Natural Polymorphisms in Tap2 Influence Negative Selection and CD4 : CD8 Lineage Commitment in the Rat

,; Aitman, Timothy J; Baud, Amelie; Ekman, Diana; Fernández-Teruel, Alberto; Flint, Jonathan; Gillett, Alan; Haag, Sabrina; Holmdahl, Rikard; Jagodic, Maja; Johannesson, Martina; Lönnblom, Erik; Maratou, Klio; Mott, Richard; Norin, Ulrika; Olsson, Tomas; Stridh, Pernilla; Thordardottir, Soley; Tuncel, Jonatan; Yau, Anthony C Y; Ytterberg, A Jimmy; Zubarev, Roman A

Natural Polymorphisms in Tap2 Influence Negative Selection and CD4 : CD8 Lineage Commitment in the Rat

Authors: ,
Timothy J Aitman
Amelie Baud
Diana Ekman
Alberto Fernández-Teruel
Jonathan Flint
Alan Gillett
Sabrina Haag
Rikard Holmdahl
Maja Jagodic
Martina Johannesson
Erik Lönnblom
Klio Maratou
Richard Mott
Ulrika Norin
Tomas Olsson
Pernilla Stridh
Soley Thordardottir
Jonatan Tuncel
Anthony C Y Yau
A Jimmy Ytterberg
Roman A Zubarev
Publication date: 1 January 2014
Publisher: 'Public Library of Science (PLoS)'
Doi

Abstract

Contains fulltext : 136368.pdf (publisher's version ) (Open Access)Genetic variation in the major histocompatibility complex (MHC) affects CD4ratioCD8 lineage commitment and MHC expression. However, the contribution of specific genes in this gene-dense region has not yet been resolved. Nor has it been established whether the same genes regulate MHC expression and T cell selection. Here, we assessed the impact of natural genetic variation on MHC expression and CD4ratioCD8 lineage commitment using two genetic models in the rat. First, we mapped Quantitative Trait Loci (QTLs) associated with variation in MHC class I and II protein expression and the CD4ratioCD8 T cell ratio in outbred Heterogeneous Stock rats. We identified 10 QTLs across the genome and found that QTLs for the individual traits colocalized within a region spanning the MHC. To identify the genes underlying these overlapping QTLs, we generated a large panel of MHC-recombinant congenic strains, and refined the QTLs to two adjacent intervals of approximately 0.25 Mb in the MHC-I and II regions, respectively. An interaction between these intervals affected MHC class I expression as well as negative selection and lineage commitment of CD8 single-positive (SP) thymocytes. We mapped this effect to the transporter associated with antigen processing 2 (Tap2) in the MHC-II region and the classical MHC class I gene(s) (RT1-A) in the MHC-I region. This interaction was revealed by a recombination between RT1-A and Tap2, which occurred in 0.2% of the rats. Variants of Tap2 have previously been shown to influence the antigenicity of MHC class I molecules by altering the MHC class I ligandome. Our results show that a restricted peptide repertoire on MHC class I molecules leads to reduced negative selection of CD8SP cells. To our knowledge, this is the first study showing how a recombination between natural alleles of genes in the MHC influences lineage commitment of T cells