Efficient presentation of phagocytosed cellular fragments on the major histocompatibility complex class II products of dendritic cells

Efficient presentation of phagocytosed cellular fragments on the major histocompatibility complex class II products of dendritic cells

Cells from the bone marrow can present peptides that are derived from tumors, transplants, and self-tissues. Here we describe how dendritic cells (DCs) process phagocytosed cell fragments onto major histocompatibility complex (MHC) class II products with unusual efficacy. This was monitored with the...

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Published in:The Journal of experimental medicine Vol. 188; no. 11; pp. 2163 - 2173
Main Authors: Inaba, K, Turley, S, Yamaide, F, Iyoda, T, Mahnke, K, Inaba, M, Pack, M, Subklewe, M, Sauter, B, Sheff, D, Albert, M, Bhardwaj, N, Mellman, I, Steinman, R M
Format: Journal Article
Language:English
Published: United States The Rockefeller University Press 07-12-1998
Subjects:
Animals
Antigen Presentation
Dendritic Cells - cytology
Dendritic Cells - immunology
Histocompatibility Antigens Class II - immunology
Humans
Mice
Mice, Inbred BALB C
Mice, Inbred C57BL
Phagocytosis - immunology
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Summary:Cells from the bone marrow can present peptides that are derived from tumors, transplants, and self-tissues. Here we describe how dendritic cells (DCs) process phagocytosed cell fragments onto major histocompatibility complex (MHC) class II products with unusual efficacy. This was monitored with the Y-Ae monoclonal antibody that is specific for complexes of I-Ab MHC class II presenting a peptide derived from I-Ealpha. When immature DCs from I-Ab mice were cultured for 5-20 h with activated I-E+ B blasts, either necrotic or apoptotic, the DCs produced the epitope recognized by the Y-Ae monoclonal antibody and stimulated T cells reactive with the same MHC-peptide complex. Antigen transfer was also observed with human cells, where human histocompatibility leukocyte antigen (HLA)-DRalpha includes the same peptide sequence as mouse I-Ealpha. Antigen transfer was preceded by uptake of B cell fragments into MHC class II-rich compartments. Quantitation of the amount of I-E protein in the B cell fragments revealed that phagocytosed I-E was 1-10 thousand times more efficient in generating MHC-peptide complexes than preprocessed I-E peptide. When we injected different I-E- bearing cells into C57BL/6 mice to look for a similar phenomenon in vivo, we found that short-lived migrating DCs could be processed by most of the recipient DCs in the lymph node. The consequence of antigen transfer from migratory DCs to lymph node DCs is not yet known, but we suggest that in the steady state, i.e., in the absence of stimuli for DC maturation, this transfer leads to peripheral tolerance of the T cell repertoire to self.
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Address correspondence to Ralph M. Steinman, Laboratory of Cellular Physiology and Immunology, The Rockefeller University, 1230 York Ave., New York, NY 10021. Phone: 212-327-8106; Fax: 212-327-8875; E-mail: steinma@rockvax.rockefeller.edu
ISSN:0022-1007
1540-9538
DOI:10.1084/jem.188.11.2163