Literature DB >> 10036633

Peptide-based molecular analyses of HLA class II-associated susceptibility to autoimmune diseases.

Y Nishimura1, M Oiso, S Fujisao, T Kanai, J Kira, Y Z Chen, S Matsushita.   

Abstract

Recent advances in knowledge of crystal structures of MHC class II molecules has advanced understanding of the molecular basis for interactions between peptides and HLA class II molecules. Polymorphism of HLA class II molecules influences structures of peptides bound to HLA class II molecules. To better understand mechanisms related to particular HLA class II alleles and autoimmune diseases, it is important to identify self-peptides presented by disease-susceptible HLA class II molecules and triggering disease-causative autoreactive T cells. Autoimmune diseases occur in Caucasians, Blacks and Asians, albeit with a different incidence. In some autoimmune diseases, disease-susceptible HLA class II alleles are closely related but different, and clinical manifestations of diseases differ among ethnic groups. These phenomena strongly suggest that difference in autoimmune self-peptide(s) in the context of disease-susceptible HLA class II molecules may explain the different clinical manifestations of diseases. Therefore, a comparison among disease-susceptible HLA class II alleles, autoimmune self-peptides and clinical manifestations of autoimmune diseases in different ethnic groups would be instructive. We directed efforts to determining: (1) HLA-class II alleles specific to Asian populations and which are associated with susceptibility to autoimmune diseases, (2) binding-peptide motifs for these HLA class II molecules, and (3) self-peptides presented by susceptible HLA class II molecules to stimulate autoreactive T cells related to the development of autoimmune diseases in Asians. In this review, our related recent investigations are described and the uniqueness of HLA class II-associated autoimmune diseases in Asians is given emphasis.

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Year:  1998        PMID: 10036633     DOI: 10.3109/08830189809054404

Source DB:  PubMed          Journal:  Int Rev Immunol        ISSN: 0883-0185            Impact factor:   5.311


  2 in total

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Review 2.  Where, How, and When: Positioning Posttranslational Modification Within Type 1 Diabetes Pathogenesis.

Authors:  Rene J McLaughlin; Matthew P Spindler; Menno van Lummel; Bart O Roep
Journal:  Curr Diab Rep       Date:  2016-07       Impact factor: 4.810

  2 in total

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