AI Article Synopsis

  • The study investigates how T cell receptor specificity influences whether thymocytes (precursor T cells) develop into CD4+ or CD8+ T cells, revealing that MHC-I signaling leads to a unique state of CD4+8lo thymocytes during this process.
  • It shows that the transient down-regulation of the CD8 gene, rather than surface protein changes, is responsible for this CD4+8lo appearance of MHC-I-signal thymocytes.
  • These findings contradict traditional beliefs about T cell lineage commitment, suggesting that thymocytes can still become CD8+ T cells despite initial down-regulation of the CD8 gene.

Article Abstract

The mechanism by which T cell receptor specificity determines the outcome of the CD4/CD8 lineage decision in the thymus is not known. An important clue is the fact that major histocompatibility complex (MHC)-I-signaled thymocytes paradoxically appear as CD4+8lo transitional cells during their differentiation into CD8+ T cells. Lineage commitment is generally thought to occur at the CD4+8+ (double positive) stage of differentiation and to result in silencing of the opposite coreceptor gene. From this perspective, the appearance of MHC-I-signaled thymocytes as CD4+8lo cells would be due to effects on CD8 surface protein expression, not CD8 gene expression. But contrary to this perspective, this study demonstrates that MHC-I-signaled thymocytes appear as CD4+8lo cells because of transient down-regulation of CD8 gene expression, not because of changes in CD8 surface protein expression or distribution. This study also demonstrates that initial cessation of CD8 gene expression in MHC-I-signaled thymocytes is not necessarily indicative of commitment to the CD4+ T cell lineage, as such thymocytes retain the potential to differentiate into CD8+ T cells. These results challenge classical concepts of lineage commitment but fulfill predictions of the kinetic signaling model.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2193957PMC
http://dx.doi.org/10.1084/jem.20030170DOI Listing

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