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Publication : Normal TCRbeta transcription and recombination in the absence of the Jbeta2-Cbeta2 intronic cis element.

First Author  Whitehurst CE Year  2001
Journal  Mol Immunol Volume  38
Issue  1 Pages  55-63
PubMed ID  11483210 Mgi Jnum  J:71207
Mgi Id  MGI:2149299 Doi  10.1016/s0161-5890(01)00031-1
Citation  Whitehurst CE, et al. (2001) Normal TCRbeta transcription and recombination in the absence of the Jbeta2-Cbeta2 intronic cis element. Mol Immunol 38(1):55-63
abstractText  The developmental regulation of antigen receptor gene transcription and recombination are mediated by cis regulatory elements. At the T cell receptor beta chain locus (TCRbeta), two DNase I hypersensitive sites within the Jbeta2-Cbeta2 intron contained binding sites for NF-kappaB and additional nuclear factors and were postulated to be involved in controlling TCRbeta transcription and V(D)J recombination. To test this possibility, we deleted these elements from the mouse genome by homologous recombination and assayed the effect on transcription of both the germline and rearranged TCRbeta locus, and on TCRbeta rearrangement in T and B lymphocytes. We found that TCRbeta transcription and V(D)J recombination and T cell development were normal in these mutant mice. Therefore, the Jbeta2-Cbeta2 intronic elements are dispensable for TCRbeta assembly and function.
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