• Title of article

    Down-Modulation of CD8 β-Chain in Response to an Altered Peptide Ligand Enables Developing Thymocytes to Escape Negative Selection

  • Author/Authors

    John A. Barnden، نويسنده , , Megan J. and Heath، نويسنده , , William R. and Carbone، نويسنده , , Francis R.، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 1997
  • Pages
    9
  • From page
    111
  • To page
    119
  • Abstract
    Mice expressing a Kb-restricted transgenic T cell receptor (TCR) and a naturally occurring MHC class I variant molecule, Kbm8, were used to study thymic selection. The transgenic TCR was specific for the major peptide determinant from ovalbumin (OVA257–264), while Kbm8has a mutation that alters the position 2 binding pocket of the Kbmolecule, abolishing antigenic peptide presentation and positive selection of transgenic T cells. Peptide presentation was restored by identifying a position 2 analog peptide with Kbm8-binding capacity. In combination with Kbm8, the E2 peptide variant was capable of deleting immature double-positive thymocytes in suspension culture. Similarly, addition of exogenous E2 peptide to fetal thymic organ culture resulted in efficient deletion of double-positive thymocytes. However, there remained a population of CD8 single-positive T cells that exhibited impaired responsiveness to the antigenic peptide and lacked expression of the CD8 β-chain. These results suggest a mechanism whereby developing thymocytes bearing an αβTCR can modify their expression of the CD8 coreceptor to escape thymic deletion and achieve self-tolerance.
  • Journal title
    Cellular Immunology
  • Serial Year
    1997
  • Journal title
    Cellular Immunology
  • Record number

    1852314