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Polymorphism ofTcrb andTcrg genes in Biozzi mice: Segregation analysis of a newTcrg haplotype with antibody responsiveness
Authors:Laurent Vidard  Thierry Roger  Ghislaine Pham  Jacques Couderc  Yolande Bouthillier  Jean-Claude Mevel  Denise Mouton  Michel Seman
Institution:(1) Service d'Immunogénétique, Section de Biologie, Institut Curie, 26 rue d'Ulm, F-75231 Paris Cedex 05, France;(2) Laboratoire d'Innnunodifférenciation, Institut Jacques Monod, CNRS-Université Paris 7, Tour 43, 2 place Jussieu, F-75251 Paris Cedex 05, France
Abstract:Tcrb andTcrg gene polymorphism was investigated in high (H) and low (L) responder Biozzi mice from selection I, II, and GS by Southern blot analysis with appropriateV andC probes. No polymorphism of theTcrb haplotype was detected between H and L mice in all selections which were all found to be of the BALB/c type. The H-I and H-II g genotype was of BALB/c and DBA/2 type, respectively. In contrast, a newTcrg haplotype shared by L-I and L-II mice was identified and characterized by Cgamma1, 2, 3, Cgamma4, Vgamma1, 2, 3, Vgamma5, and Vgamma6 restriction fragment length polymorphisms (RFLPs).Tcrg genotypes were not fixed in the GS selection and two additional new haplotypes were identified in two L-GS mice. An attempt was made to correlate the L-Ig genotype with the low responder status by analyzingg haplotypes among highest and lowest responder (H-1 x L-I)F2 hybrids immunized with sheep red blood cells (SRBC). No correlation was found in this segregation study, whereas a highly significant one was established with theH-2 haplotype, a locus already known to participate in the genetic control of H-I/L-I difference. The lack of correlation between SRBC response and theTcrg genotype was consistent with the heterogenousg haplotypes found in mice of the GS selection. Together, the present results suggest that H and L mice have the sameTcrab potential repertoire and that T-cell receptor (Tcr) genes cannot be considered as immune response genes in this model. Our results also indicate that the F2 segregation analysis, given a polymorphic gene, is suitable for an investigation of its immune response functions.
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