Interferon (IFN)-γ–induced cells express the proteasome subunits low molecular weight protein (LMP)2, LMP7, and MECL-1 (multicatalytic endopeptidase complex–like 1), leading to the formation of immunoproteasomes. Although these subunits are thought to optimize MHC class I antigen processing, the extent of their role and the mechanistic aspects involved remain unclear. Herein, we study the proteolytic generation of an human histocompatibility leukocyte antigen (HLA)-Aw68–restricted hepatitis B virus core antigen (HBcAg) cytotoxic T lymphocyte (CTL) epitope that is recognized by peripheral blood lymphocytes from patients with acute self-limited but not chronic hepatitis B virus (HBV). Immunological data suggest that IFN-γ–induced rather than uninduced HeLa cells process and present the HBV CTL epitope upon infection with HBcAg-expressing vaccinia viruses. Analyses of 20S proteasome digests of synthetic polypeptides covering the antigenic HBcAg peptide demonstrate that only immunoproteasomes efficiently perform the cleavages needed for the liberation of this HBV CTL epitope. Although the concerted presence of the three immunosubunits appears essential, we find that both catalytically active LMP7 and inactive LMP7 T1A support CTL epitope generation. We conclude that LMP7 influences the structural features of 20S proteasomes, thereby enhancing the activity of the LMP2 and MECL-1 catalytic sites, which provide cleavage specificity. Thus, LMP7 incorporation is of greater functional importance for the generation of an HBV CTL epitope than cleavage specificity.
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7 February 2000
Article|
February 07 2000
Efficient Generation of a Hepatitis B Virus Cytotoxic T Lymphocyte Epitope Requires the Structural Features of Immunoproteasomes
Alice J.A.M. Sijts,
Alice J.A.M. Sijts
aFrom the Institute of Biochemistry, Charité, Humboldt University Berlin, 10117 Berlin, Germany
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Thomas Ruppert,
Thomas Ruppert
bMax von Pettenkofer Institute, 80336 München, Germany
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Barbara Rehermann,
Barbara Rehermann
cLiver Diseases Section, Digestive Diseases Branch, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, Maryland 20892
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Marion Schmidt,
Marion Schmidt
aFrom the Institute of Biochemistry, Charité, Humboldt University Berlin, 10117 Berlin, Germany
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Ulrich Koszinowski,
Ulrich Koszinowski
bMax von Pettenkofer Institute, 80336 München, Germany
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Peter-M. Kloetzel
Peter-M. Kloetzel
aFrom the Institute of Biochemistry, Charité, Humboldt University Berlin, 10117 Berlin, Germany
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Alice J.A.M. Sijts
aFrom the Institute of Biochemistry, Charité, Humboldt University Berlin, 10117 Berlin, Germany
Thomas Ruppert
bMax von Pettenkofer Institute, 80336 München, Germany
Barbara Rehermann
cLiver Diseases Section, Digestive Diseases Branch, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, Maryland 20892
Marion Schmidt
aFrom the Institute of Biochemistry, Charité, Humboldt University Berlin, 10117 Berlin, Germany
Ulrich Koszinowski
bMax von Pettenkofer Institute, 80336 München, Germany
Peter-M. Kloetzel
aFrom the Institute of Biochemistry, Charité, Humboldt University Berlin, 10117 Berlin, Germany
Abbreviations used in this paper: DCPs, double cleavage products; HBcAg, hepatitis B virus core antigen; HBV, hepatitis B virus; LMP, low molecular weight protein; MECL, multicatalytic endopeptidase complex–like; r, recombinant; SCPs, single cleavage products.
Received:
May 17 1999
Revision Requested:
September 01 1999
Accepted:
October 29 1999
Online ISSN: 1540-9538
Print ISSN: 0022-1007
© 2000 The Rockefeller University Press
2000
The Rockefeller University Press
J Exp Med (2000) 191 (3): 503–514.
Article history
Received:
May 17 1999
Revision Requested:
September 01 1999
Accepted:
October 29 1999
Citation
Alice J.A.M. Sijts, Thomas Ruppert, Barbara Rehermann, Marion Schmidt, Ulrich Koszinowski, Peter-M. Kloetzel; Efficient Generation of a Hepatitis B Virus Cytotoxic T Lymphocyte Epitope Requires the Structural Features of Immunoproteasomes. J Exp Med 7 February 2000; 191 (3): 503–514. doi: https://doi.org/10.1084/jem.191.3.503
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