Limiting dilution comparison of the repertoires of high and low responder MHC-restricted T cells

To approach the mechanism that determines Ir gene-controlled high or low responsiveness to whole proteins, such as sperm whale myoglobin (SWMb), we compared the repertoires of high and low responder haplotype- restricted T cells for different myoglobin epitopes by limiting dilution frequency analysi...

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Language:English
Published: The Rockefeller University Press 1988
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Online Access:http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2188878
http://www.ncbi.nlm.nih.gov/pubmed/2450949
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spelling ftpubmed:oai:pubmedcentral.nih.gov:2188878 2023-05-15T18:26:54+02:00 Limiting dilution comparison of the repertoires of high and low responder MHC-restricted T cells 1988-03-01 http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2188878 http://www.ncbi.nlm.nih.gov/pubmed/2450949 en eng The Rockefeller University Press http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2188878 http://www.ncbi.nlm.nih.gov/pubmed/2450949 Articles Text 1988 ftpubmed 2013-09-01T12:37:47Z To approach the mechanism that determines Ir gene-controlled high or low responsiveness to whole proteins, such as sperm whale myoglobin (SWMb), we compared the repertoires of high and low responder haplotype- restricted T cells for different myoglobin epitopes by limiting dilution frequency analysis. Poisson analysis was performed using long- term limiting dilution cell lines of (B10.BR [low] X B10.D2[high])F1 T cells maintained on high or low responder APCs. The cell lines were tested with SWMb peptides and fragments for T cell repertoire fine specificities and Ia restrictions. The frequency of SWMb-specific F1 T cells responsive on B10.BR (H-2k) APCs was 2.5-3.6-fold lower than on B10.D2 (H-2d) APCs. Strikingly, all of the H-2k-restricted T cells used I-Ek as a restriction element, whereas both I-Ad- and I-Ed-restricted T cells were found among the H-2d-restricted lines. The I-Ad-restricted T cells were dominant, and the majority was specific for the synthetic peptide 102-118. T cells specific for peptide 132-146, dominant in association with I-Ed, were less frequent. However, no detectable H-2k- restricted T cells were specific for either of these peptides, but instead they were specific for fragment 1-55 or peptide 59-80. Fragment 1-55 also stimulated a similar number of H-2d-restricted T cells. Therefore, the low response of F1 T cells on H-2k-presenting cells may be due to the failure to see myoglobin plus I-Ak, in particular the immunodominant site around Glu 109, in contrast to the dominant response of high responder mice (both H-2d and H-2s) focused on the I-A molecule and the site around residue Glu 109. The I-E- low responder B10 strain also failed to respond to peptide 102-118, supporting the idea that the low responder status results from a limited repertoire lacking response to 102-118 plus I-A. In those strains that respond to the immunodominant site 102-118, the frequency of T cells in the repertoire specific for this site was always considerably greater than that for other sites. These results ... Text Sperm whale PubMed Central (PMC)
institution Open Polar
collection PubMed Central (PMC)
op_collection_id ftpubmed
language English
topic Articles
spellingShingle Articles
Limiting dilution comparison of the repertoires of high and low responder MHC-restricted T cells
topic_facet Articles
description To approach the mechanism that determines Ir gene-controlled high or low responsiveness to whole proteins, such as sperm whale myoglobin (SWMb), we compared the repertoires of high and low responder haplotype- restricted T cells for different myoglobin epitopes by limiting dilution frequency analysis. Poisson analysis was performed using long- term limiting dilution cell lines of (B10.BR [low] X B10.D2[high])F1 T cells maintained on high or low responder APCs. The cell lines were tested with SWMb peptides and fragments for T cell repertoire fine specificities and Ia restrictions. The frequency of SWMb-specific F1 T cells responsive on B10.BR (H-2k) APCs was 2.5-3.6-fold lower than on B10.D2 (H-2d) APCs. Strikingly, all of the H-2k-restricted T cells used I-Ek as a restriction element, whereas both I-Ad- and I-Ed-restricted T cells were found among the H-2d-restricted lines. The I-Ad-restricted T cells were dominant, and the majority was specific for the synthetic peptide 102-118. T cells specific for peptide 132-146, dominant in association with I-Ed, were less frequent. However, no detectable H-2k- restricted T cells were specific for either of these peptides, but instead they were specific for fragment 1-55 or peptide 59-80. Fragment 1-55 also stimulated a similar number of H-2d-restricted T cells. Therefore, the low response of F1 T cells on H-2k-presenting cells may be due to the failure to see myoglobin plus I-Ak, in particular the immunodominant site around Glu 109, in contrast to the dominant response of high responder mice (both H-2d and H-2s) focused on the I-A molecule and the site around residue Glu 109. The I-E- low responder B10 strain also failed to respond to peptide 102-118, supporting the idea that the low responder status results from a limited repertoire lacking response to 102-118 plus I-A. In those strains that respond to the immunodominant site 102-118, the frequency of T cells in the repertoire specific for this site was always considerably greater than that for other sites. These results ...
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title Limiting dilution comparison of the repertoires of high and low responder MHC-restricted T cells
title_short Limiting dilution comparison of the repertoires of high and low responder MHC-restricted T cells
title_full Limiting dilution comparison of the repertoires of high and low responder MHC-restricted T cells
title_fullStr Limiting dilution comparison of the repertoires of high and low responder MHC-restricted T cells
title_full_unstemmed Limiting dilution comparison of the repertoires of high and low responder MHC-restricted T cells
title_sort limiting dilution comparison of the repertoires of high and low responder mhc-restricted t cells
publisher The Rockefeller University Press
publishDate 1988
url http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2188878
http://www.ncbi.nlm.nih.gov/pubmed/2450949
genre Sperm whale
genre_facet Sperm whale
op_relation http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2188878
http://www.ncbi.nlm.nih.gov/pubmed/2450949
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