PUBLIC AND PRIVATE V-BETA T-CELL RECEPTOR REPERTOIRES AGAINST HEN EGG-WHITE LYSOZYME (HEL) IN NONTRANSGENIC VERSUS HEL TRANSGENIC MICE

被引:175
|
作者
CIBOTTI, R
CABANIOLS, JP
PANNETIER, C
DELARBRE, C
VERGNON, I
KANELLOPOULOS, JM
KOURILSKY, P
机构
[1] INST PASTEUR, DEPT IMMUNOL,INSERM,U277,UNITE BIOL MOLEC GENE, BIOL MOLEC GENE LAB, F-75724 PARIS 15, FRANCE
[2] HOP PAUL BROUSSE, INSERM, U267, F-94800 VILLEJUIF, FRANCE
来源
JOURNAL OF EXPERIMENTAL MEDICINE | 1994年 / 180卷 / 03期
关键词
D O I
10.1084/jem.180.3.861
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
We have previously produced a transgenic mouse line for hen egg lysozyme (HEL), an experimental model for analyzing tolerance to self-antigens at the peptide level. We have now characterized transgenic mice with HEL blood levels below 2 ng/ml, where significant T cell proliferative responses to HEL and its immunodominant peptide were observed. This HEL-low transgenic model was chosen because it mimics physiological conditions in which autoreactive T lymphocytes, recognizing self-components expressed at very low levels, persist without inducing a break in tolerance. Furthermore, in H-2(d) mice, HEL-specific T lymphocytes are triggered by a single immunodominant region, allowing us to compare the HEL-specific T cell V beta repertoires of transgenic and nontransgenic animals against a single peptide presented as self or foreign, respectively. We found that a V beta 8.2-D beta 1-J beta 1.5 rearrangement is found in response to HEL in all nontransgenic mice, whereas this V beta-restricted response is absent in HEL-low transgenic animals. At the nucleotide level, this rearrangement results from the trimming of the genomic segments during VDJ or DJ joining, without N additions, suggesting that the dominant rearrangement is selected early during fetal or neonatal life, before the expression of terminal deoxynucleotidyl transferase. In HEL-low transgenic mice, no dominant rearrangements are found as alternatives to the one observed in normal mice. Instead, each transgenic animal uses a different set of V beta-J beta combinations in its response to the immunodominant HEL peptide. In nontransgenic mice, besides the dominant V beta 8.2-D beta 1-J beta 1.5 combination, minor V beta repertoires were found which differed in each animal and were distinct from the rearrangements used by individual transgenic mice. These findings suggest that the T cell response to an immunodominant peptide involves a ''public'' V beta repertoire found in all animals and a ''private'' one which is specific to each individual.
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页码:861 / 872
页数:12
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