Your search keyword '"Chromosome 6P"' showing total 36 results

1. Gain of Chromosome 6p Correlates with Severe Anaplasia, Cellular Hyperchromasia, and Extraocular Spread of Retinoblastoma

Author

Gustav Stålhammar, MD, PhD, Aaron Yeung, MD, PhD, Pia Mendoza, MD, Sander R. Dubovy, MD, J. William Harbour, MD, and Hans E. Grossniklaus, MD, MBA

Subjects

Anaplasia, Chromosome 6p, Retinoblastoma, Survival, Whole genome sequencing, Ophthalmology, RE1-994

Abstract

Purpose: Gain of chromosome 6p has been associated with poor ocular survival in retinoblastoma and histopathologic grading of anaplasia with increased risk of metastatic spread and death. This study examined the correlation between these factors and other chromosomal abnormalities as well as results of whole genome sequencing, digital morphometry, and progression-free survival. Design: Retrospective cohort study from 2 United States tertiary referral centers. Participants: Forty-two children who had undergone enucleation for retinoblastoma from January 2000 through December 2017. Methods: Status of chromosomes 6p, 1q, 9q, and 16q was evaluated with fluorescence in situ hybridization, the degree of anaplasia and presence of histologic high-risk features were assessed by ocular pathologists, digital morphometry was performed on scanned tumor slides, and whole genome sequencing was performed on a subset of tumors. Progression-free survival was defined as absence of distant or local metastases or tumor growth beyond the cut end of the optic nerve. Main Outcome Measures: Correlation between each of chromosomal abnormalities, anaplasia, morphometry and sequencing results, and survival. Results: Forty-one of 42 included patients underwent primary enucleation and 1 was treated first with intra-arterial chemotherapy. Seven tumors showed mild anaplasia, 19 showed moderate anaplasia, and 16 showed severe anaplasia. All tumors had gain of 1q, 18 tumors had gain of 6p, 6 tumors had gain of 9q, and 36 tumors had loss of 16q. Tumors with severe anaplasia were significantly more likely to harbor 6p gains than tumors with nonsevere anaplasia (P < 0.001). Further, the hematoxylin staining intensity was significantly greater and that of eosin staining significantly lower in tumors with severe anaplasia (P < 0.05). Neither severe anaplasia (P = 0.10) nor gain of 6p (P = 0.21) correlated with histologic high-risk features, and severe anaplasia did not correlate to RB1, CREBBP, NSD1, or BCOR mutations in a subset of 14 tumors (P > 0.5). Patients with gain of 6p showed significantly shorter progression-free survival (P = 0.03, Wilcoxon test). Conclusions: Gain of chromosome 6p emerges as a strong prognostic biomarker in retinoblastoma because it correlates with severe anaplasia, quantifiable changes in tumor cell staining characteristics, and extraocular spread.

Published

2022

2. Genomewide scans in North American families reveal genetic linkage of essential tremor to a region on chromosome 6p23

Author

Shatunov, Alexey, Sambuughin, Nyamkhishig, Jankovic, Joseph, Elble, Rodger, Lee, Hee Suk, Singleton, Andrew B, Dagvadorj, Ayush, Ji, Jay, Zhang, Yiping, Kimonis, Virginia E, Hardy, John, Hallett, Mark, and Goldfarb, Lev G

Subjects

Genetics, Clinical Research, Human Genome, Biotechnology, 2.1 Biological and endogenous factors, Aetiology, Adult, Age of Onset, Chromosome Mapping, Chromosomes, Human, Pair 6, DNA Mutational Analysis, Dystonia, Family Health, Female, Genetic Linkage, Genetic Markers, Genetic Predisposition to Disease, Genotype, Haplotypes, Humans, Male, Microsatellite Repeats, Middle Aged, Pedigree, Phenotype, Tremor, United States, essential tremor, focal dystonia, linkage mapping, chromosome 6p, Medical and Health Sciences, Psychology and Cognitive Sciences, Neurology & Neurosurgery

Abstract

Essential tremor (ET) is the most prevalent adult-onset movement disorder showing evidence of non-random accumulation in some families. ET has previously been mapped to genetic loci on chromosomes 2p and 3q, but no causative genes identified. We conducted genomewide linkage screening with subsequent fine mapping in seven large North American families comprising a total of 325 genotyped individuals that included 65 patients diagnosed as definite ET. Linkage analysis was based on methodology implemented in SimWalk2 and LINKAGE programs. A multigenerational family revealed suggestive linkage to a locus on chromosome 6p23 with maximal nonparametric linkage (NPL) multipoint score 3.281 (P = 0.0005) and parametric multipoint log of the odds (LOD) score 2.983. A second family showed positive linkage to the same 6p23 region with a maximal NPL score 2.125 (P = 0.0075) and LOD score 1.265. Haplotype analysis led to the identification of a 600 kb interval shared by both families. Sequencing of coding regions of 15 genes located in the linked region detected numerous sequence variants, some of them predicting a change of the encoded amino acid, but each was also found in controls. Our findings provide evidence for linkage to a novel susceptibility locus on chromosome 6p23. Analysis of additional ET-affected families is needed to confirm linkage and identify the underlying gene.

Published

2006

3. Comparative methylome analysis in solid tumors reveals aberrant methylation at chromosome 6p in nasopharyngeal carcinoma.

Author

Dai, Wei, Cheung, Arthur Kwok Leung, Ko, Josephine Mun Yee, Cheng, Yue, Zheng, Hong, Ngan, Roger Kai Cheong, Ng, Wai Tong, Lee, Anne Wing Mui, Yau, Chun Chung, Lee, Victor Ho Fu, and Lung, Maria Li

Subjects

*METHYLATION, *NASOPHARYNX cancer, *TUMOR suppressor genes, *POLYCOMB group proteins, *EPIGENETICS, *GENE therapy

Abstract

Altered patterns of DNA methylation are key features of cancer. Nasopharyngeal carcinoma ( NPC) has the highest incidence in Southern China. Aberrant methylation at the promoter region of tumor suppressors is frequently reported in NPC; however, genome-wide methylation changes have not been comprehensively investigated. Therefore, we systematically analyzed methylome data in 25 primary NPC tumors and nontumor counterparts using a high-throughput approach with the Illumina HumanMethylation450 BeadChip. Comparatively, we examined the methylome data of 11 types of solid tumors collected by The Cancer Genome Atlas ( TCGA). In NPC, the hypermethylation pattern was more dominant than hypomethylation and the majority of de novo methylated loci were within or close to CpG islands in tumors. The comparative methylome analysis reveals hypermethylation at chromosome 6p21.3 frequently occurred in NPC (false discovery rate; FDR=1.33 × 10−9), but was less obvious in other types of solid tumors except for prostate and Epstein-Barr virus ( EBV)-positive gastric cancer ( FDR<10−3). Bisulfite pyrosequencing results further confirmed the aberrant methylation at 6p in an additional patient cohort. Evident enrichment of the repressive mark H3K27me3 and active mark H3K4me3 derived from human embryonic stem cells were found at these regions, indicating both DNA methylation and histone modification function together, leading to epigenetic deregulation in NPC. Our study highlights the importance of epigenetic deregulation in NPC. Polycomb Complex 2 ( PRC2), responsible for H3K27 trimethylation, is a promising therapeutic target. A key genomic region on 6p with aberrant methylation was identified. This region contains several important genes having potential use as biomarkers for NPC detection. [ABSTRACT FROM AUTHOR]

Published

2015

4. Chromosome 6p SNP microhaplotypes and IgG3 levels in hemochromatosis probands with HFE p.C282Y homozygosity

Author

Eugénia Cruz, Graça Porto, J. Clayborn Barton, Maria José Teles, João Tiago Guimarães, James C. Barton, and Instituto de Saúde Pública da Universidade do Porto

Subjects

0301 basic medicine, Proband, Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, HFE p.C282Y, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, 03 medical and health sciences, 0302 clinical medicine, SNP microhaplotype, medicine, SNP, Humans, Point Mutation, Hemochromatosis Protein, Molecular Biology, Gene, Hemochromatosis, Genetics, business.industry, IgG1, Siblings, Homozygote, IgG3, Chromosome, Cell Biology, Hematology, Middle Aged, medicine.disease, Confidence interval, Pedigree, 030104 developmental biology, Immunoglobulin G, Cohort, Chromosome 6p, Molecular Medicine, Chromosomes, Human, Pair 6, Female, business, 030215 immunology

Abstract

Subnormal IgG1 or IgG3 levels occurred in 30% of hemochromatosis probands with HFE p.C282Y homozygosity and were concordant in HLA-identical siblings. We sought to identify factors associated with IgG subclasses in Alabama probands with p.C282Y homozygosity evaluated for 500 kb microhaplotypes AAT and GGG defined by SNPs in chromosome 6p genes PGBD1, ZNF193, and ZNF165. In regressions on IgG subclasses, we used: age; sex; GGG (dichotomous); iron removed to achieve depletion; CD8+ T-lymphocytes; and other IgG subclasses. Among 49 probands, AAT and GGG occurred in 95.9% and 16.3%, respectively. Thirteen probands (26.5%) had subnormal IgG1; 11 probands (22.4%) had subnormal IgG3. Mean IgG3 was higher in probands with than without GGG (75 mg/dL [95% confidence interval 63, 89] vs. 58 mg/dL [49, 71], respectively; p = 0.0321). Regression on IgG3 revealed: GGG positivity (p = 0.0106); and IgG1 (p = 0.0015). In a replication cohort of 22 Portugal probands with p.C282Y homozygosity, mean IgG3 was higher in probands with than without GGG (46 ± 16 vs. 31 ± 12 mg/dL, respectively; p = 0.0410). We conclude that mean IgG3 levels are higher in hemochromatosis probands with p.C282Y homozygosity with chromosome 6p microhaplotype GGG than in probands homozygous for microhaplotype AAT. This work was supported in part by Southern Iron Disorders Center, Birmingham, Alabama; FEDER through the program POFC-COMPETE (COMPETE “FCOMP-01-0124-FEDER-008447”); national funds through the FCT (Portuguese Foundation for Science and Technology) grants PTDC/SAU-GMC/67868/2006 and PIC/IC/82785/2007; and by Forum Hematologico do Norte (IgG subtype measures).

Published

2020

5. Karyotype-Phenotype Correlation in Partial Trisomies of the Short Arm of Chromosome 6: A Family Case Report and Review of the Literature.

Author

Castiglione, a., Guaran, V., astolfi, L., Orioli, E., Zeri, G., Gemmati, D., Bovo, R., Montaldi, a., alghisi, a., and Martini, a.

Subjects

*CHROMOSOME abnormalities, *TRISOMY, *CARDIAC imaging, *CHRONIC kidney failure, *MAGNETIC resonance, *NUCLEIC acids

Abstract

The first child (proband) of nonconsanguineous Caucasian parents underwent genetic investigation because she was affected with congenital choanal atresia, heart defects and kidney hyposplasia with mild transient renal insufficiency. The direct DNA sequencing after PCR of the CHD7 gene, which is thought to be responsible for approximately 60-70% of the cases of CHARGE syndrome/association, found no mutations. The cytogenetic analysis (standard GTG banding karyotype) revealed the presence of extrachromosomal material on 10q. The chromosome analysis was completed with array CGH (30 kb resolution), MLPA and FISH, which allowed the identification of three 6p regions (6p.25.3p23 × 3): 2 of these regions are normally located on chromosome 6, and the third region is translocated to the long arm of chromosome 10. The same chromosomal rearrangement was subsequently found in the father, who was affected with congenital ptosis and progressive hearing loss, and in the proband's sister, the second child, who presented at birth with choanal atresia and congenital heart defects. The mutated karyotypes, which were directly inherited, are thought to be responsible for a variable phenotype, including craniofacial dysmorphisms, choanal atresia, congenital ptosis, sensorineural hearing loss, heart defects, developmental delay, and renal dysfunction. Nevertheless, to achieve a complete audiological assessment of the father, he underwent further investigation that revealed an increased level of the coagulation factor XIII (300% increased activity), fluctuating levels of fibrin D-dimer degradation products (from 296 to 1,587 ng/ml) and a homoplasmic mitochondrial DNA mutation: T961G in the MTRNR1 (12S rRNA) gene. He was made a candidate for cochlear implantation. Preoperative high-resolution computed tomography and magnetic resonance imaging of the temporal bone revealed the presence of an Arnold-Chiari malformation type I. To the best of our knowledge, this study is the second report on partial 6p trisomy that involves the 10q terminal region. Furthermore, we report the first case of documented Arnold-Chiari malformation type I and increased factor XIII activity associated with 6p trisomy. We present a comprehensive report of the familial cases and an exhaustive literature review. © 2013 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2013

6. Production and identification of wheat- Agropyron cristatum 6P translocation lines.

Author

Yang Luan, Xiaoguang Wang, Weihua Liu, Chunye Li, Jinpeng Zhang, Ainong Gao, Yandong Wang, Xinming Yang, and Lihui Li

Subjects

CRESTED wheatgrass, IN situ hybridization, CROP yields, CHROMOSOMAL translocation, CHROMOSOMES, CELL nuclei

Abstract

The narrow genetic background of wheat is the primary factor that has restricted the improvement of crop yield in recent years. The kernel number per spike is the most important factor of the many potential characteristics that determine wheat yield. Agropyron cristatum (L.) Gaertn., a wild relative of wheat, has the characteristics of superior numbers of florets and kernels per spike, which are controlled by chromosome 6P. In this study, the wheat- A. cristatum disomic addition and substitution lines were used as bridge materials to produce wheat- A. cristatum 6P translocation lines induced by gametocidal chromosomes and irradiation. The results of genomic in situ hybridization showed that the frequency of translocation induced by gametocidal chromosomes was 5.08%, which was higher than the frequency of irradiated hybrids (2.78%) and irradiated pollen (2.12%). The fluorescence in situ hybridization results of the translocation lines showed that A. cristatum chromosome 6P could be translocated to wheat ABD genome, and the recombination frequency was A genome > B genome > D genome. The alien A. cristatum chromosome 6P was translocated to wheat homoeologous groups 1, 2, 3, 5 and 6. We obtained abundant translocation lines that possessed whole-arm, terminal, segmental and intercalary translocations. Three 6PS-specific and four 6PL-specific markers will be useful to rapidly identify and trace the translocated fragments. The different wheat- A. cristatum 6P translocation lines obtained in this study can provide basic materials for analyzing the alien genes carried by chromosome 6P. The translocation line WAT33-1-3 and introgression lines WAI37-2 and WAI41-1, which had significant characteristics of multikernel (high numbers of kernels per spike), could be utilized as novel germplasms for high-yield wheat breeding. [ABSTRACT FROM AUTHOR]

Published

2010

7. Association study between the dystrobrevin binding protein 1 gene (DTNBP1) and schizophrenia: A meta-analysis

Author

Li, Dawei and He, Lin

Subjects

*SCHIZOPHRENIA, *PSYCHOSES, *META-analysis, *PSYCHOMETRICS, *CARRIER proteins, *COMPARATIVE studies, *GENETIC polymorphisms, *RESEARCH methodology, *MEDICAL cooperation, *RESEARCH, *RESEARCH funding, *EVALUATION research

Abstract

Abstract: Positional, functional and association studies have strongly implicated the dystrobrevin binding protein 1 gene (DTNBP1) as a promising novel candidate gene for schizophrenia. Since the first association study was reported, there have been many attempts to replicate it. However the results have been mixed and these subsequent studies have produced negative as well as positive results. To reconcile these conflicting findings and to give a comprehensive picture of the relationship of DTNBP1 and schizophrenia, the current meta-analysis combined all published association studies involving nine polymorphisms up to May 2006. The results (12 studies including 3429 cases, 3376 controls and 721 trios) showed that there were five single nucleotide polymorphisms (SNPs) with p values < 0.05, however, sensitivity analyses showed that only one SNP was consistent across all nine studies (four of the five SNPs became non-significant after removal of one study), indicating that one study may cause the association findings for each of these four SNPs. In conclusion, there is only a weak association of one SNP in DTNBP1 with schizophrenia, which is not significant after multiple testing. [Copyright &y& Elsevier]

Published

2007

8. Association evidence of schizophrenia with distal genomic region of NOTCH4 in Taiwanese families.

Author

Liu, C.-M., Liu, Y.-L., Fann, C. S-J., Chen, W. J., Yang, W.-C., Ouyang, W.-C., Chen, C.-Y., Jou, Y.-S., Hsieh, M.-H., Liu, S.-K., Hwang, T.-J, Faraone, S. V., Tsuang, M. T., and Hwu, H.-G.

Subjects

*SCHIZOPHRENIA, *GENETIC polymorphisms, *TRANSCRIPTION factors, *PSYCHOSES, *CHROMOSOMES

Abstract

Evidence for association with schizophrenia has been reported for NOTCH4, although results have been inconsistent. Previous studies have focused on polymorphisms in the 5′ promoter region and first exon of NOTCH4. Our aim was to test the association of the entire genomic region of NOTCH4 in 218 families with at least two siblings affected by schizophrenia in Taiwan. We genotyped seven single nucleotide polymorphisms (SNPs) of this gene, with average intermarker distances of 5.3 kb. Intermarker linkage disequilibrium (LD) was calculated usinggold software, and single-locus and haplotype association analyses were performed usingtransmit software. We found that the T allele of SNP rs2071285 ( P= 0.035) and the G allele of SNP rs204993 ( P= 0.0097) were significantly preferentially transmitted to the affected individuals in the single-locus association analysis. The two SNPs were in high LD (D′ > 0.8). Trend for overtransmission was shown for the T-G haplotype of the two SNPs to affected individuals ( P= 0.053), with the A-A haplotype significantly undertransmitted ( P= 0.034). The associated region distributed across the distal portion of the NOTCH4 gene and overlapped with the genomic region of the G-protein signaling modulator 3 and pre-B-cell leukemia transcription factor 2. In summary, we found modest association evidence between schizophrenia and the distal genomic region of NOTCH4 in this Taiwanese family sample. Further replication for association with the distal genomic region of NOTCH4 is warranted. [ABSTRACT FROM AUTHOR]

Published

2007

9. No association evidence between schizophrenia and dystrobrevin-binding protein 1 (DTNBP1) in Taiwanese families

Author

Liu, Chih-Min, Liu, Yu-Li, Fann, Cathy Shen-Jang, Yang, Wei-Chih, Wu, Jer-Yuarn, Hung, Shuen-Iu, Chen, Wei J., Chueh, Ching-Mo, Liu, Wei-Ming, Liu, Chen-Chung, Hsieh, Ming-Hsien, Hwang, Tzung-Jeng, Faraone, Stephen V., Tsuang, Ming T., and Hwu, Hai-Gwo

Subjects

*SCHIZOPHRENIA, *PSYCHOSES, *ETIOLOGY of diseases, *ECHOLALIA, *ASIANS, *SIBLINGS, *CARRIER proteins, *CHROMOSOMES, *DISEASE susceptibility, *PSYCHOLOGICAL tests, *RESEARCH funding, *GENETIC markers, *HAPLOTYPES, *GENOTYPES, *PSYCHOLOGY

Abstract

Abstract: Several linkage studies have shown significant linkage of schizophrenia to chromosome 6p region, which includes the positional candidate genes, Dystrobrevin-binding protein 1 (DTNBP1). The aim was to examine the association evidence of the candidate gene in 693 Taiwanese families with at least two affected siblings of schizophrenia. We genotyped nine SNPs of this gene with average intermarker distance of 17 kb. Intermarker linkage disequilibrium was calculated with GOLD. Single locus and haplotype association analyses were performed with TRANSMIT program. We found no significant association between schizophrenia and DTNBP1 either through single locus or haplotype analyses. We failed to replicate the association evidence between DTNBP1 and schizophrenia and this gene may not play a major role in the etiology of schizophrenia in this Taiwanese family sample. [Copyright &y& Elsevier]

Published

2007

10. Gains and overexpression identify DEK and E2F3 as targets of chromosome 6p gains in retinoblastoma.

Author

Grasemann, Corinna, Gratias, Sandrine, Stephan, Harald, Schüler, Andreas, Schramm, Alexander, Klein-Hitpass, Ludger, Rieder, Harald, Schneider, Stephanie, Kappes, Ferdinand, Eggert, Angelika, and Lohmann, Dietmar R

Subjects

*RETINOBLASTOMA, *TUMORS, *CHROMOSOMES, *TUMOR suppressor genes, *GENE expression, *ONCOLOGY

Abstract

The paediatric eye tumour retinoblastoma is initiated by inactivation of RB1, a tumour suppressor on chromosome 13q. In addition to RB1 loss, many retinoblastomas show other genetic alterations including gains on chromosomes 6p21–pter and 1q31–q32. Recently, the minimal region of gains on chromosome 6 was narrowed to band p22. We examined genomic gains and expression changes in primary retinoblastomas to identify potential target genes in 6p22. Quantitative multiplex PCR detected copy numbers ≥3 in 25 (33%) tumours and no gains in 31 of 76 (40%) tumours. The remaining 20 (26%) samples showed gains only at some loci, most often including E2F3 and DEK in 6p22.3. Analysis of RNA from 21 primary retinoblastomas showed that expression levels of these and some other genes in 6p22 correspond to DNA gains. However, KIF 13A, a reported candidate oncogene on 6p, was expressed at low levels or absent. Clinical manifestation of tumours with gains at all 6p22 loci was distinct in that distribution of age at diagnosis was markedly shifted to older age compared to tumours with no or partial gains. In summary, our results suggest that DEK and E2F3 are potential targets of 6p gains in retinoblastoma. [ABSTRACT FROM AUTHOR]

Published

2005

11. A population-based LD map of the human chromosome 6p.

Author

Yu, Hong, Chia, Jer-Ming, Bourque, Guillaume, Wong, Marie, Chan, Soh, and Ren, Ee

Subjects

*HUMAN chromosomes, *MAJOR histocompatibility complex, *GENETIC polymorphisms, *NUCLEOTIDE sequence, *GENE mapping, *POPULATION genetics

Abstract

The recent publication of the complete sequence of human chromosome 6 provides a platform from which to investigate genomic sequence variation. We report here a detailed linkage disequilibrium (LD) pattern map across the entire human chromosome 6p by using a set of 1152 single nucleotide polymorphisms (SNPs) in a population of 198 Singaporean Chinese, with 326 SNPs focused in the major histocompatibility complex (MHC) region. Our analysis shows some unexpectedly high segments of strong LD in a 10-Mb region that includes the extremely polymorphic and gene-rich MHC loci and many non-MHC genes. These include the telomeric peri-MHC region that harbors olfactory receptors, histones and zinc finger clusters, and the centromeric peri-MHC region that contains several unknown open reading frames. The data also help refine a human–mouse synteny break in the region between 28.6 and 29.4 Mb. The population-based LD map presented here will provide an essential resource for understanding the genomic sequence variation of chromosome 6p and LD mapping of disease genes of complex genetic traits. [ABSTRACT FROM AUTHOR]

Published

2005

12. Haplotypes in the tumour necrosis factor region and myeloma.

Author

Morgan, Gareth J., Adamson, Peter J., Mensah, Fiona K., Spink, Charlotte F., Law, Graham R., Keen, Leigh J., Roman, Eve, Davies, Faith E., Rollinson, Sara, Child, J. A., and Bidwell, Jeffrey L.

Subjects

*TUMOR necrosis factors, *HAPLOIDY, *CANCER cells, *NECROSIS, *TUMORS, *GROWTH factors, *MACROPHAGES

Abstract

This study described the haplotypic structure across a region of chromosome 6 including the tumour necrosis factor (TNF) gene, and investigated its influence on the aetiology of myeloma. A total of 181 myeloma cases from the Medical Research Council Myeloma VII trial and 233 controls from the Leukaemia Research Fund Case Control Study of Adult Acute Leukaemia were included in the analysis. Genotyping by induced heteroduplex generator analysis was carried out for single nucleotide polymorphisms (SNP) located at positions−1031,−863,−857,−308 and−238 of the 5′ promoter region of TNF-α gene, and 252 in the LT-α gene; and five microsatellites, TNFa,b,c,dande. Haplotypes were inferred statistically using thephasealgorithm. A limited diversity of haplotypes was observed, with the majority of variation described by 12 frequent haplotypes. Detailed characterization of the haplotype did not provide greater determination of disease risk beyond that described by the TNF-α−308 SNP. Some evidence was provided for a decreased risk of myeloma associated with the TNF-α−308 variant allele A, odds ratio, 0·57; 95% confidence interval, 0·38–0·86. The results of this study did not support our starting hypothesis; that high producer haplotypes at the TNF locus are associated with an increased risk of developing myeloma. [ABSTRACT FROM AUTHOR]

Published

2005

13. Five NOTCH4 polymorphisms show weak evidence for association with schizophrenia: evidence from meta-analyses

Author

Glatt, Stephen J., Wang, Richard S., Yeh, Yu-Chi, Tsuang, Ming T., and Faraone, Stephen V.

Subjects

*SCHIZOPHRENIA, *GENETIC polymorphisms, *PSYCHOSES, *META-analysis, *ALLELES, *CELL receptors, *COMPARATIVE studies, *DNA, *GENOMES, *RESEARCH methodology, *MEDICAL cooperation, *PROTEINS, *RESEARCH, *EVALUATION research

Abstract

Abstract: NOTCH4 initially received consideration as a risk gene for schizophrenia based on its location within a region on chromosome 6p that had previously shown strong evidence for genetic linkage with the illness. The initial published test for allelic association found strong evidence for involvement of this gene in schizophrenia, but subsequent studies failed to confirm this finding. Presently, we have used meta-analysis to derive a best estimate of the nature and magnitude of the associations between schizophrenia and five polymorphisms in and around the NOTCH4 gene. No significant association was detected between schizophrenia and repeat length of alleles at the (TAA)n, (CTG)n, or (TTAT)n polymorphisms, or between the disease and specific risk alleles at these polymorphisms or at the SNP1 or SNP2 polymorphisms. Heterogeneity and stronger evidence of association with the putative risk alleles of the (TAA)n, (CTG)n, SNP1, and SNP2 polymorphisms was observed in family-based studies than in case-control studies, suggesting that these polymorphisms may reliably influence risk for schizophrenia under certain circumstances. Since more consistent and robust associations with schizophrenia risk have been observed for haplotypes of these polymorphisms [especially those containing SNP2 and (CTG)n], additional large family-based or genomic-controlled studies would be helpful for definitively specifying the role of NOTCH4 haplotypes in risk for schizophrenia. [Copyright &y& Elsevier]

Published

2005

14. Genome Scan for Susceptibility Loci for Schizophrenia.

Author

Bailer, Ursula, Leisch, Friedrich, Meszaros, Kurt, Lenzinger, Elisabeth, Willinger, Ulrike, Strobl, Rainer, Gebhardt, Christian, Gerhard, Elisabeth, Fuchs, Karoline, Sieghart, Werner, Kasper, Siegfried, Hornik, Kurt, and Aschauer, Harald N.

Subjects

*SCHIZOPHRENIA, *PSYCHOSES, *MEDICAL genetics, *HUMAN genome, *CHROMOSOMES

Abstract

Objective: Schizophrenia is a relatively common, often chronic and debilitating mental illness. Evidence from various studies has clearly demonstrated that genetic factors contribute substantially to the etiology. The goal of this study was to identify chromosomal regions likely to contain schizophrenia susceptibility genes. Methods: A genome-wide map of 388 microsatellite DNA markers was genotyped in 5 schizophrenia families. Nonparametric linkage analysis (Genehunter) was used to assess the pattern of allele sharing at each marker locus relative to the presence of disease. Results: Nonparametric linkage scores did not reach a genome-wide level of statistical significance (p < 0.00002) or a p value suggestive of linkage (p < 0.007) for any marker; however, one p value suggested replicated linkage (p < 0.01) at chromosome 6p24 in region D6S309 (p = 0.0047). Furthermore, 11 markers resulted in p < 0.05 at chromosomes 6p, 6q, 10q, 12q and 14q. Conclusions: Despite the differences in diagnostic schemes, in markers used and methods of analyses between studies published so far, we think that our result supports the notion that there is possibly some consistent evidence for replicated linkage of a schizophrenia susceptibility locus around the region of D6S309 at chromosome 6p24.Copyright © 2000 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2000

15. Gain of Chromosome 6p Correlates with Severe Anaplasia, Cellular Hyperchromasia, and Extraocular Spread of Retinoblastoma.

Author

Stålhammar G, Yeung A, Mendoza P, Dubovy SR, William Harbour J, and Grossniklaus HE

Abstract

Purpose: Gain of chromosome 6p has been associated with poor ocular survival in retinoblastoma and histopathologic grading of anaplasia with increased risk of metastatic spread and death. This study examined the correlation between these factors and other chromosomal abnormalities as well as results of whole genome sequencing, digital morphometry, and progression-free survival., Design: Retrospective cohort study from 2 United States tertiary referral centers., Participants: Forty-two children who had undergone enucleation for retinoblastoma from January 2000 through December 2017., Methods: Status of chromosomes 6p, 1q, 9q, and 16q was evaluated with fluorescence in situ hybridization, the degree of anaplasia and presence of histologic high-risk features were assessed by ocular pathologists, digital morphometry was performed on scanned tumor slides, and whole genome sequencing was performed on a subset of tumors. Progression-free survival was defined as absence of distant or local metastases or tumor growth beyond the cut end of the optic nerve., Main Outcome Measures: Correlation between each of chromosomal abnormalities, anaplasia, morphometry and sequencing results, and survival., Results: Forty-one of 42 included patients underwent primary enucleation and 1 was treated first with intra-arterial chemotherapy. Seven tumors showed mild anaplasia, 19 showed moderate anaplasia, and 16 showed severe anaplasia. All tumors had gain of 1q, 18 tumors had gain of 6p, 6 tumors had gain of 9q, and 36 tumors had loss of 16q. Tumors with severe anaplasia were significantly more likely to harbor 6p gains than tumors with nonsevere anaplasia ( P < 0.001). Further, the hematoxylin staining intensity was significantly greater and that of eosin staining significantly lower in tumors with severe anaplasia ( P < 0.05). Neither severe anaplasia ( P  = 0.10) nor gain of 6p ( P  = 0.21) correlated with histologic high-risk features, and severe anaplasia did not correlate to RB1 , CREBBP , NSD1 , or BCOR mutations in a subset of 14 tumors ( P > 0.5). Patients with gain of 6p showed significantly shorter progression-free survival ( P  = 0.03, Wilcoxon test)., Conclusions: Gain of chromosome 6p emerges as a strong prognostic biomarker in retinoblastoma because it correlates with severe anaplasia, quantifiable changes in tumor cell staining characteristics, and extraocular spread., (© 2021 by the American Academy of Ophthalmology.)

Published

2021

16. Directly inherited partial trisomy of chromosome 6p identified in a father and daughter by chromosome microdissection.

Author

Delatycki, Martin B., Voullaire, Lucille, Francis, David, Petrovic, Vida, Robertson, Anne, Webber, Lorna M., and Slater, Howard R.

Published

1999

17. Chromosome 6p SNP microhaplotypes and IgG3 levels in hemochromatosis probands with HFE p.C282Y homozygosity.

Author

Barton, James C., Barton, J. Clayborn, Cruz, Eugénia, Teles, Maria José, Guimarães, João T., and Porto, Graça

Subjects

*HOMOZYGOSITY, *CHROMOSOMES, *T cells, *CONFIDENCE intervals

Abstract

Subnormal IgG1 or IgG3 levels occurred in 30% of hemochromatosis probands with HFE p.C282Y homozygosity and were concordant in HLA-identical siblings. We sought to identify factors associated with IgG subclasses in Alabama probands with p.C282Y homozygosity evaluated for 500 kb microhaplotypes AAT and GGG defined by SNPs in chromosome 6p genes PGBD1 , ZNF193 , and ZNF165. In regressions on IgG subclasses, we used: age; sex; GGG (dichotomous); iron removed to achieve depletion; CD8+ T-lymphocytes; and other IgG subclasses. Among 49 probands, AAT and GGG occurred in 95.9% and 16.3%, respectively. Thirteen probands (26.5%) had subnormal IgG1; 11 probands (22.4%) had subnormal IgG3. Mean IgG3 was higher in probands with than without GGG (75 mg/dL [95% confidence interval 63, 89] vs. 58 mg/dL [49, 71], respectively; p = 0.0321). Regression on IgG3 revealed: GGG positivity (p = 0.0106); and IgG1 (p = 0.0015). In a replication cohort of 22 Portugal probands with p.C282Y homozygosity, mean IgG3 was higher in probands with than without GGG (46 ± 16 vs. 31 ± 12 mg/dL, respectively; p = 0.0410). We conclude that mean IgG3 levels are higher in hemochromatosis probands with p.C282Y homozygosity with chromosome 6p microhaplotype GGG than in probands homozygous for microhaplotype AAT. [ABSTRACT FROM AUTHOR]

Published

2020

18. Lack of a genetic association between the TNXB locus and schizophrenia in a Chinese population

Author

Liu, Lin-Lin, Wei, Jun, Zhang, Xuan, Li, Xiu-Yi, Shen, Yan, Liu, Shu-Zheng, Ju, Gui-Zhi, Shi, Jie-Ping, Yu, Ya-Qin, Xu, Qi, and Hemmings, Gwynneth P.

Subjects

*TENASCIN, *SCHIZOPHRENIA, *NUCLEOTIDES, *GENETIC polymorphisms

Abstract

A recent study demonstrated that the tenascin X (TNXB) gene was associated with schizophrenia in a British population. To replicate the initial finding, we analysed two positive single nucleotide polymorphisms (SNPs), rs1009382 and rs204887 present at the TNXB locus, in a Chinese population by using PCR-based restriction fragment length polymorphism analysis. We recruited a total of 136 family trios consisting of fathers, mothers and affected offspring with schizophrenia. The transmission disequilibrium test did not show allelic association between these two SNPs and schizophrenia, and the rs1009382-rs204887 haplotypes were not associated with the illness either. The present results suggest that the TNXB locus does not appear to be associated with schizophrenia in the Chinese population. Because the TNXB gene is less than 100 kb away from the NOTCH4 locus that was also reported to be associated with schizophrenia, allelic and locus heterogeneity could be possible reasons for the failure to replicate the TNXB finding. [Copyright &y& Elsevier]

Published

2004

19. Gene expression profiling identifies different sub-types of retinoblastoma

Author

Georgia Kapatai, Pamela Kearns, Brundler Ma, Carmel McConville, Andrew C. Peet, Manoj Parulekar, and Helen Jenkinson

Subjects

Adult, retina, Cancer Research, Cell type, Retinal Neoplasm, Retinal Neoplasms, Biology, medicine.disease_cause, Models, Biological, chromosome 1q, medicine, Cluster Analysis, Humans, Gene Regulatory Networks, Regulation of gene expression, Comparative Genomic Hybridization, Mutation, Retinoblastoma, Microarray analysis techniques, Gene Expression Profiling, Genetics and Genomics, chromosome 16q, Microarray Analysis, medicine.disease, photoreceptor, Molecular biology, eye diseases, Gene Expression Regulation, Neoplastic, Gene expression profiling, Oncology, chromosome 6p, Cytogenetic Analysis, Cancer research, Carcinogenesis

Abstract

Background: Mutation of the RB1 gene is necessary but not sufficient for the development of retinoblastoma. The nature of events occurring subsequent to RB1 mutation is unclear, as is the retinal cell-of-origin of this tumour. Methods: Gene expression profiling of 21 retinoblastomas was carried out to identify genetic events that contribute to tumorigenesis and to obtain information about tumour histogenesis. Results: Expression analysis showed a clear separation of retinoblastomas into two groups. Group 1 retinoblastomas express genes associated with a range of different retinal cell types, suggesting derivation from a retinal progenitor cell type. Recurrent chromosomal alterations typical of retinoblastoma, for example, chromosome 1q and 6p gain and 16q loss were also a feature of this group, and clinically they were characterised by an invasive pattern of tumour growth. In contrast, group 2 retinoblastomas were found to retain many characteristics of cone photoreceptor cells and appear to exploit the high metabolic capacity of this cell type in order to promote tumour proliferation. Conclusion: Retinoblastoma is a heterogeneous tumour with variable biology and clinical characteristics.

Published

2013

20. PCSK6 is associated with handedness in individuals with dyslexia

Author

Susan M. Ring, Silvia Paracchini, Joel B. Talcott, Anthony P. Monaco, Andrew P. Morris, William M. Brandler, Thomas S. Scerri, John F. Stein, Alex J. Richardson, University of St Andrews. School of Medicine, and University of St Andrews. Biomedical Sciences Research Complex

Subjects

Reading disability, REading-disability, Nodal Protein, Developmental dyslexia, Population, Genome-wide association study, QH426 Genetics, Biology, Susceptibility gene, Quantitative-trait locus, Functional Laterality, Relative hand skill, Dyslexia, 03 medical and health sciences, 0302 clinical medicine, Chromosome 6P, Genetics, medicine, Humans, Allele, education, Dominance, Cerebral, QH426, Molecular Biology, Genetics (clinical), Language, 030304 developmental biology, 0303 health sciences, education.field_of_study, Genome-wide association, Association Studies Articles, Proteolytic enzymes, General Medicine, medicine.disease, United States, Minor allele frequency, Laterality, Linkage analysis, 030217 neurology & neurosurgery, Genome-Wide Association Study

Abstract

Approximately 90% of humans are right-handed. Handedness is a heritable trait, yet the genetic basis is not well understood. Here we report a genome-wide association study for a quantitative measure of relative hand skill in individuals with dyslexia [reading disability (RD)]. The most highly associated marker, rs11855415 (P = 4.7 x 10(-7)), is located within PCSK6. Two independent cohorts with RD show the same trend, with the minor allele conferring greater relative right-hand skill. Meta-analysis of all three RD samples is genome-wide significant (n = 744, P = 2.0 x 10(-8)). Conversely, in the general population (n = 2666), we observe a trend towards reduced laterality of hand skill for the minor allele (P = 0.0020). These results provide molecular evidence that cerebral asymmetry and dyslexia are linked. Furthermore, PCSK6 is a protease that cleaves the left-right axis determining protein NODAL. Functional studies of PCSK6 promise insights into mechanisms underlying cerebral lateralization and dyslexia. Publisher PDF

Published

2010

21. Finding Suitable Phenotypes for Genetic Studies of Schizophrenia: Heritability and Segregation Analysis

Author

Roel A. Ophoff, Chantal Kemner, Margriet M. Sitskoorn, René S. Kahn, Behrooz Z. Alizadeh, Jean-Paul Selten, Richard J. Sinke, Maartje F. Aukes, Life Course Epidemiology (LCE), Real World Studies in PharmacoEpidemiology, -Genetics, -Economics and -Therapy (PEGET), Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Cognitive Neuropsychology, RS: FPN CN II, Cognitive Neuroscience, MUMC+: HZC Klinische Neurofysiologie (5), Life Course Epidemiology, and Groningen Institute for Gastro Intestinal Genetics and Immunology

Subjects

Male, neurocognition, heritability, Neuropsychological Tests, Social Environment, Spatial memory, Developmental psychology, inheritance pattern, Verbal fluency test, EYE TRACKING DYSFUNCTION, Genes, Dominant, Genetics, Middle Aged, Pedigree, Phenotype, Schizophrenia, Multigene Family, Female, Schizophrenic Psychology, Psychology, Adult, Genetic Markers, Personality Tests, Genotype, Quantitative Trait Loci, Quantitative trait locus, PREPULSE INHIBITION, Genetic determinism, quantitative trait, ENVIRONMENTAL-INFLUENCES, WORKING-MEMORY, COMPLEX PHENOTYPES, 5-FACTOR MODEL, CHROMOSOME 6P, LOCUS, medicine, Humans, psychophysiology, Allele, Alleles, Biological Psychiatry, Psychiatric Status Rating Scales, LINKAGE ANALYSIS, Heritability, medicine.disease, PERSONALITY STRUCTURE, Psychotic Disorders, personality, Endophenotype

Abstract

Background Schizophrenia is a highly heritable and complex disorder. Multiple genes are likely to be involved, complicating genetic research into the etiology of this disorder. Intermediate phenotypes or endophenotypes may facilitate genetic research if they display a simpler mode of transmission than schizophrenia itself, i.e., if they reflect more closely the underlying genetic effects. Methods Twenty-five multigenerational families with multiple members affected with schizophrenia (180 subjects) were administered an extensive neuropsychological, psychophysiological, and personality test battery. Familial correlations were calculated to select heritable traits. Subsequent heritability analysis followed by commingling and segregation analysis were performed to unravel the pattern of transmission and to estimate heritability. Results Five traits, including sensorimotor gating, openness, verbal fluency, early visual perception, and spatial working memory, showed moderate familial correlations. Heritability estimates for these traits ranged from 37% to 54%. A major gene model resembling dominant transmission was found for both sensorimotor gating and openness. Verbal fluency, early visual perception, and spatial working memory may be accounted for by polygenic, multifactorial, or environmental effects. Conclusions Only 2 of 13 candidate endophenotypes showed a simple mode of transmission useful for successful application in molecular genetic research: sensorimotor gating and openness. To our knowledge, this is the first study to investigate the pattern of transmission for these traits.

Published

2008

22. Comparative methylome analysis in solid tumors reveals aberrant methylation at chromosome 6p in nasopharyngeal carcinoma

Author

Wei Dai, Anne Wing Mui Lee, Maria Li Lung, Roger Kai Cheong Ngan, Victor Ho Fu Lee, Josephine Mun Yee Ko, Hong Zheng, Yue Cheng, Arthur Kwok Leung Cheung, Wai Tong Ng, and Chun Chung Yau

Subjects

Epigenomics, Cancer Research, Nasopharyngeal neoplasm, methylome, Methylation, Epigenesis, Genetic, Histones, Meta-Analysis as Topic, EBV, Neoplasms, medicine, Humans, Radiology, Nuclear Medicine and imaging, Epigenetics, Promoter Regions, Genetic, Cancer Biology, Nasopharyngeal Carcinoma, biology, Gene Expression Profiling, Carcinoma, Computational Biology, Nasopharyngeal Neoplasms, Illumina HumanMethylation450, DNA Methylation, medicine.disease, Molecular biology, Gene Expression Regulation, Neoplastic, Histone, Oncology, CpG site, Nasopharyngeal carcinoma, DNA methylation, biology.protein, Chromosome 6p, Chromosomes, Human, Pair 6, CpG Islands, Transcriptome

Abstract

Altered patterns of DNA methylation are key features of cancer. Nasopharyngeal carcinoma (NPC) has the highest incidence in Southern China. Aberrant methylation at the promoter region of tumor suppressors is frequently reported in NPC; however, genome-wide methylation changes have not been comprehensively investigated. Therefore, we systematically analyzed methylome data in 25 primary NPC tumors and nontumor counterparts using a high-throughput approach with the Illumina HumanMethylation450 BeadChip. Comparatively, we examined the methylome data of 11 types of solid tumors collected by The Cancer Genome Atlas (TCGA). In NPC, the hypermethylation pattern was more dominant than hypomethylation and the majority of de novo methylated loci were within or close to CpG islands in tumors. The comparative methylome analysis reveals hypermethylation at chromosome 6p21.3 frequently occurred in NPC (false discovery rate; FDR=1.33 × 10(-9) ), but was less obvious in other types of solid tumors except for prostate and Epstein-Barr virus (EBV)-positive gastric cancer (FDR10(-3) ). Bisulfite pyrosequencing results further confirmed the aberrant methylation at 6p in an additional patient cohort. Evident enrichment of the repressive mark H3K27me3 and active mark H3K4me3 derived from human embryonic stem cells were found at these regions, indicating both DNA methylation and histone modification function together, leading to epigenetic deregulation in NPC. Our study highlights the importance of epigenetic deregulation in NPC. Polycomb Complex 2 (PRC2), responsible for H3K27 trimethylation, is a promising therapeutic target. A key genomic region on 6p with aberrant methylation was identified. This region contains several important genes having potential use as biomarkers for NPC detection.

Published

2015

23. Production and identification of wheat-Agropyron cristatum 6P translocation lines

Author

Luan, Yang, Wang, Xiaoguang, Liu, Weihua, Li, Chunye, Zhang, Jinpeng, Gao, Ainong, Wang, Yandong, Yang, Xinming, and Li, Lihui

Published

2010

24. Independent replication and meta-analysis for endometriosis risk loci

Author

Sapkota, Yadav, Fassbender, Amelie, Bowdler, Lisa, Fung, Jenny, Peterse, Danielle, O, Dorien, Montgomery, Grant, Nyholt, Dale, D'Hooghe, Thomas, Sapkota, Yadav, Fassbender, Amelie, Bowdler, Lisa, Fung, Jenny, Peterse, Danielle, O, Dorien, Montgomery, Grant, Nyholt, Dale, and D'Hooghe, Thomas

Abstract

Endometriosis is a complex disease that affects 6-10% of women in their reproductive years and 20-50% of women with infertility. Genome-wide and candidate-gene association studies for endometriosis have identified 10 independent risk loci, and of these, nine (rs7521902, rs13394619, rs4141819, rs6542095, rs1519761, rs7739264, rs12700667, rs1537377, and rs10859871) are polymorphic in European populations. Here we investigate the replication of nine SNP loci in 998 laparoscopically and histologically confirmed endometriosis cases and 783 disease-free controls from Belgium. SNPs rs7521902, rs13394619, and rs6542095 show nominally significant (p <.05) associations with endometriosis, while the directions of effect for seven SNPs are consistent with the original reports. Association of rs6542095 at the IL1A locus with 'All' (p =.066) and 'Grade-B' (p =.01) endometriosis is noteworthy because this is the first successful replication in an independent population. Meta-analysis with the published results yields genome-wide significant evidence for rs7521902, rs13394619, rs6542095, rs12700667, rs7739264, and rs1537377. Notably, three coding variants in GREB1 (near rs13394619) and CDKN2B-AS1 (near rs1537377) also showed nominally significant associations with endometriosis. Overall, this study provides important replication in a uniquely characterized independent population, and indicates that the majority of the original genome-wide association findings are not due to chance alone.

Published

2015

25. Anesthetic management of a patient with chromosome 6p duplication: a case report

Author

Masanori Tsukamoto, Takeshi Yokoyama, and Saori Morinaga

Subjects

medicine.medical_specialty, Tube Size, business.industry, medicine.medical_treatment, General Anesthesia, Anesthetic management, Case Report, 030206 dentistry, Oral health, Dental care, Short stature, Surgery, 03 medical and health sciences, 0302 clinical medicine, Chromosome (genetic algorithm), 030202 anesthesiology, Gene duplication, Chromosome 6p, medicine, Airway management, medicine.symptom, Dental Care, business

Abstract

Chromosome 6p duplication is very rare and clinically characterized by short stature, mental retardation, and congenital heart diseases. Patients with mental retardation may present with poor oral health conditions. Dental treatment may need to be performed under general anesthesia in such patients. Our case report deals with induction of general anesthesia to a patient with chromosome 6p duplication, for dental treatment. The selection of a nasotracheal tube of an appropriate size, because of the patient's short stature, was especially important for airway management. In the present case, the patient with chromosome 6p duplication was intubated with a nasotracheal tube, which was not age-matched but adapted to the height and physique of the patient.

Published

2017

26. Karyotype-Phenotype Correlation in Partial Trisomies of the Short Arm of Chromosome 6: A Family Case Report and Review of the Literature

Author

A. Montaldi, Alessandro Castiglione, A. Martini, A. Alghisi, Roberto Bovo, Valeria Guaran, Giulia Zeri, Donato Gemmati, Laura Astolfi, and Elisa Orioli

Subjects

Male, Proband, Pathology, Trisomy, Chromosomal translocation, Choanal atresia, Translocation, Genetic, Congenital, CHARGE syndrome, Arnold-Chiari malformation type I, Chromosome 6p, Coagulation factor XIII, Congenital heart defects, Congenital ptosis, D-dimer, Hearing loss, Partial trisomy, Renal hypoplasia, Abnormalities, Multiple, Arnold-Chiari Malformation, Base Sequence, Choanal Atresia, Chromosomes, Human, Pair 6, Cytogenetic Analysis, Female, Heart Defects, Congenital, Humans, Karyotype, Phenotype, Renal Insufficiency, Sequence Analysis, DNA, Molecular Biology, Genetics, Genetics (clinical), Heart Defects, Arnold-Chiari malformation, Sensorineural hearing loss, Pair 6, Abnormalities, Multiple, Sequence Analysis, Human, medicine.medical_specialty, Translocation, Biology, Chromosomes, Genetic, medicine, Multiplex ligation-dependent probe amplification, Coagulation FXIII, DNA, medicine.disease

Abstract

The first child (proband) of nonconsanguineous Caucasian parents underwent genetic investigation because she was affected with congenital choanal atresia, heart defects and kidney hyposplasia with mild transient renal insufficiency. The direct DNA sequencing after PCR of the CHD7 gene, which is thought to be responsible for approximately 60-70% of the cases of CHARGE syndrome/association, found no mutations. The cytogenetic analysis (standard GTG banding karyotype) revealed the presence of extrachromosomal material on 10q. The chromosome analysis was completed with array CGH (30 kb resolution), MLPA and FISH, which allowed the identification of three 6p regions (6p.25.3p23 × 3): 2 of these regions are normally located on chromosome 6, and the third region is translocated to the long arm of chromosome 10. The same chromosomal rearrangement was subsequently found in the father, who was affected with congenital ptosis and progressive hearing loss, and in the proband's sister, the second child, who presented at birth with choanal atresia and congenital heart defects. The mutated karyotypes, which were directly inherited, are thought to be responsible for a variable phenotype, including craniofacial dysmorphisms, choanal atresia, congenital ptosis, sensorineural hearing loss, heart defects, developmental delay, and renal dysfunction. Nevertheless, to achieve a complete audiological assessment of the father, he underwent further investigation that revealed an increased level of the coagulation factor XIII (300% increased activity), fluctuating levels of fibrin D-dimer degradation products (from 296 to 1,587 ng/ml) and a homoplasmic mitochondrial DNA mutation: T961G in the MTRNR1 (12S rRNA) gene. He was made a candidate for cochlear implantation. Preoperative high-resolution computed tomography and magnetic resonance imaging of the temporal bone revealed the presence of an Arnold-Chiari malformation type I. To the best of our knowledge, this study is the second report on partial 6p trisomy that involves the 10q terminal region. Furthermore, we report the first case of documented Arnold-Chiari malformation type I and increased factor XIII activity associated with 6p trisomy. We present a comprehensive report of the familial cases and an exhaustive literature review.

Published

2013

27. Familial ureteral abnormalities syndrome: genomic mapping, clinical findings

Author

Klemme, LuAnn, Fish, Alfred J., Rich, Stephen, Greenberg, Beryl, Senske, Beverly, and Segall, Miriam

Published

1998

28. Karyotype-phenotype correlation in partial trisomies of the short arm of chromosome 6 : a family case report and review of the literature

Author

Castiglione, Alessandro, Guaran, V., Astolfi, L., Orioli, E., Zeri, G., Gemmati, D., Bovo, R., Montaldi, A., Alghisi, A., Martini, A., Castiglione, Alessandro, Guaran, V., Astolfi, L., Orioli, E., Zeri, G., Gemmati, D., Bovo, R., Montaldi, A., Alghisi, A., and Martini, A.

Abstract

The first child (proband) of nonconsanguineous Caucasian parents underwent genetic investigation because she was affected with congenital choanal atresia, heart defects and kidney hyposplasia with mild transient renal insufficiency. The direct DNA sequencing after PCR of the CHD7 gene, which is thought to be responsible for approximately 60-70% of the cases of CHARGE syndrome/association, found no mutations. The cytogenetic analysis (standard GTG banding karyotype) revealed the presence of extrachromosomal material on 10q. The chromosome analysis was completed with array CGH (30 kb resolution), MLPA and FISH, which allowed the identification of three 6p regions (6p.25.3p23 × 3): 2 of these regions are normally located on chromosome 6, and the third region is translocated to the long arm of chromosome 10. The same chromosomal rearrangement was subsequently found in the father, who was affected with congenital ptosis and progressive hearing loss, and in the proband's sister, the second child, who presented at birth with choanal atresia and congenital heart defects. The mutated karyotypes, which were directly inherited, are thought to be responsible for a variable phenotype, including craniofacial dysmorphisms, choanal atresia, congenital ptosis, sensorineural hearing loss, heart defects, developmental delay, and renal dysfunction. Nevertheless, to achieve a complete audiological assessment of the father, he underwent further investigation that revealed an increased level of the coagulation factor XIII (300% increased activity), fluctuating levels of fibrin D-dimer degradation products (from 296 to 1,587 ng/ml) and a homoplasmic mitochondrial DNA mutation: T961G in the MTRNR1 (12S rRNA) gene. He was made a candidate for cochlear implantation. Preoperative high-resolution computed tomography and magnetic resonance imaging of the temporal bone revealed the presence of an Arnold-Chiari malformation type I. To the best of our knowledge, this study is the second report on p

Published

2013

29. Subtelomeric 6p monosomy and 12q trisomy in a patient with a 46,XX,der(6)t(6;12)(p25.3;q24.31) karyotype: Phenotypic overlap with Mutchinick syndrome

Author

Semerci, C.Nur, Cinbiş, Mine, Ullmann, R., Steininger, A., Bahce, M., Yağcı, Baki, Özden, Serap, Sabir, N., Gumus, D., Tepeli, E., Arteaga, J., and Mutchinick, O.M.

Subjects

Male, congenital heart malformation, partial monosomy, ear malformation, Trisomy, motor retardation, Valgus, preschool child, speech disorder, Translocation, Genetic, X chromosome, trisomy 12, Monosomy, low set ear, newborn, Pregnancy, genetics, Child, Subtelomeric 6p deletion, In Situ Hybridization, Fluorescence, lower lip, telomere, Comparative Genomic Hybridization, hypertelorism, adult, article, clinodactyly, Syndrome, karyotyping, chromosome 12, chromosome 12q, female, Phenotype, priority journal, Child, Preschool, psychomotor developmental delay, young adult, Chromosomes, Human, Pair 6, foxf2 gene, foot malformation, lip malformation, eye malformation, skeleton malformation, aCGH, FISH, mental deficiency, case report, Humans, chromosome 6, human, Partial trisomy 12q, transcription factor FOXC1, gene, fluorescence in situ hybridization, hearing loss, Chromosomes, Human, X, Chromosomes, Human, Pair 12, gene deletion, Infant, Newborn, Mutchinick syndrome, chromosome 6p, genetic disorder, gene translocation, karyotype 46,XX, pes valgus

Abstract

We report on a patient with partial monosomy 6p and partial trisomy 12q identified by fluorescent in situ hybridization (FISH) and array-based comparative genomic hybridization (aCGH). She had a complex phenotype characterized by mental retardation (MR), psychomotor developmental delay, speech disorder, hypertelorism, eye anomalies, hearing loss, low-set malformed ears, thin upper lip, heart defect, clinodactyly, pes valgus, and skeletal anomalies. There is phenotypic overlap between our case and Mutchinick syndrome. This is the first report of a combined partial monosomy 6p and partial trisomy 12q due to an unbalanced translocation between subtelomeric regions of these chromosomes. © 2010 Wiley-Liss, Inc.

Published

2010

30. Common variants at the MHC locus and at chromosome 16q24.1 predispose to Barrett's esophagus

Author

Su, Zhan, Gay, Laura, Strange, Amy, Palles, Claire, Band, Gavin, Whiteman, David, Lescai, Francesco, Langford, Cordelia, Nanji, Manoj, Brown, Matthew, other, and, Su, Zhan, Gay, Laura, Strange, Amy, Palles, Claire, Band, Gavin, Whiteman, David, Lescai, Francesco, Langford, Cordelia, Nanji, Manoj, Brown, Matthew, and other, and

Abstract

Barrett's esophagus is an increasingly common disease that is strongly associated with reflux of stomach acid and usually a hiatus hernia, and it strongly predisposes to esophageal adenocarcinoma (EAC), a tumor with a very poor prognosis. We report the first genome-wide association study on Barrett's esophagus, comprising 1,852 UK cases and 5,172 UK controls in the discovery stage and 5,986 cases and 12,825 controls in the replication stage. Variants at two loci were associated with disease risk: chromosome 6p21, rs9257809 (P combined = 4.09 × 10-9; odds ratio (OR) = 1.21, 95% confidence interval (CI) =1.13-1.28), within the major histocompatibility complex locus, and chromosome 16q24, rs9936833 (P combined = 2.74 × 10-10; OR = 1.14, 95% CI = 1.10-1.19), for which the closest protein-coding gene is FOXF1, which is implicated in esophageal development and structure. We found evidence that many common variants of small effect contribute to genetic susceptibility to Barrett's esophagus and that SNP alleles predisposing to obesity also increase risk for Barrett's esophagus. © 2012 Nature America, Inc. All rights reserved.

Published

2012

31. A human phenome-interactome network of protein complexes implicated in genetic disorders

Author

Zeynep Tümer, Anders Gorm Pedersen, Flemming Pociot, Páll Ísólfur Ólason, Anders M. Hinsby, Kasper Lage, Niels Tommerup, Zenia M Størling, Yves Moreau, Olga Rigina, E. Olof Karlberg, and Søren Brunak

Subjects

Proteomics, Candidate gene, Proteome, Protein Conformation, Biomedical Engineering, Bioengineering, nijmegen breakage syndrome, Disease, Phenome, Biology, Applied Microbiology and Biotechnology, Interactome, Databases, Genetic, Protein Interaction Mapping, medicine, Humans, Genetic Predisposition to Disease, Databases, Protein, Genetics, inflammatory-bowel-disease, SISTA, Genetic Diseases, Inborn, Proteins, Bayes Theorem, prioritization, medicine.disease, mutations, Phenotype, ovarian-cancer, molecular interaction database, interaction map, chromosome 6p, Mutation, Molecular Medicine, Alzheimer's disease, candidate genes, linkage, Biotechnology

Abstract

We performed a systematic, large-scale analysis of human protein complexes comprising gene products implicated in many different categories of human disease to create a phenome-interactome network. This was done by integrating quality-controlled interactions of human proteins with a validated, computationally derived phenotype similarity score, permitting identification of previously unknown complexes likely to be associated with disease. Using a phenomic ranking of protein complexes linked to human disease, we developed a Bayesian predictor that in 298 of 669 linkage intervals correctly ranks the known disease-causing protein as the top candidate, and in 870 intervals with no identified disease-causing gene, provides novel candidates implicated in disorders such as retinitis pigmentosa, epithelial ovarian cancer, inflammatory bowel disease, amyotrophic lateral sclerosis, Alzheimer disease, type 2 diabetes and coronary heart disease. Our publicly available draft of protein complexes associated with pathology comprises 506 complexes, which reveal functional relationships between disease-promoting genes that will inform future experimentation. ispartof: Nature Biotechnology vol:25 issue:3 pages:309-316 ispartof: location:United States status: published

Published

2007

32. Chromosome 6p Influences on Different Dyslexia-Related Cognitive Processes: Further Confirmation

Author

Frank B. Wood, David L. Pauls, Marianne S. Meyer, and Elena L. Grigorenko

Subjects

Adult, Vocabulary, Adolescent, Genetic Linkage, media_common.quotation_subject, Developmental psychology, Dyslexia, Cognition, Gene Frequency, DCDC2, Quantitative-trait loci (QTL), Report, Genetics, medicine, Humans, Genetics(clinical), Language disorder, Child, Rapid automatized naming, Genetics (clinical), Alleles, media_common, Family Health, Polymorphism, Genetic, Phonemic awareness, Models, Genetic, Chromosome Mapping, Reproducibility of Results, medicine.disease, Spelling, Phenotype, Reading, Sample Size, Chromosome 6p, Chromosomes, Human, Pair 6, Psychology, Software

Abstract

Summary In this study, which is a continuation and an extension of an earlier study, we enrolled two new families ( N =31) and recruited more individuals from the previously ascertained families ( N =56). The eight multiplex families ( N =171) presented in this study were ascertained from a sample of adult probands whose childhood reading history is well documented through archival information. Six phenotypes were constructed to span a range of dyslexia-related cognitive processes. These phenotypes were (1) phonemic awareness (of spoken words); (2) phonological decoding (of printed nonwords); (3) rapid automatized naming (of colored squares or object drawings); (4) single-word reading (orally, of printed real words); (5) vocabulary; and (6) spelling (of dictated words). In addition, the diagnosis of lifelong dyslexia was established by clinical means. Genotyping was done with nine highly polymorphic markers from the 6p22.3–6p21.3 region. The results of two- and multipoint identity-by-descent and identity-by-state analyses supported the importance of a putative locus in the D6S464–D6S273 region for a number of dyslexia-related cognitive deficits.

Published

2000

33. Anesthetic management of a patient with chromosome 6p duplication: a case report.

Author

Morinaga S, Tsukamoto M, and Yokoyama T

Abstract

Chromosome 6p duplication is very rare and clinically characterized by short stature, mental retardation, and congenital heart diseases. Patients with mental retardation may present with poor oral health conditions. Dental treatment may need to be performed under general anesthesia in such patients. Our case report deals with induction of general anesthesia to a patient with chromosome 6p duplication, for dental treatment. The selection of a nasotracheal tube of an appropriate size, because of the patient's short stature, was especially important for airway management. In the present case, the patient with chromosome 6p duplication was intubated with a nasotracheal tube, which was not age-matched but adapted to the height and physique of the patient.

Published

2017

34. Construction of a YAC contig spanning human chromosome 6p22

Author

Brunella Franco, Antonella Roetto, Clara Camaschella, Carla Jodice, Andrea Novelletto, Flavia Trettel, Patrizia Malaspina, Massimo Carella, Paola Blasi, and Marina Frontali

Subjects

Genetic Markers, gene locus, polymerase chain reaction, Pcr assay, dna marker, article, centromere, chromosome 6p, gene mapping, human, priority journal, Chromosome Mapping, Chromosomes, Artificial, Yeast, Chromosomes, Human, Pair 6, Humans, Repetitive Sequences, Nucleic Acid, Biology, Repetitive Sequences, Chromosomes, Gene mapping, SEQUENCE TAGS ESTS, HUMAN GENOME, REPEAT POLYMORPHISM, HUMAN MHC, MAP, REGION, GENE, ASSIGNMENT, LOCUS, DNA, Genetics, Gene, Contig, Nucleic Acid, food and beverages, Chromosome, Yeast, Settore BIO/18 - Genetica, Genetic marker, Artificial, Pair 6, Human

Abstract

A contig covering human chromosome 6p22 that consists of 134 YAC clones aligned based on the presence/absence of 52 DNA markers is presented. This contig overlaps with the 6p23 contig at its telomeric end and with the 6p21.3 contig at its centromeric end. The order of loci within the contig resolves the relative positions of several genetically mapped markers. Among the additional markers used here, there are eight novel PCR assays. The 12 known genes and anonymous ESTs located within the contig establish a first step toward a transcriptional map of this region. The instability of YAC clones observed during this work is also discussed.

Published

1996

35. Structure-Based Analysis of Five Novel Disease-Causing Mutations in 21-Hydroxylase-Deficient Patients

Author

Eduardo H. Charreau, Carolina Minutolo, Alejandro D. Nadra, Noemí Buzzalino, Cecilia Fernández, Liliana Alba, Bárbara Casali, Liliana Dain, Melisa Taboas, and Susana Belli

Subjects

Models, Molecular, frameshift mutation, sequence analysis, genotype, pseudogene, Structure Prediction, lcsh:Medicine, medicine.disease_cause, Biochemistry, cytochrome P450 2C21, Autosomal Recessive, Macromolecular Structure Analysis, Pathology, genetics, exon, gene mutation, lcsh:Science, CYP21A2 protein, human, Genetics, Mutation, Multidisciplinary, Protein Stability, article, Nucleic acid sequence, Esteroide 21-Hidroxilasa, Genomics, structure analysis, unclassified drug, Enzymes, heterozygote detection, Mammalia, Medicine, point mutation, Algorithms, Research Article, Protein Structure, Clinical Pathology, phenotype, Pseudogene, Argentina, Biology, chemistry, Frameshift mutation, Molecular Genetics, promoter region, Genetic Mutation, Diagnostic Medicine, steroid 21 monooxygenase, salt wasting, medicine, congenital adrenal hyperplasia, Humans, Genetic Predisposition to Disease, Congenital adrenal hyperplasia, human, protein structure, steroid 21 monooxygenase deficiency, Clinical Genetics, algorithm, FoldX, Mutación, Adrenal Hyperplasia, Congenital, gene deletion, Point mutation, lcsh:R, Proteins, Computational Biology, nucleotide sequence, Human Genetics, case control study, medicine.disease, Molecular biology, cytochrome P450 2C, Metabolism, Inborn error of metabolism, Case-Control Studies, chromosome 6p, Enzyme Structure, Genetics of Disease, chemical structure, lcsh:Q, Steroid 21-Hydroxylase, genetic predisposition

Abstract

Congenital adrenal hyperplasia (CAH) due to 21-hydroxylase deficiency is the most frequent inborn error of metabolism, and accounts for 90–95% of CAH cases. The affected enzyme, P450C21, is encoded by the CYP21A2 gene, located together with a 98% nucleotide sequence identity CYP21A1P pseudogene, on chromosome 6p21.3. Even though most patients carry CYP21A1P-derived mutations, an increasing number of novel and rare mutations in disease causing alleles were found in the last years. In the present work, we describe five CYP21A2 novel mutations, p.R132C, p.149C, p.M283V, p.E431K and a frameshift g.2511_2512delGG, in four non-classical and one salt wasting patients from Argentina. All novel point mutations are located in CYP21 protein residues that are conserved throughout mammalian species, and none of them were found in control individuals. The putative pathogenic mechanisms of the novel variants were analyzed in silico. A three-dimensional CYP21 structure was generated by homology modeling and the protein design algorithm FoldX was used to calculate changes in stability of CYP21A2 protein. Our analysis revealed changes in protein stability or in the surface charge of the mutant enzymes, which could be related to the clinical manifestation found in patients. Fil: Minutolo, Carolina. ANLIS Dr.C.G.Malbrán. Centro Nacional de Genética Médica Dr. Eduardo Castilla; Argentina. Fil: Nadra, Alejandro D. Universidad de Buenos Aires. Departamento de Fisiologı´a Biologı´a Molecular y Celular; Argentina. Fil: Fernández, Cecilia. ANLIS Dr.C.G.Malbrán. Centro Nacional de Genética Médica Dr. Eduardo Castilla; Argentina. Fil: Taboas, Melisa. ANLIS Dr.C.G.Malbrán. Centro Nacional de Genética Médica Dr. Eduardo Castilla; Argentina. Fil: Buzzalino, Noemí. ANLIS Dr.C.G.Malbrán. Centro Nacional de Genética Médica Dr. Eduardo Castilla; Argentina. Fil: Casali, Bárbara. ANLIS Dr.C.G.Malbrán. Centro Nacional de Genética Médica Dr. Eduardo Castilla; Argentina. Fil: Belli, Susana. Hospital Durand. División Endocrinología; Argentina. Fil: Charreau, Eduardo H. Instituto de Biología y Medicina Experimental; Argentina. Fil: Alba, Liliana. ANLIS Dr.C.G.Malbrán. Centro Nacional de Genética Médica Dr. Eduardo Castilla; Argentina. Fil: Dain, Liliana. ANLIS Dr.C.G.Malbrán. Centro Nacional de Genética Médica Dr. Eduardo Castilla; Argentina.

Published

2011

36. Population cytogenetics of aphidicolin-induced fragile sites

Author

B. Tedeschi, B. Nicoletti, Patrizia Vernole, and Maria Lucia Sanna

Subjects

Male, Population genetics, cytogenetics, Middle Age, chemistry.chemical_compound, chromosome 1p, chromosome 5q, newborn, Prevalence, Chromosomes, Human, Lymphocytes, Child, Non-U.S. Gov't, Genetics (clinical), Genetics, education.field_of_study, Chromosomal fragile site, Chromosome Fragile Sites, adult, Settore BIO/13, article, chromosome analysis, Age Factors, Chromosome Fragility, Middle Aged, chromosome 16p, aged, female, chromosome 4q, priority journal, Child, Preschool, Support, Human, Aphidicolin, medicine.medical_specialty, Adolescent, Population, Biology, aphidicolin, Chromosomes, lymphocyte culture, chromosome 3q, Sex Factors, chromosome 3p, chromosome fragile site, chromosome 7q, medicine, Humans, chromosome Xp, sex, normal human, education, Preschool, Chromosome Aberrations, Chi-Square Distribution, adolescent, age, child, chromosome 10q, chromosome 14q, chromosome 2q, chromosome 6p, chromosome 6q, human, human cell, infant, male, population genetics, Adult, Aged, Cytogenetics, Female, Genetics, Population, Infant, Infant, Newborn, Support, Non-U.S. Gov't, Human genetics, chemistry, Chromosome Fragile Site

Abstract

Chromosome fragile sites are inducible by aphidicolin in cultured human lymphocytes. To assess the frequency and distribution of these common fragile sites in the general population, a cytogenetic survey was performed on 126 subjects, 59 males and 67 females, whose age ranged from 1 day to 72 years. Common fragile sites, induced by aphidicolin, were widespread and showed a remarkably different sensitivity among individuals; age influenced the overall frequency of fragile sites. Moreover, both age and sex seemed to modulate the expression of specific fragile sites. In our population, the most common fragile sites were: 3p14, 16q23, Xp22, 6q26, 1p31, 4q31, 1p22, 7q22, 2q33, 3q27, 2q31, 7q32, 14q24, 10q22, 5q31, 2q37, 6p21.

Published

1992