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Complex Patterns of Chromosome 11 Aberrations in Myeloid Malignancies Target CBL, MLL, DDB1 and LMO2

Exome sequencing of primary tumors identifies complex somatic mutation patterns. Assignment of relevance of individual somatic mutations is difficult and poses the next challenge for interpretation of next generation sequencing data. Here we present an approach how exome sequencing in combination wi...

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Autores principales: Klampfl, Thorsten, Milosevic, Jelena D., Puda, Ana, Schönegger, Andreas, Bagienski, Klaudia, Berg, Tiina, Harutyunyan, Ashot S., Gisslinger, Bettina, Rumi, Elisa, Malcovati, Luca, Pietra, Daniela, Elena, Chiara, Della Porta, Matteo Giovanni, Pieri, Lisa, Guglielmelli, Paola, Bock, Christoph, Doubek, Michael, Dvorakova, Dana, Suvajdzic, Nada, Tomin, Dragica, Tosic, Natasa, Racil, Zdenek, Steurer, Michael, Pavlovic, Sonja, Vannucchi, Alessandro M., Cazzola, Mario, Gisslinger, Heinz, Kralovics, Robert
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3797696/
https://www.ncbi.nlm.nih.gov/pubmed/24147083
http://dx.doi.org/10.1371/journal.pone.0077819
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author Klampfl, Thorsten
Milosevic, Jelena D.
Puda, Ana
Schönegger, Andreas
Bagienski, Klaudia
Berg, Tiina
Harutyunyan, Ashot S.
Gisslinger, Bettina
Rumi, Elisa
Malcovati, Luca
Pietra, Daniela
Elena, Chiara
Della Porta, Matteo Giovanni
Pieri, Lisa
Guglielmelli, Paola
Bock, Christoph
Doubek, Michael
Dvorakova, Dana
Suvajdzic, Nada
Tomin, Dragica
Tosic, Natasa
Racil, Zdenek
Steurer, Michael
Pavlovic, Sonja
Vannucchi, Alessandro M.
Cazzola, Mario
Gisslinger, Heinz
Kralovics, Robert
author_facet Klampfl, Thorsten
Milosevic, Jelena D.
Puda, Ana
Schönegger, Andreas
Bagienski, Klaudia
Berg, Tiina
Harutyunyan, Ashot S.
Gisslinger, Bettina
Rumi, Elisa
Malcovati, Luca
Pietra, Daniela
Elena, Chiara
Della Porta, Matteo Giovanni
Pieri, Lisa
Guglielmelli, Paola
Bock, Christoph
Doubek, Michael
Dvorakova, Dana
Suvajdzic, Nada
Tomin, Dragica
Tosic, Natasa
Racil, Zdenek
Steurer, Michael
Pavlovic, Sonja
Vannucchi, Alessandro M.
Cazzola, Mario
Gisslinger, Heinz
Kralovics, Robert
author_sort Klampfl, Thorsten
collection PubMed
description Exome sequencing of primary tumors identifies complex somatic mutation patterns. Assignment of relevance of individual somatic mutations is difficult and poses the next challenge for interpretation of next generation sequencing data. Here we present an approach how exome sequencing in combination with SNP microarray data may identify targets of chromosomal aberrations in myeloid malignancies. The rationale of this approach is that hotspots of chromosomal aberrations might also harbor point mutations in the target genes of deletions, gains or uniparental disomies (UPDs). Chromosome 11 is a frequent target of lesions in myeloid malignancies. Therefore, we studied chromosome 11 in a total of 813 samples from 773 individual patients with different myeloid malignancies by SNP microarrays and complemented the data with exome sequencing in selected cases exhibiting chromosome 11 defects. We found gains, losses and UPDs of chromosome 11 in 52 of the 813 samples (6.4%). Chromosome 11q UPDs frequently associated with mutations of CBL. In one patient the 11qUPD amplified somatic mutations in both CBL and the DNA repair gene DDB1. A duplication within MLL exon 3 was detected in another patient with 11qUPD. We identified several common deleted regions (CDR) on chromosome 11. One of the CDRs associated with de novo acute myeloid leukemia (P=0.013). One patient with a deletion at the LMO2 locus harbored an additional point mutation on the other allele indicating that LMO2 might be a tumor suppressor frequently targeted by 11p deletions. Our chromosome-centered analysis indicates that chromosome 11 contains a number of tumor suppressor genes and that the role of this chromosome in myeloid malignancies is more complex than previously recognized.
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spelling pubmed-37976962013-10-21 Complex Patterns of Chromosome 11 Aberrations in Myeloid Malignancies Target CBL, MLL, DDB1 and LMO2 Klampfl, Thorsten Milosevic, Jelena D. Puda, Ana Schönegger, Andreas Bagienski, Klaudia Berg, Tiina Harutyunyan, Ashot S. Gisslinger, Bettina Rumi, Elisa Malcovati, Luca Pietra, Daniela Elena, Chiara Della Porta, Matteo Giovanni Pieri, Lisa Guglielmelli, Paola Bock, Christoph Doubek, Michael Dvorakova, Dana Suvajdzic, Nada Tomin, Dragica Tosic, Natasa Racil, Zdenek Steurer, Michael Pavlovic, Sonja Vannucchi, Alessandro M. Cazzola, Mario Gisslinger, Heinz Kralovics, Robert PLoS One Research Article Exome sequencing of primary tumors identifies complex somatic mutation patterns. Assignment of relevance of individual somatic mutations is difficult and poses the next challenge for interpretation of next generation sequencing data. Here we present an approach how exome sequencing in combination with SNP microarray data may identify targets of chromosomal aberrations in myeloid malignancies. The rationale of this approach is that hotspots of chromosomal aberrations might also harbor point mutations in the target genes of deletions, gains or uniparental disomies (UPDs). Chromosome 11 is a frequent target of lesions in myeloid malignancies. Therefore, we studied chromosome 11 in a total of 813 samples from 773 individual patients with different myeloid malignancies by SNP microarrays and complemented the data with exome sequencing in selected cases exhibiting chromosome 11 defects. We found gains, losses and UPDs of chromosome 11 in 52 of the 813 samples (6.4%). Chromosome 11q UPDs frequently associated with mutations of CBL. In one patient the 11qUPD amplified somatic mutations in both CBL and the DNA repair gene DDB1. A duplication within MLL exon 3 was detected in another patient with 11qUPD. We identified several common deleted regions (CDR) on chromosome 11. One of the CDRs associated with de novo acute myeloid leukemia (P=0.013). One patient with a deletion at the LMO2 locus harbored an additional point mutation on the other allele indicating that LMO2 might be a tumor suppressor frequently targeted by 11p deletions. Our chromosome-centered analysis indicates that chromosome 11 contains a number of tumor suppressor genes and that the role of this chromosome in myeloid malignancies is more complex than previously recognized. Public Library of Science 2013-10-16 /pmc/articles/PMC3797696/ /pubmed/24147083 http://dx.doi.org/10.1371/journal.pone.0077819 Text en © 2013 Klampfl et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Klampfl, Thorsten
Milosevic, Jelena D.
Puda, Ana
Schönegger, Andreas
Bagienski, Klaudia
Berg, Tiina
Harutyunyan, Ashot S.
Gisslinger, Bettina
Rumi, Elisa
Malcovati, Luca
Pietra, Daniela
Elena, Chiara
Della Porta, Matteo Giovanni
Pieri, Lisa
Guglielmelli, Paola
Bock, Christoph
Doubek, Michael
Dvorakova, Dana
Suvajdzic, Nada
Tomin, Dragica
Tosic, Natasa
Racil, Zdenek
Steurer, Michael
Pavlovic, Sonja
Vannucchi, Alessandro M.
Cazzola, Mario
Gisslinger, Heinz
Kralovics, Robert
Complex Patterns of Chromosome 11 Aberrations in Myeloid Malignancies Target CBL, MLL, DDB1 and LMO2
title Complex Patterns of Chromosome 11 Aberrations in Myeloid Malignancies Target CBL, MLL, DDB1 and LMO2
title_full Complex Patterns of Chromosome 11 Aberrations in Myeloid Malignancies Target CBL, MLL, DDB1 and LMO2
title_fullStr Complex Patterns of Chromosome 11 Aberrations in Myeloid Malignancies Target CBL, MLL, DDB1 and LMO2
title_full_unstemmed Complex Patterns of Chromosome 11 Aberrations in Myeloid Malignancies Target CBL, MLL, DDB1 and LMO2
title_short Complex Patterns of Chromosome 11 Aberrations in Myeloid Malignancies Target CBL, MLL, DDB1 and LMO2
title_sort complex patterns of chromosome 11 aberrations in myeloid malignancies target cbl, mll, ddb1 and lmo2
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3797696/
https://www.ncbi.nlm.nih.gov/pubmed/24147083
http://dx.doi.org/10.1371/journal.pone.0077819
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