Structural Basis of Chronic Beryllium Disease: Linking Allergic Hypersensitivity and Autoimmunity

• In chronic beryllium disease, T cells detect Be2+ bound to a DP2/peptide complex
• Be2+ binds in a pocket containing five acidic amino acids from DP2 and the peptide
• The T cell detects surface changes in the DP2/peptide complex, not Be2+ itself
• This disease straddles the border between allergic hypersensitivity and autoimmunity

SummaryT-cell-mediated hypersensitivity to metal cations is common in humans. How the T cell antigen receptor (TCR) recognizes these cations bound to a major histocompatibility complex (MHC) protein and self-peptide is unknown. Individuals carrying the MHCII allele, HLA-DP2, are at risk for chronic beryllium disease (CBD), a debilitating inflammatory lung condition caused by the reaction of CD4 T cells to inhaled beryllium. Here, we show that the T cell ligand is created when a Be2+ cation becomes buried in an HLA-DP2/peptide complex, where it is coordinated by both MHC and peptide acidic amino acids. Surprisingly, the TCR does not interact with the Be2+ itself, but rather with surface changes induced by the firmly bound Be2+ and an accompanying Na+ cation. Thus, CBD, by creating a new antigen by indirectly modifying the structure of preexisting self MHC-peptide complex, lies on the border between allergic hypersensitivity and autoimmunity.

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