Notch1 is a frequent mutational target in chemically induced lymphoma in mouse
(2008) In International Journal of Cancer 123(11). p.2720-2724- Abstract
Activating Notch1 mutations have been reported in human T-line-age acute lymphoblastic leukemia (T-ALL) and lymphomas from genetically modified mice. We report that Notch1 is a prevalent and major mutational target in chemically induced mouse lymphoma. The regions of the gene that are frequently mutated are the heterodimerization domain and the N-terminal ligand-binding region, important for protein stability, and the polypeptide rich in proline, glutamate, serine and threonine (PEST) domains, which is critical for protein degradation. Another gene, CDC4, is also involved in Notch1 degradation and shows frequent mutations. Mutations in the heterodimerization and the ligand-binding regions may cause ligand-independent signaling, whereas... (More)
Activating Notch1 mutations have been reported in human T-line-age acute lymphoblastic leukemia (T-ALL) and lymphomas from genetically modified mice. We report that Notch1 is a prevalent and major mutational target in chemically induced mouse lymphoma. The regions of the gene that are frequently mutated are the heterodimerization domain and the N-terminal ligand-binding region, important for protein stability, and the polypeptide rich in proline, glutamate, serine and threonine (PEST) domains, which is critical for protein degradation. Another gene, CDC4, is also involved in Notch1 degradation and shows frequent mutations. Mutations in the heterodimerization and the ligand-binding regions may cause ligand-independent signaling, whereas mutations preventing protein degradation result in accumulation of intracellular Notch1. We analyzed 103 chemical-induced mouse lymphomas for mutations in the Notch1 gene using single strand conformation analysis (SSCA) and DNA sequencing. Genetic alterations resulting in premature truncation of Notch1 were identified in 28 tumors, whereas 8 revealed alterations in the heterodimerization and 16 harbored deletions in the ligand-binding region. Dideoxycytidine-induced lymphomas displayed the highest frequency of Notch1 mutations (49%), whereas in butadiene- and phenolphthalein-induced tumors showed lower frequencies (26 and 10%, respectively). In total, 26 novel and 3 previously reported mutations were detected. This report shows that Notch1 is a prevalent and major mutational target for 2′,3′-dideoxycytidine and butadiene-induced lymphoma.
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- author
- Karlsson, Anneli ; Ungerbäck, Jonas LU ; Rasmussen, Anna LU ; French, John E. and Söderkvist, Peter
- publishing date
- 2008-12-01
- type
- Contribution to journal
- publication status
- published
- keywords
- Butadiene, Dideoxycytidine, hN1, Phenolphthalein, TAN-1
- in
- International Journal of Cancer
- volume
- 123
- issue
- 11
- pages
- 5 pages
- publisher
- John Wiley & Sons Inc.
- external identifiers
-
- scopus:57349097586
- pmid:18798262
- ISSN
- 0020-7136
- DOI
- 10.1002/ijc.23832
- language
- English
- LU publication?
- no
- id
- 967046dd-8b2d-4858-9519-f4f87d5b1373
- date added to LUP
- 2023-10-16 10:42:04
- date last changed
- 2024-01-04 06:12:15
@article{967046dd-8b2d-4858-9519-f4f87d5b1373, abstract = {{<p>Activating Notch1 mutations have been reported in human T-line-age acute lymphoblastic leukemia (T-ALL) and lymphomas from genetically modified mice. We report that Notch1 is a prevalent and major mutational target in chemically induced mouse lymphoma. The regions of the gene that are frequently mutated are the heterodimerization domain and the N-terminal ligand-binding region, important for protein stability, and the polypeptide rich in proline, glutamate, serine and threonine (PEST) domains, which is critical for protein degradation. Another gene, CDC4, is also involved in Notch1 degradation and shows frequent mutations. Mutations in the heterodimerization and the ligand-binding regions may cause ligand-independent signaling, whereas mutations preventing protein degradation result in accumulation of intracellular Notch1. We analyzed 103 chemical-induced mouse lymphomas for mutations in the Notch1 gene using single strand conformation analysis (SSCA) and DNA sequencing. Genetic alterations resulting in premature truncation of Notch1 were identified in 28 tumors, whereas 8 revealed alterations in the heterodimerization and 16 harbored deletions in the ligand-binding region. Dideoxycytidine-induced lymphomas displayed the highest frequency of Notch1 mutations (49%), whereas in butadiene- and phenolphthalein-induced tumors showed lower frequencies (26 and 10%, respectively). In total, 26 novel and 3 previously reported mutations were detected. This report shows that Notch1 is a prevalent and major mutational target for 2′,3′-dideoxycytidine and butadiene-induced lymphoma.</p>}}, author = {{Karlsson, Anneli and Ungerbäck, Jonas and Rasmussen, Anna and French, John E. and Söderkvist, Peter}}, issn = {{0020-7136}}, keywords = {{Butadiene; Dideoxycytidine; hN1; Phenolphthalein; TAN-1}}, language = {{eng}}, month = {{12}}, number = {{11}}, pages = {{2720--2724}}, publisher = {{John Wiley & Sons Inc.}}, series = {{International Journal of Cancer}}, title = {{Notch1 is a frequent mutational target in chemically induced lymphoma in mouse}}, url = {{http://dx.doi.org/10.1002/ijc.23832}}, doi = {{10.1002/ijc.23832}}, volume = {{123}}, year = {{2008}}, }