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The fate of CD4-8- T cell receptor-alpha beta+ thymocytes.

H I Levitsky, P T Golumbek and D M Pardoll
J Immunol February 15, 1991, 146 (4) 1113-1117;
H I Levitsky
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P T Golumbek
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D M Pardoll
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Abstract

CD4-8- TCR-alpha beta+ thymocytes represent a distinct population whose fate and function have remained a mystery. We show here that this thymocyte subset bears NK1, a surface Ag previously thought to be expressed exclusively by TCR- NK cells. Analysis of peripheral lymphocytes for the coexpression of TCR-alpha beta and NK1 revealed a subset with similar characteristics to the NK1+ thymocytes: a large fraction that are CD4-8- and a skewed TCR repertoire in which V beta 8 is overrepresented. Thymus transplant experiments into congenically marked athymic (nude) mice revealed that the NK1+TCR alpha beta+ subset was exclusively thymus derived and represented a distinct subset from the thymus-independent NK1+TCR- population. Finally, the NK1+TCR alpha beta+ population preferentially localizes to the bone marrow. These results demonstrate that this T cell subset is exported to the periphery after developing in the thymus. Their unique surface Ag expression and tissue localization suggest an immune function distinct from classical T cells.

  • Copyright © 1991 by American Association of Immunologists
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The Journal of Immunology
Vol. 146, Issue 4
15 Feb 1991
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The fate of CD4-8- T cell receptor-alpha beta+ thymocytes.
H I Levitsky, P T Golumbek, D M Pardoll
The Journal of Immunology February 15, 1991, 146 (4) 1113-1117;

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The fate of CD4-8- T cell receptor-alpha beta+ thymocytes.
H I Levitsky, P T Golumbek, D M Pardoll
The Journal of Immunology February 15, 1991, 146 (4) 1113-1117;
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Print ISSN 0022-1767        Online ISSN 1550-6606