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Query: UMLS:C0004135 (
ATM
)
13,001
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Ataxia telangiectasia
(AT) is an autosomal recessive disease of unknown etiology associated with cerebellar ataxia, oculocutaneous telangiectasia, immunodeficiency, and hypersensitivity to ionizing radiation. Although AT has been divided into four complementation groups by its radioresistant-DNA synthesis phenotype, the
ATM
gene has been isolated as the candidate gene responsible for all AT groups. We identified a new gene, designated NPAT, from the major AT locus on human chromosome 11q22-q23. The gene encoded a 1421-amino-acid protein containing nuclear localization signals and phosphorylation target sites by cyclin-dependent protein kinases associated with E2F. The messenger RNA of NPAT was detected in all human tissues examined, and its genomic sequence was strongly conserved through eukaryotes, suggesting that the NPAT gene may be essential for cell maintenance and may be a member of the
housekeeping
genes. Analysis of the genomic region of NPAT surprisingly revealed that the gene existed only 0.5 kb apart from the 5' end of the
ATM
transcript with opposite transcriptional direction. It may be possible to propose the idea that the promoter region could be shared by both
housekeeping
genes and that each gene could influence the expression of the other.
...
PMID:Identification and characterization of a new gene physically linked to the ATM gene. 874 93
In an earlier report we showed that the 5' end of the gene for
ataxia telangiectasia
ATM
is within 700 bp of the 5' end of a novel gene E14, and suggested that the CpG island that separates these genes functions as a bidirectional promoter. We have now determined the complete amino acid sequence of the E14 protein, defined the exon/intron structure of the gene and estimate that the complete gene is more than 55 kb in length. The E14 gene appears to be a
housekeeping
gene that is expressed in all tissues, including all parts of the brain. The E14/
ATM
promoter organisation is conserved in man, monkey and mouse, although the mouse promoter is more compact and appears to lack two of the four putative Sp1 boxes found in the human promoter. Reporter gene constructs showed that the human and mouse E14/
ATM
promoters were indeed bidirectional, that the
ATM
side of the human promoter was three times stronger than the E14 side, and that the mouse promoter (in human cells) directed transcription with equal efficiency in both directions, but at a lower level than the human promoter. Analysis of a small number of A-T patients for mutations in the promoter region or the E14 coding sequence did not provide evidence to suggest that E14 contributes to the A-T phenotype.
...
PMID:A gene transcribed from the bidirectional ATM promoter coding for a serine rich protein: amino acid sequence, structure and expression studies. 892 7
Using a magnetic beads-mediated cDNA selection procedure and a fetal brain expression library, we identified a transcriptional unit within a cosmid positive for the marker D11S384. Pursuit of its full-length cDNA led to the cloning of the third candidate gene (CAND3) we studied in our quest for the
ataxia-telangiectasia
(
A-T
) gene,
ATM
. CAND3 spans approximately 140 kb of genomic DNA and is located immediately centrimeric to
ATM
, with 544 bp of DNA separating the two genes. CAND3 encodes two ubiquitously expressed transcripts of approximately 5.8 kb and approximately 4.6 kb that are divergently transcribed from a promoter region common to
ATM
. Nucleotide sequence was determined for one of its alternately spliced transcripts. The predicted protein has 1175 amino acids and is novel in sequence, with only weak homologies to transcriptional factors, nucleoporin protein, and protein kinases, including members of the phosphatidylinositol 3-kinase (PI-3 kinase) family. Although neither homology to
ATM
nor any mutation of CAND3 in
A-T
patients has been found, the head-to-head arrangement of CAND3 and
ATM
, with expression of both
housekeeping
genes from a common stretch of 544 bp intergenic DNA, suggests a bi-directional promoter possibly for co-regulation of biologically related functions. YACs, BACs, cosmids, and STSs are defined to aid in further study of this gene.
...
PMID:CAND3: a ubiquitously expressed gene immediately adjacent and in opposite transcriptional orientation to the ATM gene at 11q23.1. 906 Apr 12
Ataxia telangiectasia
(AT) is an autosomal recessive gene disorder, and
ATM
, a
housekeeping
gene, has been identified as the gene responsible for AT. Recently we found that another
housekeeping
gene, NPAT, is located upstream of
ATM
on human chromosome 11. The two
housekeeping
genes are transcribed in opposite directions and share a 0.5-kb 5' flanking sequence. The structure and organization of NPAT were determined by direct sequencing of cosmid clones carrying the gene and by application of the long and accurate (LA)-PCR method to amplify regions encompassing the exon/intron boundaries and all of the exons. The gene spans at least 44 kb and consists of 18 exons and 17 introns. It has been suggested that AT heterozygotes have an increased risk of developing cancer, especially breast cancer in women. Frequently, loss of heterozygosity at loci on 11q22-q24 has been observed in DNA isolated from tumors of the breast, uterine cervix, and colon, perhaps suggesting the location of a tumor suppressor gene in 11q22-q24. For investigation of the role of NPAT in AT and these tumors with allelic loss of 11q22-q24, appropriate primer sequences and PCR conditions for amplification of all the NPAT exons from genomic DNA were determined. We previously reported that no recombinations are found among Atm, Npat, and Acat1 (acetoacetyl-CoA thiolase) loci as determined by fine genetic linkage mapping of the mouse AT region. The results of the LA-PCR analysis using NPAT- and ACAT-specific primers and human genomic DNA allowed us to map ACAT 12 kb centromeric to NPAT.
...
PMID:The structure and organization of the human NPAT gene. 920 9
The gene mutated in
ataxia telangiectasia
(
A-T
) patients (
ATM
) is located on chromosome 11q22-23, a region frequently altered in mammary tumors. Patients homozygous for
ATM
mutations are prone to develop a variety of different neoplasms. Female heterozygotes have been reported to carry a 5- to 8-fold increased risk of breast cancer. However, germline mutations in the
ATM
gene are rare in women with sporadic breast carcinomas. Most of the alterations described in
A-T
patients result in a functionally inactive ATM protein. Moreover, it has been suggested that mutations of the
ATM
gene in
A-T
patients influence the amount of
ATM
mRNA and that this may affect the severity of the disease. In the present study, we have analyzed
ATM
transcripts in a series of 39 breast carcinomas, 14 benign breast lesions and 12 normal breast tissue samples.
ATM
mRNA levels were determined by semiquantitative competitive RT-PCR. Competitor RNA molecules for the
ATM
gene and the
housekeeping
gene beta-2-microglobulin (B2M) were generated by PCR mutagenesis. Low concentrations of
ATM
transcripts were detected in breast carcinomas, intermediate levels in benign lesions and highest levels in normal breast tissue specimens (F-test, p = 0.0013). Our results indicate that reduced expression of the
ATM
gene may contribute to the development and/or malignant progression of breast carcinomas.
...
PMID:Expression of the ATM gene is significantly reduced in sporadic breast carcinomas. 976 63
Using a magnetic beads-mediated cDNA selection procedure and a fetal brain expression library, we identified a transcriptional unit within a cosmid positive for the marker D11S384. Pursuit of its full-length cDNA led to the cloning of the third candidate gene (CAND3) we studied in our quest for the ataxiatelangiectasia (A-T) gene,
ATM
. CAND3 spans ~140 kb of genomic DNA and is located immediately centrimeric to
ATM
, with 544 bp of DNA separating the two genes. CAND3 encodes two ubiquitously expressed transcripts of ~5.8 kb and ~4.6 kb that are divergently transcribed from a promoter region common to
ATM
. Nucleotide sequence was determined for one of its alternately spliced transcripts. The predicted protein has 1175 amino acids and is novel in sequence, with only weak homologies to transcriptional factors, nucleoporin protein, and protein kinases, including members of the phosphatidylinositol 3-kinase (PI-3 kinase) family. Although neither homology to
ATM
nor any mutation of CAND3 in A-T patients has been found, the head-to-head arrangement of CAND3 and
ATM
, with expression of both
housekeeping
genes from a common stretch of 544 bp intergenic DNA, suggests a bi-directional promoter possibly for co-regulation of biologically related functions. YACs, BACs, cosmids, and STSs are defined to aid in the further study of this gene.
...
PMID:CAND3: A ubiquitously expressed gene immediately adjacent and in opposite transcriptional orientation to the ATM gene at 1lq23.1. 2751 7
