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Saposins utilize two strategies for lipid transfer and CD1 antigen presentation

  作者 Leon, L; Tatituri, RVV; Grenha, R; Sun, Y; Barral, DC; Minnaard, AJ; Bhowruth, V; Veerapen, N; Besra, GS; Kasmar, A; Peng, W; Moody, DB; Grabowski, GA; Brenner, MB  
  选自 期刊  Proceedings of the National Academy of Sciences of the United States of America;  卷期  2012年109-12;  页码  4357-4364  
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[摘要]Transferring lipid antigens from membranes into CD1 antigen-presenting proteins represents a major molecular hurdle necessary for T-cell recognition. Saposins facilitate this process, but the mechanisms used are not well understood. We found that saposin B forms soluble saposin protein-lipid complexes detected by native gel electrophoresis that can directly load CD1 proteins. Because saposin B must bind lipids directly to function, we found it could not accommodate long acyl chain containing lipids. In contrast, saposin C facilitates CD1 lipid loading in a different way. It uses a stable, membrane-associated topology and was capable of loading lipid antigens without forming soluble saposin-lipid antigen complexes. These findings reveal how saposins use different strategies to facilitate transfer of structurally diverse lipid antigens.

 
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