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The loss of PTEN allows TCR alphabeta lineage thymocytes to bypass IL-7 and Pre-TCR-mediated signaling.

Thijs J Hagenbeek ,
Marianne Naspetti ,
Fabrice Malergue ,
Fabien Garçon ,
Jacques A Nunès ,
Kitty B J M Cleutjens ,
Jan Trapman ,
Paul Krimpenfort ,
Hergen Spits

Abstract

The phosphatase and tensin homologue deleted on chromosome 10 (PTEN) negatively regulates cell survival and proliferation mediated by phosphoinositol 3 kinases. We have explored the role of the phosphoinositol(3,4,5)P3-phosphatase PTEN in T cell development by analyzing mice with a T cell-specific deletion of PTEN. Pten(flox/flox)Lck-Cre mice developed thymic lymphomas, but before the onset of tumors, they showed normal thymic cellularity. To reveal a regulatory role of PTEN in proliferation of developing T cells we have crossed PTEN-deficient mice with mice deficient for interleukin (IL)-7 receptor and pre-T cell receptor (TCR) signaling. Analysis of mice deficient for Pten and CD3gamma; Pten and gammac; or Pten, gammac, and Rag2 revealed that deletion of PTEN can substitute for both IL-7 and pre-TCR signals. These double- and triple-deficient mice all develop normal levels of CD4CD8 double negative and double positive thymocytes. These data indicate that PTEN is an important regulator of proliferation of developing T cells in the thymus.

More about this publication

The Journal of experimental medicine

Volume 200
Issue nr. 7
Pages 883-94
Publication date 04-10-2004

Full text links

Publisher website (DOI) 10.1084/jem.20040495
Europe PubMed Central 15452180
Pubmed 15452180

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