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Natural micropolymorphism in human leukocyte antigens provides a basis for genetic control of antigen recognition.


ABSTRACT: Human leukocyte antigen (HLA) gene polymorphism plays a critical role in protective immunity, disease susceptibility, autoimmunity, and drug hypersensitivity, yet the basis of how HLA polymorphism influences T cell receptor (TCR) recognition is unclear. We examined how a natural micropolymorphism in HLA-B44, an important and large HLA allelic family, affected antigen recognition. T cell-mediated immunity to an Epstein-Barr virus determinant (EENLLDFVRF) is enhanced when HLA-B*4405 was the presenting allotype compared with HLA-B*4402 or HLA-B*4403, each of which differ by just one amino acid. The micropolymorphism in these HLA-B44 allotypes altered the mode of binding and dynamics of the bound viral epitope. The structure of the TCR-HLA-B*4405(EENLLDFVRF) complex revealed that peptide flexibility was a critical parameter in enabling preferential engagement with HLA-B*4405 in comparison to HLA-B*4402/03. Accordingly, major histocompatibility complex (MHC) polymorphism can alter the dynamics of the peptide-MHC landscape, resulting in fine-tuning of T cell responses between closely related allotypes.

SUBMITTER: Archbold JK 

PROVIDER: S-EPMC2626662 | biostudies-literature | 2009 Jan

REPOSITORIES: biostudies-literature

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Natural micropolymorphism in human leukocyte antigens provides a basis for genetic control of antigen recognition.

Archbold Julia K JK   Macdonald Whitney A WA   Gras Stephanie S   Ely Lauren K LK   Miles John J JJ   Bell Melissa J MJ   Brennan Rebekah M RM   Beddoe Travis T   Wilce Matthew C J MC   Clements Craig S CS   Purcell Anthony W AW   McCluskey James J   Burrows Scott R SR   Rossjohn Jamie J  

The Journal of experimental medicine 20090112 1


Human leukocyte antigen (HLA) gene polymorphism plays a critical role in protective immunity, disease susceptibility, autoimmunity, and drug hypersensitivity, yet the basis of how HLA polymorphism influences T cell receptor (TCR) recognition is unclear. We examined how a natural micropolymorphism in HLA-B44, an important and large HLA allelic family, affected antigen recognition. T cell-mediated immunity to an Epstein-Barr virus determinant (EENLLDFVRF) is enhanced when HLA-B*4405 was the presen  ...[more]

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