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Alternative Spliced Transcripts as Cancer Markers

Eukaryotic mRNAs are transcribed as precursors containing their intronic sequences. These are subsequently excised and the exons are spliced together to form mature mRNAs. This process can lead to transcript diversification through the phenomenon of alternative splicing. Alternative splicing can tak...

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Detalles Bibliográficos
Autores principales: Caballero, Otavia L., de Souza, Sandro J., Brentani, Ricardo R., Simpson, Andrew J. G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: IOS Press 2001
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3851395/
https://www.ncbi.nlm.nih.gov/pubmed/11673653
http://dx.doi.org/10.1155/2001/184856
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author Caballero, Otavia L.
de Souza, Sandro J.
Brentani, Ricardo R.
Simpson, Andrew J. G.
author_facet Caballero, Otavia L.
de Souza, Sandro J.
Brentani, Ricardo R.
Simpson, Andrew J. G.
author_sort Caballero, Otavia L.
collection PubMed
description Eukaryotic mRNAs are transcribed as precursors containing their intronic sequences. These are subsequently excised and the exons are spliced together to form mature mRNAs. This process can lead to transcript diversification through the phenomenon of alternative splicing. Alternative splicing can take the form of one or more skipped exons, variable position of intron splicing or intron retention. The effect of alternative splicing in expanding protein repertoire might partially underlie the apparent discrepancy between gene number and the complexity of higher eukaryotes. It is likely that more than 50% form. Many cancer-associated genes, such as CD44 and WT1 are alternatively spliced. Variation of the splicing process occurs during tumor progression and may play a major role in tumorigenesis. Furthermore, alternatively spliced transcripts may be extremely useful as cancer markers, since it appears likely that there may be striking contrasts in usage of alternatively spliced transcript variants between normal and tumor tissue than in alterations in the general levels of gene expression.
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spelling pubmed-38513952013-12-22 Alternative Spliced Transcripts as Cancer Markers Caballero, Otavia L. de Souza, Sandro J. Brentani, Ricardo R. Simpson, Andrew J. G. Dis Markers Other Eukaryotic mRNAs are transcribed as precursors containing their intronic sequences. These are subsequently excised and the exons are spliced together to form mature mRNAs. This process can lead to transcript diversification through the phenomenon of alternative splicing. Alternative splicing can take the form of one or more skipped exons, variable position of intron splicing or intron retention. The effect of alternative splicing in expanding protein repertoire might partially underlie the apparent discrepancy between gene number and the complexity of higher eukaryotes. It is likely that more than 50% form. Many cancer-associated genes, such as CD44 and WT1 are alternatively spliced. Variation of the splicing process occurs during tumor progression and may play a major role in tumorigenesis. Furthermore, alternatively spliced transcripts may be extremely useful as cancer markers, since it appears likely that there may be striking contrasts in usage of alternatively spliced transcript variants between normal and tumor tissue than in alterations in the general levels of gene expression. IOS Press 2001 2002-06-07 /pmc/articles/PMC3851395/ /pubmed/11673653 http://dx.doi.org/10.1155/2001/184856 Text en Copyright © 2001 Hindawi Publishing Corporation.
spellingShingle Other
Caballero, Otavia L.
de Souza, Sandro J.
Brentani, Ricardo R.
Simpson, Andrew J. G.
Alternative Spliced Transcripts as Cancer Markers
title Alternative Spliced Transcripts as Cancer Markers
title_full Alternative Spliced Transcripts as Cancer Markers
title_fullStr Alternative Spliced Transcripts as Cancer Markers
title_full_unstemmed Alternative Spliced Transcripts as Cancer Markers
title_short Alternative Spliced Transcripts as Cancer Markers
title_sort alternative spliced transcripts as cancer markers
topic Other
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3851395/
https://www.ncbi.nlm.nih.gov/pubmed/11673653
http://dx.doi.org/10.1155/2001/184856
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