1997
DOI: 10.1006/geno.1997.4621
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Mapping of the Gene for the Mouse Telomerase RNA Component,Terc,to Chromosome 3 by Fluorescencein SituHybridization and Mouse Chromosome Painting

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Cited by 18 publications
(7 citation statements)
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“…The 3q26‐29 amplicon is spread over four major cytogenetic bands with 10 subdivisions, and contains 188 protein‐encoding genes with associated TCGA genomic data: 62% of these genes also have increased gene expression ( z ‐score > 2 in > 10% patients, E. J. Shanks, M. A. Davidson & M. Neilson, unpublished results) . Figure provides current genomic alteration data (copy number amplification, mRNA upregulation and mutation status) for genes known to arbitrate key oncogenic driver events in HNSCC, including PIK3CA (which encodes the p110 catalytic subunit of PI3K) and TERC, the telomerase RNA component gene , as well as novel genes revealed in our analysis. However, it is unlikely that all of the genes within the amplicon will be relevant to disease, thus necessitating the implementation of other characteristics such as survival and mutation status.…”
Section: Identification Of Pro‐oncogenic Factors In 3q26‐29mentioning
confidence: 99%
“…The 3q26‐29 amplicon is spread over four major cytogenetic bands with 10 subdivisions, and contains 188 protein‐encoding genes with associated TCGA genomic data: 62% of these genes also have increased gene expression ( z ‐score > 2 in > 10% patients, E. J. Shanks, M. A. Davidson & M. Neilson, unpublished results) . Figure provides current genomic alteration data (copy number amplification, mRNA upregulation and mutation status) for genes known to arbitrate key oncogenic driver events in HNSCC, including PIK3CA (which encodes the p110 catalytic subunit of PI3K) and TERC, the telomerase RNA component gene , as well as novel genes revealed in our analysis. However, it is unlikely that all of the genes within the amplicon will be relevant to disease, thus necessitating the implementation of other characteristics such as survival and mutation status.…”
Section: Identification Of Pro‐oncogenic Factors In 3q26‐29mentioning
confidence: 99%
“…34,35 Several studies based on this approach and using CGH data have also been documented. 31,36,37 Clustering of aberrations between SK and SCC demonstrates a dispersion of SK samples among the SCC population. If SK were a dysplasia distinct from SCC, most samples would cluster into a separate subset.…”
Section: Commentmentioning
confidence: 99%
“…The gain of 3q may be linked to the human telomerase RNA gene, which maps to this arm. 37 Aberrant telomerase activity has been linked to cellular immortality and tumor progression in a wide array of tumor types, including nonmelanoma skin cancer, and in many of these types overexpression of the 3q arm can be observed. [38][39][40] Interestingly, the loss of 3p and gain of 3q was a significant occurrence in SCC.…”
Section: Commentmentioning
confidence: 99%
“…The gene encoding hTR was cloned in 1995 [120]. It is a single copy gene localized to chromosome 3 at 3q26.3 by fluorescence in situ hybridization [121]. The half-life of this RNA, transcribed in mammals by RNA polymerase II, varies from 4 to 32 days [122], and thus is the longest ever reported for an eukaryotic RNA.…”
Section: Htr (Human Telomerase Rna)mentioning
confidence: 99%