4.6 Review Book Chapter

The Innate Biologies of Adaptive Antigen Receptors

Journal

ANNUAL REVIEW OF IMMUNOLOGY, VOL 38
Volume 38, Issue -, Pages 487-510

Publisher

ANNUAL REVIEWS
DOI: 10.1146/annurev-immunol-102819-023144

Keywords

T cell receptors; butyrophilins; superantigens; immunoglobulins; tonic signaling; preparedness

Categories

Funding

  1. Wellcome Trust (WT) [106292/Z/14/Z]
  2. Francis Crick Institute from Cancer Research UK (CRUK) [FC001093]
  3. UK Medical Research Council [FC001093]
  4. WT [FC001093]

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Nonclonal innate immune responses mediated by germ line-encoded receptors, such as Toll-like receptors or natural killer receptors, are commonly contrasted with diverse, clonotypic adaptive responses of lymphocyte antigen receptors generated by somatic recombination. However, the Variable (V) regions of antigen receptors include germ line-encoded motifs unaltered by somatic recombination, and theoretically available to mediate nonclonal, innate responses, that are independent of or largely override clonotypic responses. Recent evidence demonstrates that such responses exist, underpinning the associations of particular gamma delta T cell receptors (TCRs) with specific anatomical sites. Thus, TCR gamma delta can make innate and adaptive responses with distinct functional outcomes. Given that alpha beta T cells and B cells can also make nonclonal responses, we consider that innate responses of antigen receptor V-regions may be more widespread, for example, inducing states of preparedness from which adaptive clones are better selected. We likewise consider that potent, nonclonal T cell responses tomicrobial superantigens may reflect subversion of physiologic innate responses of TCR alpha/beta chains.

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