The University of Southampton
×
Filter your search:
University of Southampton Institutional Repository

Analysis of the chronic lymphocytic leukemia coding genome: role of NOTCH1 mutational activation

Analysis of the chronic lymphocytic leukemia coding genome: role of NOTCH1 mutational activation
Analysis of the chronic lymphocytic leukemia coding genome: role of NOTCH1 mutational activation
The pathogenesis of chronic lymphocytic leukemia (CLL), the most common leukemia in adults, is still largely unknown. The full spectrum of genetic lesions that are present in the CLL genome, and therefore the number and identity of dysregulated cellular pathways, have not been identified. By combining next-generation sequencing and copy number analysis, we show here that the typical CLL coding genome contains <20 clonally represented gene alterations/case, including predominantly nonsilent mutations, and fewer copy number aberrations. These analyses led to the discovery of several genes not previously known to be altered in CLL. Although most of these genes were affected at low frequency in an expanded CLL screening cohort, mutational activation of NOTCH1, observed in 8.3% of CLL at diagnosis, was detected at significantly higher frequency during disease progression toward Richter transformation (31.0%), as well as in chemorefractory CLL (20.8%). Consistent with the association of NOTCH1 mutations with clinically aggressive forms of the disease, NOTCH1 activation at CLL diagnosis emerged as an independent predictor of poor survival. These results provide initial data on the complexity of the CLL coding genome and identify a dysregulated pathway of diagnostic and therapeutic relevance.
0022-1007
1389-1401
Fabbri, Giulia
44c82463-9d9f-4b17-8070-251ff7c780df
Rasi, Silvia
13639ced-c17f-4350-87e4-fb670cee592b
Rossi, Davide
b4b2506d-794c-4c79-8b2d-6767554fd52a
Trifonov, Vladimir
3d2082e4-8dca-4d86-acd2-2c8e486f25d1
Khiabanian, Hossein
a3d879f0-f4db-4146-8520-ecdc98ca9d54
Ma, Jing
3495e3ca-6f13-42ae-8b6a-7d8d4e3166fe
Grunn, Adina
8ca3d4c0-8e4d-41f3-82fe-0db99835ff4a
Fangazio, Marco
054da702-e7e5-4721-84f6-c0cca9abd043
Capello, Daniela
f4d381f4-aaa6-47ae-bebf-53b0aed65055
Monti, Sara
b8d4905b-c63d-47bf-a30a-993be44e0799
Cresta, Stefania
bc5c756c-4800-4ca2-a825-888a607ace3d
Gargiulo, Ernesto
dfc5f5ab-a4f4-45a3-96fb-07a7493661e3
Forconi, Francesco
ce9ed873-58cf-4876-bf3a-9ba1d163edc8
Guarini, Anna
f851faa6-7a52-424b-b788-359c81ed7c4f
Arcaini, Luca
e3e9186c-2630-460f-9116-cde55ad8b625
Paulli, Marco
0d2f2c46-215a-41b1-ad4e-6f8025130a5b
Laurenti, Luca
23c6052d-80af-4fac-92da-2a495a8cb440
Larocca, Luigi M.
9429df66-edeb-46d4-b148-bb5137d91c63
Marasca, Roberto
918148d0-8f99-4a29-8322-1b34f6d7dd00
Gattei, Valter
df828ae8-1b40-4acb-8908-5a6b3d16cf99
Oscier, David
2e7f0cc1-93e2-441e-857d-7314efae08ec
Bertoni, Francesco
13297a2f-854a-4841-a410-d6bfca8afee8
Mullighan, Charles G.
822ead4e-b582-4926-aa6a-5ffe3ddb13fb
Foá, Robin
28cfade0-287d-467e-8882-4d9467b62e5a
Pasqualucci, Laura
1179c741-8c20-4d4e-b9a9-503e41a8e6fe
Rabadan, Raul
4ec979bf-39e8-409f-8671-c71064faae41
Dalla-Favera, Riccardo
74900c86-4420-4aac-a60e-1103fb60182b
Gaidano, Gianluca
1a6a7107-107b-4891-82e0-5fedadd2f65a
Fabbri, Giulia
44c82463-9d9f-4b17-8070-251ff7c780df
Rasi, Silvia
13639ced-c17f-4350-87e4-fb670cee592b
Rossi, Davide
b4b2506d-794c-4c79-8b2d-6767554fd52a
Trifonov, Vladimir
3d2082e4-8dca-4d86-acd2-2c8e486f25d1
Khiabanian, Hossein
a3d879f0-f4db-4146-8520-ecdc98ca9d54
Ma, Jing
3495e3ca-6f13-42ae-8b6a-7d8d4e3166fe
Grunn, Adina
8ca3d4c0-8e4d-41f3-82fe-0db99835ff4a
Fangazio, Marco
054da702-e7e5-4721-84f6-c0cca9abd043
Capello, Daniela
f4d381f4-aaa6-47ae-bebf-53b0aed65055
Monti, Sara
b8d4905b-c63d-47bf-a30a-993be44e0799
Cresta, Stefania
bc5c756c-4800-4ca2-a825-888a607ace3d
Gargiulo, Ernesto
dfc5f5ab-a4f4-45a3-96fb-07a7493661e3
Forconi, Francesco
ce9ed873-58cf-4876-bf3a-9ba1d163edc8
Guarini, Anna
f851faa6-7a52-424b-b788-359c81ed7c4f
Arcaini, Luca
e3e9186c-2630-460f-9116-cde55ad8b625
Paulli, Marco
0d2f2c46-215a-41b1-ad4e-6f8025130a5b
Laurenti, Luca
23c6052d-80af-4fac-92da-2a495a8cb440
Larocca, Luigi M.
9429df66-edeb-46d4-b148-bb5137d91c63
Marasca, Roberto
918148d0-8f99-4a29-8322-1b34f6d7dd00
Gattei, Valter
df828ae8-1b40-4acb-8908-5a6b3d16cf99
Oscier, David
2e7f0cc1-93e2-441e-857d-7314efae08ec
Bertoni, Francesco
13297a2f-854a-4841-a410-d6bfca8afee8
Mullighan, Charles G.
822ead4e-b582-4926-aa6a-5ffe3ddb13fb
Foá, Robin
28cfade0-287d-467e-8882-4d9467b62e5a
Pasqualucci, Laura
1179c741-8c20-4d4e-b9a9-503e41a8e6fe
Rabadan, Raul
4ec979bf-39e8-409f-8671-c71064faae41
Dalla-Favera, Riccardo
74900c86-4420-4aac-a60e-1103fb60182b
Gaidano, Gianluca
1a6a7107-107b-4891-82e0-5fedadd2f65a

Fabbri, Giulia, Rasi, Silvia, Rossi, Davide, Trifonov, Vladimir, Khiabanian, Hossein, Ma, Jing, Grunn, Adina, Fangazio, Marco, Capello, Daniela, Monti, Sara, Cresta, Stefania, Gargiulo, Ernesto, Forconi, Francesco, Guarini, Anna, Arcaini, Luca, Paulli, Marco, Laurenti, Luca, Larocca, Luigi M., Marasca, Roberto, Gattei, Valter, Oscier, David, Bertoni, Francesco, Mullighan, Charles G., Foá, Robin, Pasqualucci, Laura, Rabadan, Raul, Dalla-Favera, Riccardo and Gaidano, Gianluca (2011) Analysis of the chronic lymphocytic leukemia coding genome: role of NOTCH1 mutational activation. Journal of Experimental Medicine, 208 (7), 1389-1401. (doi:10.1084/jem.20110921). (PMID:21670202)

Record type: Article

Abstract

The pathogenesis of chronic lymphocytic leukemia (CLL), the most common leukemia in adults, is still largely unknown. The full spectrum of genetic lesions that are present in the CLL genome, and therefore the number and identity of dysregulated cellular pathways, have not been identified. By combining next-generation sequencing and copy number analysis, we show here that the typical CLL coding genome contains <20 clonally represented gene alterations/case, including predominantly nonsilent mutations, and fewer copy number aberrations. These analyses led to the discovery of several genes not previously known to be altered in CLL. Although most of these genes were affected at low frequency in an expanded CLL screening cohort, mutational activation of NOTCH1, observed in 8.3% of CLL at diagnosis, was detected at significantly higher frequency during disease progression toward Richter transformation (31.0%), as well as in chemorefractory CLL (20.8%). Consistent with the association of NOTCH1 mutations with clinically aggressive forms of the disease, NOTCH1 activation at CLL diagnosis emerged as an independent predictor of poor survival. These results provide initial data on the complexity of the CLL coding genome and identify a dysregulated pathway of diagnostic and therapeutic relevance.

This record has no associated files available for download.

More information

e-pub ahead of print date: 13 June 2011
Published date: 4 July 2011
Organisations: Cancer Sciences

Identifiers

Local EPrints ID: 358121
URI: http://eprints.soton.ac.uk/id/eprint/358121
DOI: doi:10.1084/jem.20110921
ISSN: 0022-1007
PURE UUID: f8fd245e-b0e1-4a1e-87d2-e47cd8df0813
ORCID for Francesco Forconi: ORCID iD orcid.org/0000-0002-2211-1831

Catalogue record

Date deposited: 04 Oct 2013 13:24
Last modified: 15 Mar 2024 03:40

Export record

Altmetrics

Contributors

Author: Giulia Fabbri
Author: Silvia Rasi
Author: Davide Rossi
Author: Vladimir Trifonov
Author: Hossein Khiabanian
Author: Jing Ma
Author: Adina Grunn
Author: Marco Fangazio
Author: Daniela Capello
Author: Sara Monti
Author: Stefania Cresta
Author: Ernesto Gargiulo
Author: Francesco Forconi ORCID iD
Author: Anna Guarini
Author: Luca Arcaini
Author: Marco Paulli
Author: Luca Laurenti
Author: Luigi M. Larocca
Author: Roberto Marasca
Author: Valter Gattei
Author: David Oscier
Author: Francesco Bertoni
Author: Charles G. Mullighan
Author: Robin Foá
Author: Laura Pasqualucci
Author: Raul Rabadan
Author: Riccardo Dalla-Favera
Author: Gianluca Gaidano

Download statistics

Downloads from ePrints over the past year. Other digital versions may also be available to download e.g. from the publisher's website.

View more statistics

Library staff additional information
Atom RSS 1.0 RSS 2.0

Contact ePrints Soton: eprints@soton.ac.uk

ePrints Soton supports OAI 2.0 with a base URL of http://eprints.soton.ac.uk/cgi/oai2

This repository has been built using EPrints software, developed at the University of Southampton, but available to everyone to use.

We use cookies to ensure that we give you the best experience on our website. If you continue without changing your settings, we will assume that you are happy to receive cookies on the University of Southampton website.

×