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MHC recognition in thymic development: distinct, parallel pathways for survival and lineage commitment.

D Chang1, P Valdez, T Ho

  • 1Department of Molecular and Cell Biology, University of California, Berkeley, CA 94720, USA.

Journal of Immunology (Baltimore, Md. : 1950)
|December 20, 2000
PubMed
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Mature CD8 T cells require both survival and lineage commitment signals, which are distinct pathways initiated by MHC recognition. Constitutive Notch and Bcl-2 signaling can drive CD8 T cell development even without MHC engagement.

Area of Science:

  • Immunology
  • T cell development
  • Molecular signaling

Background:

  • The precise molecular mechanisms linking T cell receptor (TCR) and major histocompatibility complex (MHC) recognition to mature CD4 and CD8 T cell development in the thymus remain unclear.
  • Understanding these pathways is crucial for dissecting T cell maturation and potential therapeutic interventions.

Purpose of the Study:

  • To investigate the essential signaling pathways required for CD8 lineage thymocyte development.
  • To determine if TCR/MHC engagement is absolutely necessary for CD8 T cell maturation.

Main Methods:

  • Utilized TCRalpha(-) mice, which lack functional TCR/MHC engagement.
  • Manipulated constitutive Notch activity and Bcl-2 expression to assess their impact on thymocyte development.
  • Monitored the up-regulation of HES1 as an indicator of Notch pathway activation.

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Main Results:

  • Constitutive Notch activity combined with constitutive Bcl-2 expression was sufficient to promote mature CD8 lineage thymocyte development in TCRalpha(-) mice.
  • Notch signaling alone could induce HES1 up-regulation, indicating thymocyte responsiveness independent of MHC recognition.
  • Survival and lineage commitment were identified as separate, parallel pathways downstream of MHC recognition.

Conclusions:

  • TCR/MHC engagement initiates distinct, parallel pathways for T cell survival and lineage commitment.
  • Notch and Bcl-2 signaling play critical roles in CD8 T cell development, partially independent of direct TCR/MHC interaction.
  • These findings provide insights into the molecular regulation of T cell maturation in the thymus.