Clarifying the role of Stat5 in lymphoid development and Abelson-induced transformation

Author:

Hoelbl Andrea1,Kovacic Boris1,Kerenyi Marc A.1,Simma Olivia1,Warsch Wolfgang1,Cui Yongzhi1,Beug Hartmut1,Hennighausen Lothar1,Moriggl Richard1,Sexl Veronika1

Affiliation:

1. From the Institute of Pharmacology and Max F. Perutz Laboratories, Medical University of Vienna (MUW), Austria; Institute of Molecular Pathology (IMP), Vienna, Austria; Laboratory of Genetics and Physiology, National Institutes of Health (NIH), Bethesda, MD; and Ludwig Boltzmann Institute for Cancer Research (LBI-CR), Vienna, Austria.

Abstract

AbstractThe Stat5 transcription factors Stat5a and Stat5b have been implicated in lymphoid development and transformation. Most studies have employed Stat5a/b-deficient mice where gene targeting disrupted the first protein-coding exon, resulting in the expression of N-terminally truncated forms of Stat5a/b (Stat5a/bΔN/ΔN mice). We have now reanalyzed lymphoid development in Stat5a/bnull/null mice having a complete deletion of the Stat5a/b gene locus. The few surviving Stat5a/bnull/null mice lacked CD8+ T lymphocytes. A massive reduction of CD8+ T cells was also found in Stat5a/bfl/fllck-cre transgenic animals. While γδ T-cell receptor–positive (γδTCR+) cells were expressed at normal levels in Stat5a/bΔN/ΔN mice, they were completely absent in Stat5a/bnull/null animals. Moreover, B-cell maturation was abrogated at the pre–pro-B-cell stage in Stat5a/bnull/null mice, whereas Stat5a/bΔN/ΔN B-lymphoid cells developed to the early pro-B-cell stage. In vitro assays using fetal liver-cell cultures confirmed this observation. Most strikingly, Stat5a/bnull/null cells were resistant to transformation and leukemia development induced by Abelson oncogenes, whereas Stat5a/bΔN/ΔN-derived cells readily transformed. These findings show distinct lymphoid defects for Stat5a/bΔN/ΔN and Stat5a/bnull/null mice and define a novel functional role for the N-termini of Stat5a/b in B-lymphoid transformation.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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