Natural HLA Class I Polymorphism Controls the Pathway of Antigen Presentation and Susceptibility to Viral Evasion

نویسندگان

  • Danielle Zernich
  • Anthony W. Purcell
  • Whitney A. Macdonald
  • Lars Kjer-Nielsen
  • Lauren K. Ely
  • Nihay Laham
  • Tanya Crockford
  • Nicole A. Mifsud
  • Mandvi Bharadwaj
  • Linus Chang
  • Brian D. Tait
  • Rhonda Holdsworth
  • Andrew G. Brooks
  • Stephen P. Bottomley
  • Travis Beddoe
  • Chen Au Peh
  • Jamie Rossjohn
  • James McCluskey
چکیده

HLA class I polymorphism creates diversity in epitope specificity and T cell repertoire. We show that HLA polymorphism also controls the choice of Ag presentation pathway. A single amino acid polymorphism that distinguishes HLA-B*4402 (Asp116) from B*4405 (Tyr116) permits B*4405 to constitutively acquire peptides without any detectable incorporation into the transporter associated with Ag presentation (TAP)-associated peptide loading complex even under conditions of extreme peptide starvation. This mode of peptide capture is less susceptible to viral interference than the conventional loading pathway used by HLA-B*4402 that involves assembly of class I molecules within the peptide loading complex. Thus, B*4402 and B*4405 are at opposite extremes of a natural spectrum in HLA class I dependence on the PLC for Ag presentation. These findings unveil a new layer of MHC polymorphism that affects the generic pathway of Ag loading, revealing an unsuspected evolutionary trade-off in selection for optimal HLA class I loading versus effective pathogen evasion.

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عنوان ژورنال:
  • The Journal of Experimental Medicine

دوره 200  شماره 

صفحات  -

تاریخ انتشار 2004