Expression of recombination-activating gene in mature peripheral T cells in Peyer's patch

doi:10.1093/intimm/dxg040

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International Immunology, Vol. 15, No. 3, pp. 393-402, March 2003
© 2003 Japanese Society for Immunology

FEATURED ARTICLE OF THE MONTH

Expression of recombination-activating gene in mature peripheral T cells in Peyer’s patch

Eisuke Kondo¹, Hiroshi Wakao¹, Haruhiko Koseki², Toshitada Takemori³, Satoshi Kojo¹, Michishige Harada¹, Minako Takahashi¹, Sakura Sakata¹, Chiori Shimizu¹, Toshihiro Ito¹, Toshinori Nakayama¹ and Masaru Taniguchi¹

¹ Laboratory for Immune Regulation, RIKEN Research Center for Allergy and Immunology, and Department of Molecular Immunology, and ² Department of Molecular Embryology, Graduate School of Medicine, Chiba University, Chiba 260-8670, Japan ³ Department of Immunology, National Institute of Infectious Diseases Tokyo 162-8640, Japan

Correspondence to: M. Taniguchi, Department of Molecular Immunology, Graduate School of Medicine, Chiba University, 1-8-1 Inohana, Chuo-ku, Chiba 260-8670, Japan. E-mail: taniguti{at}med.m.chiba-u.ac.jp
Transmitting editor: M. Miyasaka

Recombination-activating gene (RAG) 1 and 2 are essential forthe gene rearrangement of antigen receptors of both T and Bcells. To investigate RAG gene expression in peripheral lymphoidorgans other than the thymus and bone marrow, we establishedmice in which a green fluorescent protein (GFP) gene is knocked-inthe RAG2 gene locus (RAG2-GFP mice). In the thymus and bonemarrow of heterozygous RAG2-GFP mice, as expected, GFP expressionwas detected in the appropriate stages of developing T and Bcells. Interestingly, only a fraction of Thy-1.2⁺ cells in thePeyer’s patch were found to be GFP⁺ amongst the peripherallymphoid organs. The GFP⁺ cells expressed high levels of surfaceTCRß and CD3, suggesting mature T cells with rearrangedTCR ${alpha}$ ß. However, they showed activated/memory phenotypes,i.e. CD45RB^low, CD69^high, CD44^high and CD62L^low, and belongedto a CD4⁺CD8⁺ population expressing c-kit, IL-7R and pT ${alpha}$ characteristicof immature developing lymphocytes. Moreover, RAG⁺ Peyer’spatch T cells seem to be of thymic origin as judged by theirexpression of CD8 ${alpha}$ ß. These results show that thereexists a fraction of mature T cells expressing RAG genes inthe Peyer’s patch, implying a potential for a secondaryrearrangement of TCR in extrathymic tissues.

Keywords: green fluorescent protein, knock-in mice, RAG2, TCR rearrangement

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