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The dark matter of the cancer genome: aberrations in regulatory elements, untranslated regions, splice sites, non‐coding RNA and synonymous mutations

Cancer is a disease of the genome caused by oncogene activation and tumor suppressor gene inhibition. Deep sequencing studies including large consortia such as TCGA and ICGC identified numerous tumor‐specific mutations not only in protein‐coding sequences but also in non‐coding sequences. Although 9...

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Autores principales: Diederichs, Sven, Bartsch, Lorenz, Berkmann, Julia C, Fröse, Karin, Heitmann, Jana, Hoppe, Caroline, Iggena, Deetje, Jazmati, Danny, Karschnia, Philipp, Linsenmeier, Miriam, Maulhardt, Thomas, Möhrmann, Lino, Morstein, Johannes, Paffenholz, Stella V, Röpenack, Paula, Rückert, Timo, Sandig, Ludger, Schell, Maximilian, Steinmann, Anna, Voss, Gjendine, Wasmuth, Jacqueline, Weinberger, Maria E, Wullenkord, Ramona
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5126213/
https://www.ncbi.nlm.nih.gov/pubmed/26992833
http://dx.doi.org/10.15252/emmm.201506055
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author Diederichs, Sven
Bartsch, Lorenz
Berkmann, Julia C
Fröse, Karin
Heitmann, Jana
Hoppe, Caroline
Iggena, Deetje
Jazmati, Danny
Karschnia, Philipp
Linsenmeier, Miriam
Maulhardt, Thomas
Möhrmann, Lino
Morstein, Johannes
Paffenholz, Stella V
Röpenack, Paula
Rückert, Timo
Sandig, Ludger
Schell, Maximilian
Steinmann, Anna
Voss, Gjendine
Wasmuth, Jacqueline
Weinberger, Maria E
Wullenkord, Ramona
author_facet Diederichs, Sven
Bartsch, Lorenz
Berkmann, Julia C
Fröse, Karin
Heitmann, Jana
Hoppe, Caroline
Iggena, Deetje
Jazmati, Danny
Karschnia, Philipp
Linsenmeier, Miriam
Maulhardt, Thomas
Möhrmann, Lino
Morstein, Johannes
Paffenholz, Stella V
Röpenack, Paula
Rückert, Timo
Sandig, Ludger
Schell, Maximilian
Steinmann, Anna
Voss, Gjendine
Wasmuth, Jacqueline
Weinberger, Maria E
Wullenkord, Ramona
author_sort Diederichs, Sven
collection PubMed
description Cancer is a disease of the genome caused by oncogene activation and tumor suppressor gene inhibition. Deep sequencing studies including large consortia such as TCGA and ICGC identified numerous tumor‐specific mutations not only in protein‐coding sequences but also in non‐coding sequences. Although 98% of the genome is not translated into proteins, most studies have neglected the information hidden in this “dark matter” of the genome. Malignancy‐driving mutations can occur in all genetic elements outside the coding region, namely in enhancer, silencer, insulator, and promoter as well as in 5′‐UTR and 3′‐UTR. Intron or splice site mutations can alter the splicing pattern. Moreover, cancer genomes contain mutations within non‐coding RNA, such as microRNA, lncRNA, and lincRNA. A synonymous mutation changes the coding region in the DNA and RNA but not the protein sequence. Importantly, oncogenes such as TERT or miR‐21 as well as tumor suppressor genes such as TP53/p53,APC,BRCA1, or RB1 can be affected by these alterations. In summary, coding‐independent mutations can affect gene regulation from transcription, splicing, mRNA stability to translation, and hence, this largely neglected area needs functional studies to elucidate the mechanisms underlying tumorigenesis. This review will focus on the important role and novel mechanisms of these non‐coding or allegedly silent mutations in tumorigenesis.
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spelling pubmed-51262132016-12-09 The dark matter of the cancer genome: aberrations in regulatory elements, untranslated regions, splice sites, non‐coding RNA and synonymous mutations Diederichs, Sven Bartsch, Lorenz Berkmann, Julia C Fröse, Karin Heitmann, Jana Hoppe, Caroline Iggena, Deetje Jazmati, Danny Karschnia, Philipp Linsenmeier, Miriam Maulhardt, Thomas Möhrmann, Lino Morstein, Johannes Paffenholz, Stella V Röpenack, Paula Rückert, Timo Sandig, Ludger Schell, Maximilian Steinmann, Anna Voss, Gjendine Wasmuth, Jacqueline Weinberger, Maria E Wullenkord, Ramona EMBO Mol Med Reviews Cancer is a disease of the genome caused by oncogene activation and tumor suppressor gene inhibition. Deep sequencing studies including large consortia such as TCGA and ICGC identified numerous tumor‐specific mutations not only in protein‐coding sequences but also in non‐coding sequences. Although 98% of the genome is not translated into proteins, most studies have neglected the information hidden in this “dark matter” of the genome. Malignancy‐driving mutations can occur in all genetic elements outside the coding region, namely in enhancer, silencer, insulator, and promoter as well as in 5′‐UTR and 3′‐UTR. Intron or splice site mutations can alter the splicing pattern. Moreover, cancer genomes contain mutations within non‐coding RNA, such as microRNA, lncRNA, and lincRNA. A synonymous mutation changes the coding region in the DNA and RNA but not the protein sequence. Importantly, oncogenes such as TERT or miR‐21 as well as tumor suppressor genes such as TP53/p53,APC,BRCA1, or RB1 can be affected by these alterations. In summary, coding‐independent mutations can affect gene regulation from transcription, splicing, mRNA stability to translation, and hence, this largely neglected area needs functional studies to elucidate the mechanisms underlying tumorigenesis. This review will focus on the important role and novel mechanisms of these non‐coding or allegedly silent mutations in tumorigenesis. John Wiley and Sons Inc. 2016-03-18 2016-05 /pmc/articles/PMC5126213/ /pubmed/26992833 http://dx.doi.org/10.15252/emmm.201506055 Text en © 2016 The Authors. Published under the terms of the CC BY 4.0 license This is an open access article under the terms of the Creative Commons Attribution 4.0 (http://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Reviews
Diederichs, Sven
Bartsch, Lorenz
Berkmann, Julia C
Fröse, Karin
Heitmann, Jana
Hoppe, Caroline
Iggena, Deetje
Jazmati, Danny
Karschnia, Philipp
Linsenmeier, Miriam
Maulhardt, Thomas
Möhrmann, Lino
Morstein, Johannes
Paffenholz, Stella V
Röpenack, Paula
Rückert, Timo
Sandig, Ludger
Schell, Maximilian
Steinmann, Anna
Voss, Gjendine
Wasmuth, Jacqueline
Weinberger, Maria E
Wullenkord, Ramona
The dark matter of the cancer genome: aberrations in regulatory elements, untranslated regions, splice sites, non‐coding RNA and synonymous mutations
title The dark matter of the cancer genome: aberrations in regulatory elements, untranslated regions, splice sites, non‐coding RNA and synonymous mutations
title_full The dark matter of the cancer genome: aberrations in regulatory elements, untranslated regions, splice sites, non‐coding RNA and synonymous mutations
title_fullStr The dark matter of the cancer genome: aberrations in regulatory elements, untranslated regions, splice sites, non‐coding RNA and synonymous mutations
title_full_unstemmed The dark matter of the cancer genome: aberrations in regulatory elements, untranslated regions, splice sites, non‐coding RNA and synonymous mutations
title_short The dark matter of the cancer genome: aberrations in regulatory elements, untranslated regions, splice sites, non‐coding RNA and synonymous mutations
title_sort dark matter of the cancer genome: aberrations in regulatory elements, untranslated regions, splice sites, non‐coding rna and synonymous mutations
topic Reviews
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5126213/
https://www.ncbi.nlm.nih.gov/pubmed/26992833
http://dx.doi.org/10.15252/emmm.201506055
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