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Structural reorganization of the antigen-binding groove of human CD1b for presentation of mycobacterial sulfoglycolipids
Authors:Garcia-Alles Luis F  Collmann Anthony  Versluis Cees  Lindner Buko  Guiard Julie  Maveyraud Laurent  Huc Emilie  Im Jin S  Sansano Sebastiano  Brando Thérèse  Julien Sylviane  Prandi Jacques  Gilleron Martine  Porcelli Steven A  de la Salle Henri  Heck Albert J R  Mori Lucia  Puzo Germain  Mourey Lionel  De Libero Gennaro
Affiliation:Centre National de la Recherche Scientifique, Institut de Pharmacologie et de Biologie Structurale, F-31077 Toulouse, France.
Abstract:The mechanisms permitting nonpolymorphic CD1 molecules to present lipid antigens that differ considerably in polar head and aliphatic tails remain elusive. It is also unclear why hydrophobic motifs in the aliphatic tails of some antigens, which presumably embed inside CD1 pockets, contribute to determinants for T-cell recognition. The 1.9-Å crystal structure of an active complex of CD1b and a mycobacterial diacylsulfoglycolipid presented here provides some clues. Upon antigen binding, endogenous spacers of CD1b, which consist of a mixture of diradylglycerols, moved considerably within the lipid-binding groove. Spacer displacement was accompanied by F’ pocket closure and an extensive rearrangement of residues exposed to T-cell receptors. Such structural reorganization resulted in reduction of the A’ pocket capacity and led to incomplete embedding of the methyl-ramified portion of the phthioceranoyl chain of the antigen, explaining why such hydrophobic motifs are critical for T-cell receptor recognition. Mutagenesis experiments supported the functional importance of the observed structural alterations for T-cell stimulation. Overall, our data delineate a complex molecular mechanism combining spacer repositioning and ligand-induced conformational changes that, together with pocket intricacy, endows CD1b with the required molecular plasticity to present a broad range of structurally diverse antigens.
Keywords:three-dimensional structure   groove shrinking   diacylglycerol endogenous ligand   T lymphocyte activation   CD1b mutant transfectant
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