Immunological tolerance-t cells

Yael Goldfarb, Cristina Peligero-Cruz, Jakub Abramson

Research output: Chapter in Book/Report/Conference proceedingChapterpeer-review

1 Citation (Scopus)

Abstract

T lymphocytes are essential guardians against a plethora of pathogens and are thus characterized by an unprecedented diversity for antigen recognition. Their repertoire diversity is achieved by an elaborate, semirandom rearrangement of the genes encoding their respective antigen-specific receptors which inevitably generates many T cells that recognize not only foreign and potentially harmful antigens, but also the body’s own components. Therefore to deal with this problem and to prevent autoimmune destruction, the immune system has evolved a comprehensive network of several complementary mechanisms that are guided by four major principles to ensure tolerance to the body’s own antigens: (1) complete physical elimination of the self-reactive T-cell clone from the repertoire (clonal deletion), (2) conversion of the self-reactive clone into a tolerogenic and/or harmless T-cell subtype (anergy, phenotype skewing), (3) prevention of T-cell encounter with its specific self-antigen in the immune periphery (ignorance, antigen sequestering), and (4) prevention of clonal expansion or reactivation upon self-antigen (re)encounter (immunosuppression, T-cell intrinsic inhibitory mechanisms). In this chapter, we shall try to provide a fresh look at these key concepts and mechanisms underlying the establishment, maintenance, and breakdown of T-cell tolerance to the body’s own components.

Original languageEnglish
Title of host publicationThe Autoimmune Diseases
PublisherElsevier
Chapter5
Pages65-90
Number of pages26
Edition6
ISBN (Electronic)9780128121023
ISBN (Print)9780128122426
DOIs
Publication statusPublished - 1 Jan 2019

Bibliographical note

We would like to thank members of the Abramson lab and Prof. Eystein S. Husebye for their critical reading of this manuscript. J.A. is an incumbent of the Dr. Celia Zwillenberg-Fridman and Dr. Lutz Fridman Career Development Chair. Research in the Abramson lab is kindly supported by European Research Council Consolidator grant (ERC-2016-CoG-724821), Israel Science Foundation (1796/16 and 722/14), the Sy Syms Foundation; US–Israel Binational Foundation, Maurice and Vivienne Wohl Charitable Foundation; Goodman Family Charitable Lead Annuity Trust; Ruth and Samuel David Gameroff Family Foundation.

Publisher Copyright:
© 2020 Elsevier Inc. All rights reserved.

All Science Journal Classification (ASJC) codes

  • General Medicine
  • General Immunology and Microbiology

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