Your search keyword '"Yumiko Ishikawa-Brush"' showing total 14 results

1. Effects on promoter activity of common SNPs in 5′ region of GABRB3 exon 1A

Author

Miyabi Tanaka, Antonio V. Delgado-Escueta, Richard W. Olsen, Yumiko Ishikawa-Brush, Julia N. Bailey, and Dongsheng Bai

Subjects

Genetics, Exon, Neurology, Repressor, Promoter, Luciferase, Neurology (clinical), Allele, Biology, Enhancer, Gene, Allele frequency, Molecular biology

Abstract

Summary Purpose: The β3 subunit of the γ-aminobutyric acid type A receptors (GABAA–Rs) is an essential component of GABAA–Rs in fetal, perinatal, and adult mammalian brain. Various transcripts of the β3 subunit gene (GABRB3) produce various proteins with different N-termini. Rare variants in this N-terminus (exon 1A and exon 2) of GABRB3 protein segregate in affected family members of two multigeneration-multiplex families with remitting childhood absence epilepsy (rCAE), suggesting GABRB3 is a major Mendelian epilepsy gene for rare families with CAE. Therefore, the N-terminus of GABRB3 could be important for GABRB3 regulation in development, and its alteration could produce rCAE. Herein we determine if single nucleotide polymorphisms (SNPs) within the 1,148-bp region upstream from exon 1A influence the expression of GABRB3. Methods: We studied luciferase reporter expression for promoter activity, 1,148-bp upstream from exon 1A, using human embryonic kidney 293 cells. We generated constructs of the promoter region and compared different SNP haplotypes in 48 patients with rCAE. Next, we compared frequencies of rs20317, located in the core promoter region, and rs4906902, located in the enhancer region between 48 patients with rCAE and >500 healthy controls matched for ethnicity and ancestral origin. Key Findings: Highest luciferase expression occurred 230-bp upstream of exon 1A. The construct that excluded this region lost luciferase activity. Therefore, this region contains the core promoter of exon 1A. Allele C but not allele G (rs20317) significantly increased luciferase expression activity. Allele C creates binding motifs for cMYB and EGR-3. Longer constructs overlapping this region have a binding motif for REST (RE1-silencing transcription factor), a critical epigenetic modulator for neuronal genes. REST represses expression of neuronal genes in nonneuronal tissues, resulting in reduced luciferase expression activity. Even in the suppressed condition, the longer construct enhanced luciferase expression activity of the shorter construct, which excluded the distal end containing rs4906902. However, allele frequencies of rs20317 and rs4906902 were not significantly associated with 48 rCAE patients in comparison to >500 controls matched for ethnicity and ancestral origin. Significance: Common SNPs in the promoter region increase luciferase expression activity. An epigenetic modulator, REST, specifically alters expression of GABRB3 exon 1A transcripts, suggesting epigenetic regulation by REST dominantly controls the expression of GABRB3 variant 2 transcript in early life GABAA signaling. Abnormal epigenetic regulation could be involved in absence seizures.

Published

2012

2. Structure−Function Analysis of the Auxilin J-Domain Reveals an Extended Hsc70 Interaction Interface

Author

Jianwen Jiang, Alexander B. Taylor, Eileen M. Lafer, Rui J Sousa, Kondury Prasad, Yumiko Ishikawa-Brush, and P. John Hart

Subjects

Models, Molecular, HSC70 Heat-Shock Proteins, Auxilins, Molecular Sequence Data, Static Electricity, Plasma protein binding, Auxilin, In Vitro Techniques, Biology, Biochemistry, Protein structure, Animals, Humans, HSP70 Heat-Shock Proteins, Amino Acid Sequence, Surface plasmon resonance, Binding site, Binding Sites, Sequence Homology, Amino Acid, Peptide Fragments, Protein Structure, Tertiary, Crystallography, Directed mutagenesis, Helix, Mutagenesis, Site-Directed, Cattle

Abstract

J-domains are widespread protein interaction modules involved in recruiting and stimulating the activity of Hsp70 family chaperones. We have determined the crystal structure of the J-domain of auxilin, a protein which is involved in uncoating clathrin-coated vesicles. Comparison to the known structures of J-domains from four other proteins reveals that the auxilin J-domain is the most divergent of all J-domain structures described to date. In addition to the canonical J-domain features described previously, the auxilin J-domain contains an extra N-terminal helix and a long loop inserted between helices I and II. The latter loop extends the positively charged surface which forms the Hsc70 binding site, and is shown by directed mutagenesis and surface plasmon resonance to contain side chains important for binding to Hsc70.

Published

2003

3. A Genomewide Scan Identifies Two Novel Loci Involved in Specific Language Impairment**Members of the consortium are listed in the Appendix

Author

Dianne F. Newbury, M. J. Merricks, Vicky Slonims, Peter Joseph Benedict Helms, Angela J. Marlow, Dorothy V. M. Bishop, Gillian Baird, Simon E. Fisher, Yumiko Ishikawa-Brush, Ian M. Goodyer, Gina Conti-Ramsden, Patrick Bolton, Anthony P. Monaco, Carol Stott, L. Jannoun, J. D. Cleak, and Andrew Pickles

Subjects

Genetics, 0303 health sciences, Concordance, Locus (genetics), Specific language impairment, Biology, Quantitative trait locus, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, Chromosome 16, Genetic linkage, medicine, Genetics(clinical), Nuclear family, 030217 neurology & neurosurgery, Genetics (clinical), X chromosome, 030304 developmental biology

Abstract

Approximately 4% of English-speaking children are affected by specific language impairment (SLI), a disorder in the development of language skills despite adequate opportunity and normal intelligence. Several studies have indicated the importance of genetic factors in SLI; a positive family history confers an increased risk of development, and concordance in monozygotic twins consistently exceeds that in dizygotic twins. However, like many behavioral traits, SLI is assumed to be genetically complex, with several loci contributing to the overall risk. We have compiled 98 families drawn from epidemiological and clinical populations, all with probands whose standard language scores fall > or =1.5 SD below the mean for their age. Systematic genomewide quantitative-trait-locus analysis of three language-related measures (i.e., the Clinical Evaluation of Language Fundamentals-Revised [CELF-R] receptive and expressive scales and the nonword repetition [NWR] test) yielded two regions, one on chromosome 16 and one on 19, that both had maximum LOD scores of 3.55. Simulations suggest that, of these two multipoint results, the NWR linkage to chromosome 16q is the most significant, with empirical P values reaching 10(-5), under both Haseman-Elston (HE) analysis (LOD score 3.55; P=.00003) and variance-components (VC) analysis (LOD score 2.57; P=.00008). Single-point analyses provided further support for involvement of this locus, with three markers, under the peak of linkage, yielding LOD scores >1.9. The 19q locus was linked to the CELF-R expressive-language score and exceeds the threshold for suggestive linkage under all types of analysis performed-multipoint HE analysis (LOD score 3.55; empirical P=.00004) and VC (LOD score 2.84; empirical P=.00027) and single-point HE analysis (LOD score 2.49) and VC (LOD score 2.22). Furthermore, both the clinical and epidemiological samples showed independent evidence of linkage on both chromosome 16q and chromosome 19q, indicating that these may represent universally important loci in SLI and, thus, general risk factors for language impairment

Published

2002

4. Construction of a YAC contig spanning the Xq13.3 subband

Author

Laurent Villard, Anne-Marie Lossi, Michel Fontes, Jamel Chelly, Jozef Gecz, Yumiko Ishikawa-Brush, Laurence Colleaux, and Anthony P. Monaco

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Candidate gene, X Chromosome, Transcription, Genetic, Centromere, Molecular Sequence Data, Biology, Polymerase Chain Reaction, DNA sequencing, Bacterial Proteins, Gene mapping, Pregnancy, Genetics, Humans, Deoxyribonucleases, Type II Site-Specific, Chromosomes, Artificial, Yeast, X chromosome, Sequence Tagged Sites, Base Sequence, Contig, DNA–DNA hybridization, Chromosome Mapping, genomic DNA, Chromosomal region, Female

Abstract

The loci involved in several X-linked mental retardation syndromes have been linked to the pericentromeric region of the X chromosome long arm (Xq 12-q21). To isolate candidate genes for these diseases, the authors set up the construction of YAC contigs spanning this region. Two of these syndromes (the Juberg-Marsidi syndrome and the {alpha}-thalessemia mental retardation syndrome) have been recently linked, with high lod scores, to polymorphic probes previously assigned to Xq13.3. The authors therefore constructed a first YAC contig, encompassing this band, from DXS441 to PGK1. The physical map, deduced from the isolated clones, extends over 2.1 Mb of genomic DNA. Restriction analysis of the YAC contig allowed mapping precisely the loci previously assigned to that chromosomal region and to define their relative order. The validity of this physical map has been checked by comparing SfiI digest of the YACs to genomic fragments obtained with the same enzyme. A cDNA selection approach, already performed with a previous partial contig, has been extended to cover the whole region. 26 refs., 5 figs., 2 tabs.

Published

1995

5. Autism, mental retardation, multiple exostoses and short stature in a female with 46,X,t(X;8)(p22.13;q22.1)

Author

Anthony P. Monaco, Patrick Bolton, John Powell, Michael Rutter, Yumiko Ishikawa-Brush, Veronica J. Buckle, and John R.W. Yates

Subjects

Adult, X Chromosome, Chromosome Disorders, Dwarfism, Chromosomal translocation, Biology, Short stature, Translocation, Genetic, Pregnancy, Intellectual Disability, Chromosomal Abnormality, Genetics, medicine, Humans, Abnormalities, Multiple, Autistic Disorder, Young adult, Biological Psychiatry, Genetics (clinical), Chromosome Aberrations, Asphyxia Neonatorum, Multiple exostosis, Breakpoint, Infant, Newborn, medicine.disease, Phenotype, Obstetric Labor Complications, Psychiatry and Mental health, Hematoma, Subdural, Autism, Female, medicine.symptom, Exostoses, Multiple Hereditary, Chromosomes, Human, Pair 8

Abstract

A young adult female with multiple exostoses, short stature, autism, mental retardation and 46,X,t(X;8)(p22.13;q22.1) is described. Although the clinical features and translocation breakpoints raise the possibility of a number of specific conditions, the constellation of problems is not consistent with any previously reported genetic syndrome. It is argued that her clinical disorder is likely due to the chromosomal abnormality and that further detailed molecular genetic investigation may shed light on the genetic basis to various components of her phenotype including the autism.

Published

1995

6. Fluorescencein situhybridisation of multiple probes on a single microscope slide

Author

Eddy Maher, Zoia Larin, Edwin M. Southern, Yumiko Ishikawa-Brush, and Mark D. Fricker

Subjects

Chromosome paints, Microscope, business.industry, Hybridization probe, Microscope slide, Biology, Molecular biology, Fluorescence, Chromosomes, law.invention, Optics, law, Karyotyping, In situ hybridisation, Bone plate, Genetics, Silicon rubber, Humans, DNA Probes, business, In Situ Hybridization, Fluorescence

Abstract

We report a method to analyse multiple samples by fluorescence in situ hybridisation on a single glass microscope slide. Wells were formed in which independent hybridisation reactions could proceed by sealing a silicon rubber gasket to the slide. In the largest format tested, different probes were hybridised simultaneously by applying them directly from a 96-well microtitre dish which was inverted on a glass plate. This technique will increase the rate of analysis of multiple probes against a standard set of chromosomes and could also be used to analyse different karyotypes using a panel of probes such as single chromosome paints during a single operation. It should be useful for both chromosomal mapping projects and screening for chromosome abnormalities in clinical diagnostic laboratories.

Published

1994

7. Independent genome-wide scans identify a chromosome 18 quantitative-trait locus influencing dyslexia

Author

Yumiko Ishikawa-Brush, Alex J. Richardson, Richard K. Olson, John F. Stein, John C. DeFries, Bruce F. Pennington, Clyde Francks, Shelley D. Smith, I. Laurence MacPhie, Anthony P. Monaco, Javier Gayán, Lon R. Cardon, Joel B. Talcott, Dianne F. Newbury, Simon E. Fisher, and Angela J. Marlow

Subjects

Genetic Markers, Male, Genotype, Genetic Linkage, Locus (genetics), Biology, Quantitative trait locus, Dyslexia, Genetic Heterogeneity, Quantitative Trait, Heritable, DCDC2, Genetic linkage, Genetics, medicine, Diseases in Twins, Humans, Child, Psychological Tests, Genetic heterogeneity, Chromosome Mapping, medicine.disease, Twin study, United Kingdom, United States, Trait, Chromosomes, Human, Pair 6, Female, Lod Score, Chromosomes, Human, Pair 18

Abstract

Developmental dyslexia is defined as a specific and significant impairment in reading ability that cannot be explained by deficits in intelligence, learning opportunity, motivation or sensory acuity. It is one of the most frequently diagnosed disorders in childhood, representing a major educational and social problem. It is well established that dyslexia is a significantly heritable trait with a neurobiological basis. The etiological mechanisms remain elusive, however, despite being the focus of intensive multidisciplinary research. All attempts to map quantitative-trait loci (QTLs) influencing dyslexia susceptibility have targeted specific chromosomal regions, so that inferences regarding genetic etiology have been made on the basis of very limited information. Here we present the first two complete QTL-based genome-wide scans for this trait, in large samples of families from the United Kingdom and United States. Using single-point analysis, linkage to marker D18S53 was independently identified as being one of the most significant results of the genome in each scan (P< or =0.0004 for single word-reading ability in each family sample). Multipoint analysis gave increased evidence of 18p11.2 linkage for single-word reading, yielding top empirical P values of 0.00001 (UK) and 0.0004 (US). Measures related to phonological and orthographic processing also showed linkage at this locus. We replicated linkage to 18p11.2 in a third independent sample of families (from the UK), in which the strongest evidence came from a phoneme-awareness measure (most significant P value=0.00004). A combined analysis of all UK families confirmed that this newly discovered 18p QTL is probably a general risk factor for dyslexia, influencing several reading-related processes. This is the first report of QTL-based genome-wide scanning for a human cognitive trait.

Published

2002

8. Autism and multiple exostoses associated with an X;8 translocation occurring within the GRPR gene and 3' to the SDC2 gene

Author

Patrick Bolton, John Powell, Huntington F. Willard, Hans Lehrach, Andrew P. Miller, Fiona Francis, Anthony P. Monaco, and Yumiko Ishikawa-Brush

Subjects

Adult, Yeast artificial chromosome, Candidate gene, X Chromosome, Hereditary multiple exostoses, Molecular Sequence Data, Restriction Mapping, Gene Expression, Translocation Breakpoint, Chromosomal translocation, Biology, Translocation, Genetic, Fusion gene, Genetics, medicine, Humans, Autistic Disorder, Cloning, Molecular, Chromosomes, Artificial, Yeast, Molecular Biology, Genetics (clinical), X chromosome, Membrane Glycoproteins, Base Sequence, DNA, Exons, General Medicine, Cosmids, medicine.disease, Receptors, Bombesin, Position effect, Female, Proteoglycans, Syndecan-2, Exostoses, Multiple Hereditary, Chromosomes, Human, Pair 8

Abstract

An X;8 translocation was identified in a 27-year-old female patient manifesting multiple exostoses and autism accompanied by mental retardation and epilepsy. Through molecular analysis using yeast artificial chromosomes (YACs) and cosmid clones, the translocation breakpoint was isolated and confirmed to be reciprocal within a 5'-GGCA-3' sequence found on both X and 8 chromosomes without gain or loss of a single nucleotide. The translocation breakpoint on the X chromosome occurred in the first intron of the gastrin-releasing peptide receptor (GRPR) gene and that on chromosome 8 occurred approximately 30 kb distal to the 3' end of the Syndecan-2 gene (SDC2), also known as human heparan sulfate proteoglycan or fibroglycan. The GRPR gene was shown to escape X-inactivation. A dosage effect of the GRPR and a position effect of the SDC2 gene may, however, contribute the phenotype observed in this patient since the orientation of these genes with respect to the translocation was incompatible with the formation of a fusion gene. Investigation of mutations in these two genes in unrelated patients with either autism or multiple exostoses as well as linkage and association studies is needed to validate them as candidate genes.

Published

1997

9. X-linked mixed deafness (DFN3): cloning and characterization of the critical region allows the identification of novel microdeletions

Author

Silvère M. van der Maarel, David O. Robinson, S. Malcolm, Hans-Hilger Ropers, Frans P.M. Cremers, I. Huber, Yumiko Ishikawa-Brush, Maria Bitner-Gllndzicz, Han G. Brunner, Marcus Pembrey, Anthony P. Monaco, and Yvette J. M. de Kok

Subjects

Male, Yeast artificial chromosome, Genetics, X Chromosome, Contig, Hearing Loss, Sensorineural, DNA Mutational Analysis, General Medicine, Biology, Chromosome Walking, Gene mapping, Genetic marker, Chromosomal region, Cosmid, otorhinolaryngologic diseases, Humans, Female, Cloning, Molecular, Chromosomes, Artificial, Yeast, Molecular Biology, Genetics (clinical), X chromosome, Sequence Deletion, Southern blot

Abstract

We have found that the microsatellite marker AFM207zg5 (DXS995) maps to all previously described deletions which are associated with X-linked mixed deafness (DFN3) with or without choroideremia and mental retardation. Employing this marker and pHU16 (DXS26) we have identified two partially overlapping yeast artificial chromosome clones which were used to construct a complete 850 kb cosmid contig. Cosmids from this contig have been tested by Southern blot analysis on DNA from 16 unrelated males with X-linked deafness. Two novel microdeletions were detected in patients which exhibit the characteristic DFN3 phenotype. Both deletions are completely contained within one of the known DFN3-deletions, but one of them does not overlap with two previously described deletions in patients with contiguous gene syndromes consisting of DFN3, choroideremia, and mental retardation. Assuming that only a single gene is involved, this suggests that the DFN3 gene spans a chromosomal region of at least 400 kb.

Published

1994

10. Identification of YAC and cosmid clones encompassing the ZFX-POLA region using irradiation hybrid cell lines

Author

Chee Gee See, Fiona Francis, Yumiko Ishikawa-Brush, Renata M.J. Hamvas, Birgit Weiss, Gudrun A. Rappold, Margaret Fox, Anthony P. Monaco, Hans Lehrach, and Frances Benham

Subjects

Genetic Markers, congenital, hereditary, and neonatal diseases and abnormalities, X Chromosome, Genetic Linkage, chemical and pharmacologic phenomena, Hybrid Cells, Biology, Molecular cloning, Mice, Restriction map, Species Specificity, Gene mapping, hemic and lymphatic diseases, Genetics, medicine, Animals, Humans, Cloning, Molecular, Chromosomes, Artificial, Yeast, In Situ Hybridization, Fluorescence, X chromosome, Gene Library, Contig, medicine.diagnostic_test, DNA–DNA hybridization, fungi, Chromosome Mapping, hemic and immune systems, DNA Polymerase II, Cosmids, Electrophoresis, Gel, Pulsed-Field, Cosmid, bacteria, Fluorescence in situ hybridization

Abstract

The human Xp21.3-p22.1 region is poorly mapped relative to other X chromosome regions. To target cosmid and YAC clones specifically from Xp21.3-p22.1 for rapid contig construction, a hybridization-based screening approach using irradiation hybrids has been used. Alu-PCR products generated from hybrid lines containing small overlapping fragments from Xp21-p22 were hybridized to an X chromosome cosmid library, and cosmids predicted by their hybridization pattern to map to the region of interest were analyzed by fluorescence in situ hybridization (FISH). Hybridization of the cosmids in pools to gridded YAC libraries identified 15 YACs, which were verified and tested for chimerism by FISH. Cosmid content analysis of the YACs defined two contigs, one with 12 YACs covering about 1.5 Mb and one with 3 YACs. Five YACs from the 12-YAC cluster had been previously recognized by DNA polymerase alpha (POLA). ZFX identified a single YAC; hence, the physical linkage of ZFX and POLA was demonstrated within the contig. Four YACs had been isolated previously with ZRX and these extend the contig to 2 Mb. Restriction mapping of several YACs demonstrates that ZFX and POLA are about 700 kb apart, a distance similar to that reported in the mouse between Zfx and Pola. Themore » order of these two loci and two additional loci identified by homologous mouse linking clones was found to be conserved between human and mouse; tel-ZFX-DXCre57-DXCre140-POLA-cen. The authors have shown that YAC contigs can be rapidly constructed from targeted regions without the need for time-consuming YAC end rescue and chromosomal walking. This approach also generates a series of ordered cosmids, which is particularly valuable for marker generation in regions in which disease gene localization is hampered by low marker density. 32 refs., 4 figs., 2 tabs.« less

Published

1994

11. Physical mapping of Xq24-25 around loci closely linked to the X-linked lymphoproliferative syndrome locus: an overlapping YAC map and linkage between DXS12, DXS42, and DXS37

Author

Bakary S. Sylla, Q Wang, C T Caskey, S P Pauly, Anthony P. Monaco, Gilbert M. Lenoir, David L. Nelson, and Yumiko Ishikawa-Brush

Subjects

Genetics, Genetic Markers, X Chromosome, Genetic Linkage, Restriction Mapping, Locus (genetics), Genes, Recessive, Biology, Lymphoproliferative Disorders, Electrophoresis, Gel, Pulsed-Field, Chromosome Walking, Restriction map, Genetic marker, Genetic linkage, Primer walking, Humans, X-Linked Lymphoproliferative Syndrome, DNA Probes, Gene, Chromosomes, Artificial, Yeast, Genetics (clinical), X chromosome

Abstract

We have localized several markers in the Xq24-25 region containing DXS12, DXS42 and DXS37 which are closely linked to the X-linked lymphoproliferative syndrome (XLP) locus. A 850-kb restriction map has been established by mapping overlapping YACs and showed that DXS12 and DXS42 are physically linked within about 50 kb. DXS37 is separated from these two loci at a maximum distance of 3,700 kb. Several new probes have been generated which will contribute to further physical mapping of this region.

Published

1993

12. Isolation of a candidate gene for Menkes disease that encodes a potential heavy metal binding protein

Author

T. Tønnesen, Anne Petterson, Jamel Chelly, Zeynep Tümer, Niels Tommerup, Yumiko Ishikawa-Brush, Anthony P. Monaco, and Nina Horn

Subjects

Male, Candidate gene, X Chromosome, Recombinant Fusion Proteins, Molecular Sequence Data, ATP7A, Occipital horn syndrome, Biology, Genetics, medicine, Humans, Amino Acid Sequence, Menkes Kinky Hair Syndrome, Cloning, Molecular, Cation Transport Proteins, Cells, Cultured, Adenosine Triphosphatases, Base Sequence, Sequence Homology, Amino Acid, DNA, medicine.disease, Wilson disease protein, Blotting, Southern, ATP7A Gene, Copper-Transporting ATPases, Metals, biology.protein, Female, Menkes disease, Carrier Proteins, Menkes' syndrome

Abstract

Menkes disease is a lethal-X linked recessive disorder associated with copper metabolism disturbance. We have recently mapped two chromosome breakpoints related to this disease in a 1 megabase yeast artificial chromosome contig at Xq13.3. We now report the construction of a phage contig and the isolation of candidate partial cDNAs for the Menkes disease gene. The candidate gene expresses an 8 kb message in all investigated tissues, and deletions were detected in 16% of 100 unrelated Menkes patients. The deduced partial protein sequence shared the GMTCXXC motif with bacterial metal resistance operons, suggesting a potential heavy metal binding protein. These findings should lead to more accurate prenatal diagnosis of this severe disease and a better understanding of the cellular homeostasis of essential heavy metals.

Published

1993

13. Characterization of a 1.0 Mb YAC contig spanning two chromosome breakpoints related to Menkes disease

Author

Niels Tommerup, Jamel Chelly, T. Tønnesen, Nina Horn, Anthony P. Monaco, Zeynep Tümer, and Yumiko Ishikawa-Brush

Subjects

Yeast artificial chromosome, Male, congenital, hereditary, and neonatal diseases and abnormalities, X Chromosome, Chromosome Breakpoints, Biology, Polymerase Chain Reaction, Restriction map, Gene mapping, Genetics, medicine, Humans, Menkes Kinky Hair Syndrome, Molecular Biology, Genetics (clinical), In Situ Hybridization, Chromosome Aberrations, Genomic Library, Contig, Genome, Human, General Medicine, medicine.disease, Molecular biology, Electrophoresis, Gel, Pulsed-Field, Cosmid, Menkes disease, Female, Chromosomes, Fungal, Menkes' syndrome

Abstract

Menkes disease, an X-linked recessive disorder of copper metabolism, has recently been mapped to Xq13.3 by two Menkes patients carrying chromosome rearrangements within this region. The breakpoints have been investigated by nonisotopic in situ suppression hybridization using YACs isolated from this region with the flanking markers DXS56 and PGK1. Three YACs were extending over the breakpoints at Xq13.3 and were shown to be overlapping by partial digest restriction maps, IRS-PCR fingerprinting and by the presence of common cosmid clones. These cosmids were subcloned and one of the single copy probes detected both breakpoints using rare-cutting restriction enzyme digests of the patients. All the results together localize the breakpoints to about 100 kb within the overlapping region of the YACs. Mapping of both breakpoints in a 1 Mb YAC contig implies that these YACs contain at least partially, the gene responsible for Menkes disease.

Published

1992

14. A YAC contig in Xp21 containing the adrenal hypoplasia congenita and glycerol kinase deficiency genes

Author

Yumiko Ishikawa Brush, Beat Steinman, Donald R. Love, D. Recan, Maurice Super, Jamel Chelly, John R.W. Yates, Anthony P. Monaco, Armand Bottani, J.Michael Connor, Jean-Louis Chaussain, Christine A. Oley, Ann P. Walker, Kay E. Davies, Jean-Claude Kaplan, David A. Price, University of Zurich, and Walker, Ann P

Subjects

Yeast artificial chromosome, clone (Java method), Male, congenital, hereditary, and neonatal diseases and abnormalities, 2716 Genetics (clinical), X Chromosome, Adrenal Gland Diseases, 610 Medicine & health, Polymerase Chain Reaction, 142-005 142-005, 1311 Genetics, X-linked adrenal hypoplasia congenita, Glycerol Kinase, Genetics, medicine, 1312 Molecular Biology, Humans, Deletion mapping, Molecular Biology, Genetics (clinical), Repetitive Sequences, Nucleic Acid, Genomic Library, biology, Contig, Genome, Human, Chromosome Mapping, Glycerol kinase deficiency, General Medicine, medicine.disease, Cosmids, Molecular biology, Cosmid, biology.protein, 570 Life sciences, DAX1, Chromosome Deletion, Chromosomes, Fungal, Deficiency Diseases

Abstract

The gene loci for adrenal hypoplasia congenita (AHC) and glycerol kinase deficiency (GK) map in Xp21 distal to Duchenne muscular dystrophy (DMD), and proximal to DXS28 (C7), by analysis of patient deletions. We have constructed a yeast artificial chromosome (YAC) contig encompassing a 1.2 Mb region extending distally from DMD, and containing DXS708 (JC-1), the distal junction clone of a patient with GK and DMD. A pulsed-field gel electrophoresis map of the YAC contig identified 3 potential CpG islands. Whole YAC hybridization identified cosmids both for construction of cosmid contigs, and isolation of single copy probes. Thirteen new single copy probes and DXS28 and DXS708 were hybridized on a panel of patients; the deletion mapping indicates that the YAC contig contains both GK and at least part of AHC, and together with the physical map defines a GK critical region of 50-250 kb. In one AHC patient with a cytogenetically detectable deletion we used the new probes to characterize a complex double deletion. Non-overlapping deletions observed in other unrelated AHC patients indicate that the AHC gene is large, extending over at least 200-500 kb. This mapping provides the basis for the identification of the AHC and GK genes.

Published

1992