In most human and mouse antigen-presenting cells, the majority of intracellular major histocompatibility complex (MHC) class II molecules resides in late endocytic MHC class II compartments (MIICs), thought to function in antigen processing and peptide loading. However, in mouse A20 B cells, early endocytic class II-containing vesicles (CIIVs) have been reported to contain most of the intracellular MHC class II molecules and have also been implicated in formation of MHC class II–peptide complexes. To address this discrepancy, we have studied in great detail the endocytic pathways of both a human (6H5.DM) and a mouse (A20.Ab) B cell line. Using quantitative immunoelectron microscopy on cryosections of cells that had been pulse–chased with transferrin-HRP or BSA-gold as endocytic tracers, we have identified up to six endocytic subcompartments including an early MIIC type enriched in invariant chain, suggesting that it serves as an important entrance to the endocytic pathway for newly synthesized MHC class II/invariant chain complexes. In addition, early MIICs represented the earliest endocytic compartment containing MHC class II– peptide complexes, as shown by using an antibody against an abundant endogenous class II–peptide complex. The early MIIC exhibited several though not all of the characteristics reported for the CIIV and was situated just downstream of early endosomes. We have not encountered any special class II-containing endocytic structures besides those normally present in nonantigen-presenting cells. Our results therefore suggest that B cells use conventional endocytic compartments rather than having developed a unique compartment to accomplish MHC class II presentation.
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3 November 1997
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November 03 1997
Major Histocompatibility Complex Class II Compartments in Human and Mouse B Lymphoblasts Represent Conventional Endocytic Compartments
Monique J. Kleijmeer,
Monique J. Kleijmeer
*Department of Cell Biology, School of Medicine and Institute of Biomembranes, Utrecht University, 3584 CX Utrecht, The Netherlands; and ‡Department of Immunology and §Howard Hughes Medical Institute, University of Washington, School of Medicine, Seattle, Washington 98105
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Stanislaw Morkowski,
Stanislaw Morkowski
*Department of Cell Biology, School of Medicine and Institute of Biomembranes, Utrecht University, 3584 CX Utrecht, The Netherlands; and ‡Department of Immunology and §Howard Hughes Medical Institute, University of Washington, School of Medicine, Seattle, Washington 98105
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Janice M. Griffith,
Janice M. Griffith
*Department of Cell Biology, School of Medicine and Institute of Biomembranes, Utrecht University, 3584 CX Utrecht, The Netherlands; and ‡Department of Immunology and §Howard Hughes Medical Institute, University of Washington, School of Medicine, Seattle, Washington 98105
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Alexander Y. Rudensky,
Alexander Y. Rudensky
*Department of Cell Biology, School of Medicine and Institute of Biomembranes, Utrecht University, 3584 CX Utrecht, The Netherlands; and ‡Department of Immunology and §Howard Hughes Medical Institute, University of Washington, School of Medicine, Seattle, Washington 98105
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Hans J. Geuze
Hans J. Geuze
*Department of Cell Biology, School of Medicine and Institute of Biomembranes, Utrecht University, 3584 CX Utrecht, The Netherlands; and ‡Department of Immunology and §Howard Hughes Medical Institute, University of Washington, School of Medicine, Seattle, Washington 98105
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Monique J. Kleijmeer
*Department of Cell Biology, School of Medicine and Institute of Biomembranes, Utrecht University, 3584 CX Utrecht, The Netherlands; and ‡Department of Immunology and §Howard Hughes Medical Institute, University of Washington, School of Medicine, Seattle, Washington 98105
Stanislaw Morkowski
*Department of Cell Biology, School of Medicine and Institute of Biomembranes, Utrecht University, 3584 CX Utrecht, The Netherlands; and ‡Department of Immunology and §Howard Hughes Medical Institute, University of Washington, School of Medicine, Seattle, Washington 98105
Janice M. Griffith
*Department of Cell Biology, School of Medicine and Institute of Biomembranes, Utrecht University, 3584 CX Utrecht, The Netherlands; and ‡Department of Immunology and §Howard Hughes Medical Institute, University of Washington, School of Medicine, Seattle, Washington 98105
Alexander Y. Rudensky
*Department of Cell Biology, School of Medicine and Institute of Biomembranes, Utrecht University, 3584 CX Utrecht, The Netherlands; and ‡Department of Immunology and §Howard Hughes Medical Institute, University of Washington, School of Medicine, Seattle, Washington 98105
Hans J. Geuze
*Department of Cell Biology, School of Medicine and Institute of Biomembranes, Utrecht University, 3584 CX Utrecht, The Netherlands; and ‡Department of Immunology and §Howard Hughes Medical Institute, University of Washington, School of Medicine, Seattle, Washington 98105
Address all correspondence to Hans J. Geuze, Medical School, Department of Cell Biology, AZU H02.314, Heidelberglaan 100, 3584 CX Utrecht, The Netherlands. Tel.: (31) 30-2507652. Fax: (31) 30-2541797. E-mail: [email protected]
Received:
February 17 1997
Revision Received:
August 22 1997
Online ISSN: 1540-8140
Print ISSN: 0021-9525
1997
J Cell Biol (1997) 139 (3): 639–649.
Article history
Received:
February 17 1997
Revision Received:
August 22 1997
Citation
Monique J. Kleijmeer, Stanislaw Morkowski, Janice M. Griffith, Alexander Y. Rudensky, Hans J. Geuze; Major Histocompatibility Complex Class II Compartments in Human and Mouse B Lymphoblasts Represent Conventional Endocytic Compartments . J Cell Biol 3 November 1997; 139 (3): 639–649. doi: https://doi.org/10.1083/jcb.139.3.639
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