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Publication : Conventional and Regulatory CD4+ T Cells That Share Identical TCRs Are Derived from Common Clones.

First Author  Wolf KJ Year  2016
Journal  PLoS One Volume  11
Issue  4 Pages  e0153705
PubMed ID  27100298 Mgi Jnum  J:252444
Mgi Id  MGI:6093352 Doi  10.1371/journal.pone.0153705
Citation  Wolf KJ, et al. (2016) Conventional and Regulatory CD4+ T Cells That Share Identical TCRs Are Derived from Common Clones. PLoS One 11(4):e0153705
abstractText  Results from studies comparing the diversity and specificity of the TCR repertoires expressed by conventional (Tconv) and regulatory (Treg) CD4+ T cell have varied depending on the experimental system employed. We developed a new model in which T cells express a single fixed TCRalpha chain, randomly rearranged endogenous TCRbeta chains, and a Foxp3-GFP reporter. We purified CD4+Foxp3- and CD4+Foxp3+ cells, then performed biased controlled multiplex PCR and high throughput sequencing of endogenous TCRbeta chains. We identified >7,000 different TCRbeta sequences in the periphery of 5 individual mice. On average, ~12% of TCR sequences were expressed by both conventional and regulatory populations within individual mice. The CD4+ T cells that expressed shared TCR sequences were present at higher frequencies compared to T cells expressing non-shared TCRs. Furthermore, nearly all (>90%) of the TCR sequences that were shared within mice were identical at the DNA sequence level, indicating that conventional and regulatory T cells that express shared TCRs are derived from common clones. Analysis of TCR repertoire overlap in the thymus reveals that a large proportion of Tconv and Treg sharing observed in the periphery is due to clonal expansion in the thymus. Together these data show that there are a limited number of TCR sequences shared between Tconv and Tregs. Also, Tconv and Tregs sharing identical TCRs are found at relatively high frequencies and are derived from common progenitors, of which a large portion are generated in the thymus.
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