Literature DB >> 29440397

Sex bias in MHC I-associated shaping of the adaptive immune system.

Tilman Schneider-Hohendorf1, Dennis Görlich2, Paula Savola3, Tiina Kelkka3, Satu Mustjoki3, Catharina C Gross1, Geoffrey C Owens4, Luisa Klotz1, Klaus Dornmair5, Heinz Wiendl1, Nicholas Schwab6.   

Abstract

HLA associations, T cell receptor (TCR) repertoire bias, and sex bias have independently been shown for many diseases. While some immunological differences between the sexes have been described, they do not fully explain bias in men toward many infections/cancers, and toward women in autoimmunity. Next-generation TCR variable beta chain (TCRBV) immunosequencing of 824 individuals was evaluated in a multiparametric analysis including HLA-A -B/MHC class I background, TCRBV usage, sex, age, ethnicity, and TCRBV selection/expansion dynamics. We found that HLA-associated shaping of TCRBV usage differed between the sexes. Furthermore, certain TCRBVs were selected and expanded in unison. Correlations between these TCRBV relationships and biochemical similarities in HLA-binding positions were different in CD8 T cells of patients with autoimmune diseases (multiple sclerosis and rheumatoid arthritis) compared with healthy controls. Within patients, men showed higher TCRBV relationship Spearman's rhos in relation to HLA-binding position similarities compared with women. In line with this, CD8 T cells of men with autoimmune diseases also showed higher degrees of TCRBV perturbation compared with women. Concerted selection and expansion of CD8 T cells in patients with autoimmune diseases, but especially in men, appears to be less dependent on high HLA-binding similarity than in CD4 T cells. These findings are consistent with studies attributing autoimmunity to processes of epitope spreading and expansion of low-avidity T cell clones and may have further implications for the interpretation of pathogenic mechanisms of infectious and autoimmune diseases with known HLA associations. Reanalysis of some HLA association studies, separating the data by sex, could be informative.

Entities:  

Keywords:  T cell receptor repertoire; autoimmunity; immunological sex bias; multiple sclerosis; rheumatoid arthritis

Mesh:

Year:  2018        PMID: 29440397      PMCID: PMC5834686          DOI: 10.1073/pnas.1716146115

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  64 in total

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Journal:  Science       Date:  1972-04-21       Impact factor: 47.728

Review 7.  T-cell receptor binding affinities and kinetics: impact on T-cell activity and specificity.

Authors:  Jennifer D Stone; Adam S Chervin; David M Kranz
Journal:  Immunology       Date:  2009-02       Impact factor: 7.397

Review 8.  Molecular mimicry as a mechanism of autoimmune disease.

Authors:  Matthew F Cusick; Jane E Libbey; Robert S Fujinami
Journal:  Clin Rev Allergy Immunol       Date:  2012-02       Impact factor: 8.667

9.  Genetic variation in MHC proteins is associated with T cell receptor expression biases.

Authors:  Eilon Sharon; Leah V Sibener; Alexis Battle; Hunter B Fraser; K Christopher Garcia; Jonathan K Pritchard
Journal:  Nat Genet       Date:  2016-08-01       Impact factor: 38.330

10.  High-resolution analysis of the human T-cell receptor repertoire.

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Journal:  Nat Commun       Date:  2015-09-01       Impact factor: 14.919

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7.  Evaluation of an outbred mouse model for Francisella tularensis vaccine development and testing.

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8.  Evidence for sexual conflict over major histocompatibility complex diversity in a wild songbird.

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Review 9.  Adaptive Immunity in Hypertension.

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10.  iCAT: diagnostic assessment tool of immunological history using high-throughput T-cell receptor sequencing.

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