HES1 opposes a PTEN-dependent check on survival, differentiation, and proliferation of TCRβ-selected mouse thymocytes

GW Wong, GC Knowles, TW Mak… - Blood, The Journal …, 2012 - ashpublications.org
GW Wong, GC Knowles, TW Mak, AA Ferrando, JC Zúñiga-Pflücker
Blood, The Journal of the American Society of Hematology, 2012ashpublications.org
The developmental progression of immature thymocytes requires cooperative input from
several pathways, with Notch signals playing an indispensable role at the T-cell receptor
(TCR)–β selection checkpoint. Notch signals affect the activation of the PI3K/Akt pathway,
which is required for pTα/TCRβ (pre-TCR)–induced survival, differentiation, and proliferation
of developing αβ-lineage thymocytes. However, the molecular players responsible for the
interaction between the Notch and PI3K pathways at this critical developmental stage are …
Abstract
The developmental progression of immature thymocytes requires cooperative input from several pathways, with Notch signals playing an indispensable role at the T-cell receptor (TCR)–β selection checkpoint. Notch signals affect the activation of the PI3K/Akt pathway, which is required for pTα/TCRβ (pre-TCR)–induced survival, differentiation, and proliferation of developing αβ-lineage thymocytes. However, the molecular players responsible for the interaction between the Notch and PI3K pathways at this critical developmental stage are unknown. Here, we show that Notch induction of Hes1 is necessary to repress the PI3K/Akt pathway inhibitor, PTEN (phosphatase and tensin homolog), which in turn facilitates pre-TCR–induced differentiation. In support of this mechanism, deletion or down-regulation of Pten overcomes the Notch signaling requirement for survival and differentiation during β-selection. In addition, c-Myc is a critical target of Notch at this stage, as c-Myc expression overcomes the Notch signaling requirement for proliferation during β-selection. Collectively, our results point to HES1, via repression of PTEN, and c-Myc as critical mediators of Notch function at the β-selection checkpoint.
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