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HLA-DM captures partially empty HLA-DR molecules for catalyzed removal of peptide.
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Bidirectional binding of invariant chain peptides to an MHC class II molecule.
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A reductionist cell-free major histocompatibility complex class II antigen processing system identifies immunodominant epitopes.
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H2-O, a MHC class II-like protein, sets a threshold for B-cell entry into germinal centers.
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Targeted regulation of self-peptide presentation prevents type I diabetes in mice without disrupting general immunocompetence.
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Recruitment of antigen-specific CD8+ T cells in response to infection is markedly efficient.
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The quality control of MHC class I peptide loading.
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The convergent roles of tapasin and HLA-DM in antigen presentation.
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