Your search keyword '"chromosome 12q"' showing total 5 results

1. A Second Locus for Familial High Myopia Maps to Chromosome 12q

Author

Larry D. Atwood, Douglas J. Wilkin, Terri L. Young, William S. Oetting, Scott C. Wildenberg, Shawn M. Ronan, Richard A. King, and Alison B. Alvear

Subjects

Adult, Genetic Markers, Male, Marfan syndrome, genetic structures, Glaucoma, Locus (genetics), Marfan Syndrome, Gene mapping, Genetic linkage, Germany, medicine, Myopia, Genetics, Humans, Chromosome 12q, Genetics(clinical), Pathologic myopia, Age of Onset, Child, Genetics (clinical), Aged, Recombination, Genetic, Chromosomal mapping, Chromosomes, Human, Pair 12, business.industry, Genetic heterogeneity, Chromosome Mapping, Middle Aged, medicine.disease, Introns, United States, eye diseases, Pedigree, Autosomal dominant, Italy, Child, Preschool, Eye disorder, Female, sense organs, Age of onset, business, Linkage analysis, Research Article

Abstract

SummaryMyopia, or nearsightedness, is the most common eye disorder worldwide. “Pathologic” high myopia, or myopia of ≤−6.00 diopters, predisposes individuals to retinal detachment, macular degeneration, cataract, or glaucoma. A locus for autosomal dominant pathologic high myopia has been mapped to 18p11.31. We now report significant linkage of high myopia to a second locus at the 12q21-23 region in a large German/Italian family. The family had no clinical evidence of connective-tissue abnormalities or glaucoma. The average age at diagnosis of myopia was 5.9 years. The average spherical-component refractive error for the affected individuals was −9.47 diopters. Markers flanking or intragenic to the genes for the 18p locus, Stickler syndromes type I and II (12q13.1-q13.3 and 6p21.3), Marfan syndrome (15q21.1), and juvenile glaucoma (chromosome 1q21-q31) showed no linkage to the myopia in this family. The maximum LOD score with two-point linkage analysis in this pedigree was 3.85 at a recombination fraction of .0010, for markers D12S1706 and D12S327. Recombination events identified markers D12S1684 and D12S1605 as flanking markers that define a 30.1-cM interval on chromosome 12q21-23, for the second myopia gene. These results confirm genetic heterogeneity of myopia. The identification of this gene may provide insight into the pathophysiology of myopia and eye development.

Published

1998

2. 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

3. Pitfalls of mapping a large Turkish consanguineous family with vertical monilethrix inheritance

Author

Celep, F., Uzumcu, A., Sonmez, F.M., Uyguner, O., Isik Balci, Y., Bahadir, S., and Karaguzel, A.

Subjects

gene segregation, mutational analysis, Male, haplotype, Keratins, Type II, Turkey, Dominant inheritance, gene sequence, Polymorphism, Single Nucleotide, preschool child, Turkey (republic), monilethrix, Consanguinity, genetic linkage, Single nucleotide polymorphism (SNP), HHb6 coding keratin gene (KRT86), single nucleotide polymorphism, Keratins, Hair-Specific, Humans, human, gene mutation, gene, Family Health, segregation analysis, child, clinical article, integumentary system, Genetic Screening, hHb6 coding keratin gene, article, microsatellite marker, Chromosome Mapping, gene mapping, heterozygote, clinical feature, Pedigree, autosomal dominant inheritance, chromosome 12q, female, tandem repeat, Haplotypes, Hotspot mutations, Child, Preschool, vertical transmission, homozygosity, Hair Diseases

Abstract

Pitfalls of mapping a large Turkish consanguineous family with vertical monilethrix inheritance: Monilethrix, a rare autosomal dominant disease characterized by hair fragility and follicular hyperkeratosis, is caused by mutations in three type II hair cortex keratins. The human keratin family comprises 54 members, 28 type I and 26 type II. The phenotype shows variable penetrance and results in hair fragility and patchy dystrophic alopecia. In our study, Monilethrix was diagnosed on the basis of clinical characteristics and microscopic examination in a family with 11 affected members. Haplotype analysis was performed by three Simple Tandem Repeat markers (STR) and KRT86 gene was sequenced for the identification of the disease causing mutation. In the results of this, autosomal dominant mutation (E402K) in exon 7 of KRT86 gene was identified as a cause of Moniltherix in the large family from Turkey.

Published

2009

4. MITOSTATIN, a putative tumor suppressor on chromosome 12q24.1, is downregulated in human bladder and breast cancer

Author

V. Anesti, Raffaele Baffa, Andrea Vecchione, Gustavo Baldassarre, Silvia Goldoni, Matteo Fassan, Joshua Lloyd, Luca Scorrano, Andrea Morrione, Leonard G. Gomella, Domenico D'Arca, Juan P. Palazzo, Renato V. Iozzo, and Dolores Byrne

Subjects

Male, Cancer Research, HSP27 Heat-Shock Proteins, Apoptosis, HSP27, medicine.disease_cause, law.invention, 0302 clinical medicine, law, COMPARATIVE GENOMIC HYBRIDIZATION, Genes, Tumor Suppressor, RNA, Neoplasm, Cloning, Molecular, IN-VIVO, Heat-Shock Proteins, Tumor Stem Cell Assay, Regulation of gene expression, Genetics, 0303 health sciences, Gene knockdown, Bladder cancer, 3. Good health, PROSTATE-CANCER, Mitochondria, Neoplasm Proteins, mitochondria, chromosome 12q, Gene Expression Regulation, Neoplastic, Cell Transformation, Neoplastic, 030220 oncology & carcinogenesis, SMALL STRESS-PROTEINS, Chromosomal region, Disease Progression, bladder cancer, Female, Cell Division, Tumor suppressor gene, tumor suppressor, Recombinant Fusion Proteins, Molecular Sequence Data, Down-Regulation, Breast Neoplasms, Biology, HEAT-SHOCK-PROTEIN, BINDING PROTEIN, Article, breast cancer, GROWTH-FACTOR RECEPTOR, CELL CARCINOMA, ANDROGEN ABLATION, 03 medical and health sciences, Hsp27, Species Specificity, Cell Line, Tumor, medicine, Animals, Humans, RNA, Messenger, Molecular Biology, 030304 developmental biology, Chromosomes, Human, Pair 12, Tumor Suppressor Proteins, Cancer, medicine.disease, Urinary Bladder Neoplasms, biology.protein, Cancer research, Suppressor, Carcinogenesis, Carrier Proteins, Molecular Chaperones

Abstract

Allelic deletions on human chromosome 12q24 are frequently reported in a variety of malignant neoplasms, indicating the presence of a tumor suppressor gene(s) in this chromosomal region. However, no reasonable candidate has been identified so far. In this study, we report the cloning and functional characterization of a novel mitochondrial protein with tumor suppressor activity, henceforth designated MITOSTATIN. Human MITOSTATIN was found within a 3.2-kb transcript, which encoded a approximately 62 kDa, ubiquitously expressed protein with little homology to any known protein. We found homozygous deletions and mutations of MITOSTATIN gene in approximately 5 and approximately 11% of various cancer-derived cells and solid tumors, respectively. When transiently overexpressed, MITOSTATIN inhibited colony formation, tumor cell growth and was proapoptotic, all features shared by established tumor suppressor genes. We discovered a specific link between MITOSTATIN overexpression and downregulation of Hsp27. Conversely, MITOSTATIN knockdown cells showed an increase in cell growth and cell survival rates. Finally, MITOSTATIN expression was significantly reduced in primary bladder and breast tumors, and its reduction was associated with advanced tumor stages. Our findings support the hypothesis that MITOSTATIN has many hallmarks of a classical tumor suppressor in solid tumors and may play an important role in cancer development and progression.

Published

2009

5. Linkage disequilibrium and demographic history of the isolated population of the Faroe Islands

Author

Tove H. Jorgensen, Gursharan Kalsi, Andrew McQuillin, Torben A Kruse, Ole Mors, Henrik Ewald, Birte Degn, Maria Vang, Hugh Gurling, and August G. Wang

Subjects

Linkage disequilibrium, demography, haplotype, Denmark, Variation (Genetics), genetic analysis, Linkage Disequilibrium, genetic variability, Atlantic Islands, Association mapping, Genetics (clinical), chromosome map, education.field_of_study, Linkage Disequilibrium Mapping, article, microsatellite marker, Chromosome Mapping, bottleneck population, chromosome 12, chromosome 12q, priority journal, Microsatellite, genetic marker, history, Genetic Markers, Demographic history, Population, Biology, randomization, Gene mapping, Genetic drift, Genetics, Humans, Faroe Islands, controlled study, human, Support, Non-U.S. Gov't, education, Demography, Chromosomes, Human, Pair 12, population genetics, Atlantic Islands, Genetic Variation, gene mapping, United Kingdom, gene linkage disequilibrium, Atlantic islands, Genetics, Population, Haplotypes, Evolutionary biology, Humans, microsatellite DNA, genetic disorder, genetic drift, population research, Microsatellite Repeats

Abstract

The isolated population of the Faroe Islands has a history of recent expansion after being limited to a small size for centuries. Such an isolated population may be ideal for linkage disequilibrium mapping of disease genes if linkage disequilibrium (LD) extends over large regions. Analyses of 18 markers on 12q24.3, spanning a region of 4.3 Mb (16 cM), revealed extensive LD in the Faroese population. Maximum LD was found between marker pairs separated by more than 3.8 Mb. The same region had a maximum LD of only 1.2 and 1.4 Mb respectively in two outbred Danish and British populations analysed here for comparison. The analyses of gene diversity excess at 15 unlinked microsatellite markers did not reveal any sign of a severe bottleneck to have occurred within approximately 1200 years' history of the Faroese population. The extensive LD in this population may, therefore, have arisen primarily by random genetic drift. The implications for future gene mapping studies are discussed.

Published

2002