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Blood, 1 July 2005, Vol. 106, No. 1, pp. 193-200.
Prepublished online as a Blood First Edition Paper on March 3, 2005; DOI 10.1182/blood-2004-12-4886.


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Submitted December 22, 2004
Accepted February 27, 2005

T cell generation by lymph node resident progenitor cells

Rafik Terra, Isabelle Louis, Richard Le Blanc, Sophie Ouellet, Juan C Zuniga-Pflucker, and Claude Perreault*

Institute of Research in Immunology and Cancer, University of Montreal, Montreal, Quebec, Canada; Guy-Bernier Research Center, Maisonneuve-Rosemont Hospital, Montreal, Quebec, Canada
Centre Hospitalier Universitaire de Sherbrooke, Fleurimont, Quebec, Canada
Guy-Bernier Research Center, Maisonneuve-Rosemont Hospital, Montreal, Quebec, Canada
Department of Immunology, Sunnybrook and Women's College Health Sciences Centre, University of Toronto, Toronto, Ontario, Canada

* Corresponding author; email: c.perreault{at}videotron.ca.

In the thymus, two types of Lin-Sca-1+ progenitors can generate T lineage cells: c-KithiIL-7R{alpha}- and c-KitloIL-7R{alpha}+. While c-KithiIL-7R{alpha}- progenitors are absent, c-KitloIL-7R{alpha}+ progenitors are abundant in the LN. c-KitloIL-7R{alpha}+ progenitors undergo abortive T cell commitment in the LN and become arrested in G1 phase of the cell cycle because they fail both to upregulate c-myb, c-myc, and cyclin D2 and to repress junB, p16INK4a and p21Cip1/WAF. As a result, development of LN c-KitloIL-7R{alpha}+ progenitors is blocked at an intermediate CD44+CD25lo development stage in vivo, and LN derived progenitors fail to generate mature T cells when cultured with OP9-DL1 stromal cells. LN stroma can provide key signals for T cell development including IL-7, Kit-ligand, and Delta-like1, but lacks Wnt4 and Wnt7b transcripts. LN c-KitloIL-7R{alpha}+ progenitors are able to generate mature T cells when cultured with stromal cells producing Wnt4, or upon in vivo exposure to Oncostatin M whose signaling pathway intersects with Wnt. Thus, supplying Wnt signals to c-KitloIL-7R{alpha}+ progenitors may be sufficient to transform the LN into a primary T lymphoid organ. These data provide unique insights into the essence of a primary T lymphoid organ, and into how a cryptic extrathymic T cell development pathway can be amplified.


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