Limitations in plasticity of the T-cell receptor repertoire.

How constrained is T-cell recognition? Is a truncated T-cell receptor (TCR) repertoire, missing half of its V beta components (where V indicates variable), still broad enough to produce an antigen-specific T-cell response to all determinants? These questions can be answered for certain T-cell antige...

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Main Authors: Nanda, N K, Apple, R, Sercarz, E
Format: Text
Language:English
Published: 1991
Subjects:
Research Article
Sperm whale
Online Access:http://www.ncbi.nlm.nih.gov/pmc/articles/PMC52746
http://www.ncbi.nlm.nih.gov/pubmed/1719532
id ftpubmed:oai:pubmedcentral.nih.gov:52746
record_format openpolar
spelling ftpubmed:oai:pubmedcentral.nih.gov:52746 2023-05-15T18:26:51+02:00 Limitations in plasticity of the T-cell receptor repertoire. Nanda, N K Apple, R Sercarz, E 1991-11-01 http://www.ncbi.nlm.nih.gov/pmc/articles/PMC52746 http://www.ncbi.nlm.nih.gov/pubmed/1719532 en eng http://www.ncbi.nlm.nih.gov/pmc/articles/PMC52746 http://www.ncbi.nlm.nih.gov/pubmed/1719532 Research Article Text 1991 ftpubmed 2013-08-29T08:25:59Z How constrained is T-cell recognition? Is a truncated T-cell receptor (TCR) repertoire, missing half of its V beta components (where V indicates variable), still broad enough to produce an antigen-specific T-cell response to all determinants? These questions can be answered for certain T-cell antigenic determinants whose response in the wild type is limited to specific gene segments. Our results show that mice with such a deletion in their TCR V beta genes (V beta truncated haplotype, Va beta) are unable to respond to two antigen determinants (sperm whale myoglobin 111-121/I-Ed and myelin basic protein 1-11/I-Au) whose response in the wild type is restricted to the missing V beta (V beta 8.2 in the case of 111-121/I-Ed and V beta 8.2 and V beta 13 in the case of 1-11/I-Au) gene segments. Fundamentally, this restriction could have been attributed to another aspect of immunodominance--that a favored TCR with high affinity would dominate the response, but in its absence, a hierarchy of T cells with lesser efficiency and expressing alternate TCR V genes could take over. However, from our experiments it has become evident that there is an absolute limit to the flexibility inherent in the TCR repertoire. Since it is clear that mouse populations have many ambient deletion ligands (such as self-superantigens) that can result in the loss of multiple V beta gene segments during normal T-cell development, these deletions can have serious consequences, such as unresponsiveness to the antigen as a whole--a hole in the repertoire--if a dominant determinant of that antigen normally shows restricted TCR V beta gene usage. Text Sperm whale PubMed Central (PMC)
institution Open Polar
collection PubMed Central (PMC)
op_collection_id ftpubmed
language English
topic Research Article
spellingShingle Research Article
Nanda, N K
Apple, R
Sercarz, E
Limitations in plasticity of the T-cell receptor repertoire.
topic_facet Research Article
description How constrained is T-cell recognition? Is a truncated T-cell receptor (TCR) repertoire, missing half of its V beta components (where V indicates variable), still broad enough to produce an antigen-specific T-cell response to all determinants? These questions can be answered for certain T-cell antigenic determinants whose response in the wild type is limited to specific gene segments. Our results show that mice with such a deletion in their TCR V beta genes (V beta truncated haplotype, Va beta) are unable to respond to two antigen determinants (sperm whale myoglobin 111-121/I-Ed and myelin basic protein 1-11/I-Au) whose response in the wild type is restricted to the missing V beta (V beta 8.2 in the case of 111-121/I-Ed and V beta 8.2 and V beta 13 in the case of 1-11/I-Au) gene segments. Fundamentally, this restriction could have been attributed to another aspect of immunodominance--that a favored TCR with high affinity would dominate the response, but in its absence, a hierarchy of T cells with lesser efficiency and expressing alternate TCR V genes could take over. However, from our experiments it has become evident that there is an absolute limit to the flexibility inherent in the TCR repertoire. Since it is clear that mouse populations have many ambient deletion ligands (such as self-superantigens) that can result in the loss of multiple V beta gene segments during normal T-cell development, these deletions can have serious consequences, such as unresponsiveness to the antigen as a whole--a hole in the repertoire--if a dominant determinant of that antigen normally shows restricted TCR V beta gene usage.
format Text
author Nanda, N K
Apple, R
Sercarz, E
author_facet Nanda, N K
Apple, R
Sercarz, E
author_sort Nanda, N K
title Limitations in plasticity of the T-cell receptor repertoire.
title_short Limitations in plasticity of the T-cell receptor repertoire.
title_full Limitations in plasticity of the T-cell receptor repertoire.
title_fullStr Limitations in plasticity of the T-cell receptor repertoire.
title_full_unstemmed Limitations in plasticity of the T-cell receptor repertoire.
title_sort limitations in plasticity of the t-cell receptor repertoire.
publishDate 1991
url http://www.ncbi.nlm.nih.gov/pmc/articles/PMC52746
http://www.ncbi.nlm.nih.gov/pubmed/1719532
genre Sperm whale
genre_facet Sperm whale
op_relation http://www.ncbi.nlm.nih.gov/pmc/articles/PMC52746
http://www.ncbi.nlm.nih.gov/pubmed/1719532
_version_ 1766208826795622400

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