1. Comprehensive analysis of structural and sequencing data reveals almost unconstrained chain pairing in TCRαβ complex
- Author
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Dmitrii S. Shcherbinin, Mikhail Shugay, and Vlad A. Belousov
- Subjects
0301 basic medicine ,Physiology ,Protein Conformation ,Receptors, Antigen, T-Cell, alpha-beta ,Antigen Processing and Recognition ,Immune Receptors ,Biochemistry ,Major Histocompatibility Complex ,White Blood Cells ,Database and Informatics Methods ,Mice ,0302 clinical medicine ,Chain (algebraic topology) ,Animal Cells ,Immune Physiology ,Medicine and Health Sciences ,Amino Acids ,Biology (General) ,Databases, Protein ,chemistry.chemical_classification ,Immune System Proteins ,Ecology ,biology ,T Cells ,Chemistry ,Repertoire ,Amino acid ,Order (biology) ,Computational Theory and Mathematics ,Modeling and Simulation ,Amino Acid Analysis ,Cellular Types ,Sequence Analysis ,Research Article ,Signal Transduction ,Bioinformatics ,Sequence analysis ,QH301-705.5 ,Immune Cells ,Sequencing data ,Immunology ,Sequence Databases ,Computational biology ,Research and Analysis Methods ,Major histocompatibility complex ,03 medical and health sciences ,Cellular and Molecular Neuroscience ,Antigen ,Genetics ,Animals ,Humans ,Antigens ,Molecular Biology Techniques ,Molecular Biology ,Ecology, Evolution, Behavior and Systematics ,Molecular Biology Assays and Analysis Techniques ,Blood Cells ,T-cell receptor ,Biology and Life Sciences ,Proteins ,Computational Biology ,Cooperative binding ,Cell Biology ,T Cell Receptors ,Biological Databases ,030104 developmental biology ,Pairing ,biology.protein ,Clinical Immunology ,Clinical Medicine ,030217 neurology & neurosurgery - Abstract
Antigen recognition by T-cells is guided by the T-cell receptor (TCR) heterodimer formed by α and β chains. A huge diversity of TCR sequences should be maintained by the immune system in order to be able to mount an effective response towards foreign pathogens, so, due to cooperative binding of α and β chains to the pathogen, any constraints on chain pairing can have a profound effect on immune repertoire structure, diversity and antigen specificity. By integrating available structural data and paired chain sequencing results we were able to show that there are almost no constraints on pairing in TCRαβ complexes, allowing naive T-cell repertoire to reach the highest possible diversity. Additional analysis reveals that the specific choice of contacting amino acids can still have a profound effect on complex conformation. Moreover, antigen-driven selection can distort the uniform landscape of chain pairing, while small, yet significant, differences in the pairing can be attributed to various specialized T-cell subsets such as MAIT and iNKT T-cells, as well as other TCR sets specific to certain antigens., Author summary In the present paper we study chain pairing preferences in the T-cell receptor (TCR) heterodimer complex. The TCR molecule is formed by α and β chains and binding of both of these chains to an antigen presented by the major histocompatibility complex (MHC) molecule is required in order to trigger an immune response against foreign pathogens and neoantigens. We show that chain pairing in the TCR complex is nearly random ensuring a highly diverse set of TCRs required for recognition of a vast set of antigens. Our results also show that chain pairing preferences can nevertheless influence TCR complex geometry and biases in TCR chain pairing can be used to identify antigen-driven selection or selection towards specialized subsets of T-cells such as mucosal-associated and natural killer invariant T-cells.
- Published
- 2020