilities, DEVELOPMENTAL disabilities, GENOTYPE-environment interaction, PHENOTYPES, HEART abnormalities

Abstract

Introduction: Clinical variability associated with the common 22q11.2 microdeletion is well known, and has led to a broad application of FISH diagnostics with probes for loci TUPLE1 or D22S75 (N25), although, rarely reported atypical deletions associated with the same phenotypic spectrum would not be discovered by these probes. As most types of 22q11.2 deletions occur between low copy repeats within the region (LCR22), we assumed that atypical deletions should be more common than has been reported. To address this question and the possibility of a deletion size related genotype-phenotype correlation, we systematically assessed the frequency of typical and atypical 22q11.2 deletions in a large cohort of patients. Methods: We used a set of 10 fluorescent in situ hybridisation (FISH) DNA probes, capable of detecting all reported and hypothetical deletions between the LCR22, and analysed 350 patients. Deletion sizes in atypical deletions were established by use of further FISH probes. Frequency of certain atypical deletions was analysed in controls by FISH and quantitative PCR. Results: Patients with conotruncal heart defects (ctCHD) and with typical VCFS phenotype showed the common 3 Mb or nested 1.5 Mb deletions (in 18.5% and 78.6%, respectively), but no atypical deletion, while 5% (3/63) of patients with a mildly suggestive, atypical phenotype showed atypical distal deletions, which were not detected in patients with mental retardation of unknown origin or in healthy controls. Discussion: These statistically significant differences demonstrate that atypical distal 22q11.2 deletions are very uncommon in patients with ctCHDs, while atypical congenital heart defects and mild dysmorphism are recognisable feature of atypical distal deletions. Further phenotype-genotype analysis disclosed association of significant developmental delay with the distal part of the common deletion region, and choanal atresia and atypical CHDs with the adjacent distal deletion region. [ABSTRACT FROM AUTHOR]

Published

2005

3. Lack of genetic association of the three more common polymorphisms of CARD15 with psoriatic arthritis and psoriasis in a German cohort.

Author

Lascorz, J., Burkhardt, H., Hüffmeier, U., Böhm, B., Schürmeyer-Horst, F., Lohmann, J., Ständer, M., Wendler, J., Kelsch, R., Baumann, C., Küster, W., Traupe, H., and Reis, A.

Published

2005