Cathepsin L: Critical Role in Ii Degradation and CD4 T Cell Selection in the Thymus

T Nakagawa; Wera Roth; Phillip Wong; Andrew Nelson; Andrew G. Farr; Jan M. Deussing; Jóse A. Villadangos; Hidde L. Ploegh; Christoph Peters; Alexander Y. Rudensky

doi:10.1126/science.280.5362.450

Cathepsin L: Critical Role in Ii Degradation and CD4 T Cell Selection in the Thymus

T Nakagawa(Howard Hughes Medical Institute), Wera Roth(Howard Hughes Medical Institute), Phillip Wong(Howard Hughes Medical Institute), Andrew Nelson(Howard Hughes Medical Institute), Andrew G. Farr(Howard Hughes Medical Institute), Jan M. Deussing(Howard Hughes Medical Institute), Jóse A. Villadangos(Howard Hughes Medical Institute), Hidde L. Ploegh(Howard Hughes Medical Institute), Christoph Peters(Howard Hughes Medical Institute), Alexander Y. Rudensky(Howard Hughes Medical Institute)

Science

April 17, 1998

10.1126/science.280.5362.450

Cited by 659

Abstract

Degradation of invariant chain (Ii) is a critical step in major histocompatibility complex class II–restricted antigen presentation. Cathepsin L was found to be necessary for Ii degradation in cortical thymic epithelial cells (cTECs), but not in bone marrow (BM)–derived antigen-presenting cells (APCs). Consequently, positive selection of CD4 + T cells was reduced. Because different cysteine proteinases are responsible for specific Ii degradation steps in cTECs and BM-derived APCs, the proteolytic environment in cells mediating positive and negative selection may be distinct. The identification of a protease involved in class II presentation in a tissue-specific manner suggests a potential means of manipulating CD4 + T cell responsiveness in vivo.

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