[PDF][PDF] TLX homeodomain oncogenes mediate T cell maturation arrest in T-ALL via interaction with ETS1 and suppression of TCRα gene expression

S Dadi, S Le Noir, D Payet-Bornet, L Lhermitte… - Cancer cell, 2012 - cell.com
S Dadi, S Le Noir, D Payet-Bornet, L Lhermitte, J Zacarias-Cabeza, J Bergeron, P Villarèse
Cancer cell, 2012cell.com
Acute lymphoblastic leukemias (ALLs) are characterized by multistep oncogenic processes
leading to cell-differentiation arrest and proliferation. Specific abrogation of maturation
blockage constitutes a promising therapeutic option in cancer, which requires precise
understanding of the underlying molecular mechanisms. We show that the cortical thymic
maturation arrest in T-lineage ALLs that overexpress TLX1 or TLX3 is due to binding of
TLX1/TLX3 to ETS1, leading to repression of T cell receptor (TCR) α enhanceosome activity …
Summary
Acute lymphoblastic leukemias (ALLs) are characterized by multistep oncogenic processes leading to cell-differentiation arrest and proliferation. Specific abrogation of maturation blockage constitutes a promising therapeutic option in cancer, which requires precise understanding of the underlying molecular mechanisms. We show that the cortical thymic maturation arrest in T-lineage ALLs that overexpress TLX1 or TLX3 is due to binding of TLX1/TLX3 to ETS1, leading to repression of T cell receptor (TCR) α enhanceosome activity and blocked TCR-Jα rearrangement. TLX1/TLX3 abrogation or enforced TCRαβ expression leads to TCRα rearrangement and apoptosis. Importantly, the autoextinction of clones carrying TCRα-driven TLX1 expression supports TLX "addiction" in TLX-positive leukemias and provides further rationale for targeted therapy based on disruption of TLX1/TLX3.
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