Title of article
Block of T cell development in P53-deficient mice accelerates development of lymphomas with characteristic RAG-dependent cytogenetic alterations
Author/Authors
Haines، نويسنده , , Brian B. and Ryu، نويسنده , , Chun Jeih and Chang، نويسنده , , Sandy and Protopopov، نويسنده , , Alexei and Luch، نويسنده , , Andreas and Kang، نويسنده , , Yun Hee and Draganov، نويسنده , , Dobrin D. and Fragoso، نويسنده , , Maria F. and Paik، نويسنده , , Sang Gi and Hong، نويسنده , , Hyo Jeong and DePinho، نويسنده , , Ronald A. and Chen، نويسنده , , Jianzhu، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2006
Pages
12
From page
109
To page
120
Abstract
Summary
eficient in the DNA damage sensor P53 display normal T cell development but eventually succumb to thymic lymphomas. Here, we show that inactivation of the TCR β gene enhancer (Eβ) results in a block of T cell development at stages where recombination-activating genes (RAG) are expressed. Introduction of the Eβ mutation into p53−/− mice dramatically accelerates the onset of lethal thymic lymphomas that harbor RAG-dependent aberrant rearrangements, chromosome 14 and 12 translocations, and amplification of the chromosomal region 9A1–A5.3. Phenotypic and genetic analyses suggest that lymphomas emerge through a normal thymocyte development pathway. These findings provide genetic evidence that block of lymphocyte development at stages with RAG endonuclease activity can provoke lymphomagenesis on a background with deficient DNA damage responses.
Keywords
CELLCYCLE
Journal title
Cancer Cell
Serial Year
2006
Journal title
Cancer Cell
Record number
1336358
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