T cell allorecognition via molecular mimicry.

نویسندگان

  • Whitney A Macdonald
  • Zhenjun Chen
  • Stephanie Gras
  • Julia K Archbold
  • Fleur E Tynan
  • Craig S Clements
  • Mandvi Bharadwaj
  • Lars Kjer-Nielsen
  • Philippa M Saunders
  • Matthew C J Wilce
  • Fran Crawford
  • Brian Stadinsky
  • David Jackson
  • Andrew G Brooks
  • Anthony W Purcell
  • John W Kappler
  • Scott R Burrows
  • Jamie Rossjohn
  • James McCluskey
چکیده

T cells often alloreact with foreign human leukocyte antigens (HLA). Here we showed the LC13 T cell receptor (TCR), selected for recognition on self-HLA-B( *)0801 bound to a viral peptide, alloreacts with B44 allotypes (HLA-B( *)4402 and HLA-B( *)4405) bound to two different allopeptides. Despite extensive polymorphism between HLA-B( *)0801, HLA-B( *)4402, and HLA-B( *)4405 and the disparate sequences of the viral and allopeptides, the LC13 TCR engaged these peptide-HLA (pHLA) complexes identically, accommodating mimicry of the viral peptide by the allopeptide. The viral and allopeptides adopted similar conformations only after TCR ligation, revealing an induced-fit mechanism of molecular mimicry. The LC13 T cells did not alloreact against HLA-B( *)4403, and the single residue polymorphism between HLA-B( *)4402 and HLA-B( *)4403 affected the plasticity of the allopeptide, revealing that molecular mimicry was associated with TCR specificity. Accordingly, molecular mimicry that is HLA and peptide dependent is a mechanism for human T cell alloreactivity between disparate cognate and allogeneic pHLA complexes.

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عنوان ژورنال:
  • Immunity

دوره 31 6  شماره 

صفحات  -

تاریخ انتشار 2009