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Publication : The endogenous Mtv8 locus and the immunoglobulin repertoire.

First Author  Beilinson HA Year  2024
Journal  Front Immunol Volume  15
Pages  1345467 PubMed ID  38504980
Mgi Jnum  J:346992 Mgi Id  MGI:7615429
Doi  10.3389/fimmu.2024.1345467 Citation  Beilinson HA, et al. (2024) The endogenous Mtv8 locus and the immunoglobulin repertoire. Front Immunol 15:1345467
abstractText  The vast diversity of mammalian adaptive antigen receptors allows for robust and efficient immune responses against a wide number of pathogens. The antigen receptor repertoire is built during the recombination of B and T cell receptor (BCR, TCR) loci and hypermutation of BCR loci. V(D)J recombination rearranges these antigen receptor loci, which are organized as an array of separate V, (D), and J gene segments. Transcription activation at the recombining locus leads to changes in the local three-dimensional architecture, which subsequently contributes to which gene segments are utilized for recombination. The endogenous retrovirus (ERV) mouse mammary tumor provirus 8 (Mtv8) resides on mouse chromosome 6 interposed within the large array of light chain kappa V gene segments. As ERVs contribute to changes in genomic architecture by driving high levels of transcription of neighboring genes, it was suggested that Mtv8 could influence the BCR repertoire. We generated Mtv8-deficient mice to determine if the ERV influences V(D)J recombination to test this possibility. We find that Mtv8 does not influence the BCR repertoire.
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