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Structural basis of molecular mimicry.
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A highly tilted binding mode by a self-reactive T cell receptor results in altered engagement of peptide and MHC.
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Structure of a TCR with high affinity for self-antigen reveals basis for escape from negative selection.
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Lupus Susceptibility Loci Predispose Mice to Clonal Lymphocytic Responses and Myeloid Expansion.
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Molecular Rules Underpinning Enhanced Affinity Binding of Human T Cell Receptors Engineered for Immunotherapy.
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T cell receptor interactions with human leukocyte antigen govern indirect peptide selectivity for the cancer testis antigen MAGE-A4.
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Peptide mimotopes alter T cell function in cancer and autoimmunity.
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本文引用的文献

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Processing of X-ray diffraction data collected in oscillation mode.
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Crystal structure of the HLA-DM-HLA-DR1 complex defines mechanisms for rapid peptide selection.
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Self-awareness: how self-peptide/MHC complexes are essential in the development of T cells.
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Structural basis for self-recognition by autoimmune T-cell receptors.
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The genetics of multiple sclerosis: an up-to-date review.
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Crystal structure of a complete ternary complex of T-cell receptor, peptide-MHC, and CD4.
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Molecular mimicry as an inducing trigger for CNS autoimmune demyelinating disease.
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T cell receptor signaling is limited by docking geometry to peptide-major histocompatibility complex.
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TCRs used in cancer gene therapy cross-react with MART-1/Melan-A tumor antigens via distinct mechanisms.
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