Cathepsin L Regulates CD4+ T Cell Selection Independently of Its Effect on Invariant Chain: A Role in the Generation of Positively Selecting Peptide Ligands

doi:10.1084/jem.20011904

Published 20 May 2002. doi:10.1084/jem.20011904

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© Rockefeller University Press, 0022-1007/2002/5/1349/ $5.00
The Journal of Experimental Medicine, Volume 195, Number 10, May 20, 2002 1349-1358
Cathepsin L Regulates CD4⁺ T Cell Selection Independently of Its Effect on Invariant Chain : A Role in the Generation of Positively Selecting Peptide Ligands

Karen Honey¹^,2, Terry Nakagawa¹, Christoph Peters³ and Alexander Rudensky¹^,2

¹ Department of Immunology, University of Washington School of Medicine, Seattle, WA 98195
² Howard Hughes Medical Institute, University of Washington School of Medicine, Seattle, WA 98195
³ Medizinische Molekularbiologie, Abteilung Heamatologie-Onkologie, Klinikum der Albert Ludwigs Universitat Freiburg, 79106 Freiburg, Germany

Address correspondence to A. Rudensky, Department of Immunology, UW I 604 J, 1959 NE Pacific St., Seattle, WA 98195-7370. Phone: 206-685-9310; Fax: 206-685-3612; E-mail: aruden{at}u.washington.edu

CD4⁺ T cells are positively selected in the thymus on peptidespresented in the context of major histocompatibility complexclass II molecules expressed on cortical thymic epithelial cells.Molecules regulating this peptide presentation play a role indetermining the outcome of positive selection. Cathepsin L mediatesinvariant chain processing in cortical thymic epithelial cells,and animals of the I-A^b haplotype deficient in this enzyme exhibitimpaired CD4⁺ T cell selection. To determine whether the selectiondefect is due solely to the block in invariant chain cleavagewe analyzed cathepsin L–deficient mice expressing theI-A^q haplotype which has little dependence upon invariant chainprocessing for peptide presentation. Our data indicate the cathepsinL defect in CD4⁺ T cell selection is haplotype independent,and thus imply it is independent of invariant chain degradation.This was confirmed by analysis of I-A^b mice deficient in bothcathepsin L and invariant chain. We show that the defect inpositive selection in the cathepsin L^-/- thymus is specificfor CD4⁺ T cells that can be selected in a wild-type and provideevidence that the repertoire of T cells selected differs fromthat in wild-type mice, suggesting cortical thymic epithelialcells in cathepsin L knockout mice express an altered peptiderepertoire. Thus, we propose a novel role for cathepsin L inregulating positive selection by generating the major histocompatibilitycomplex class II bound peptide ligands presented by corticalthymic epithelial cells.

Key Words: cathepsin • positive selection • CD4 T cells • invariant chain • epitope generation

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