PRL2 phosphatase enhances oncogenic FLT3 signaling via dephosphorylation of the E3 ubiquitin ligase CBL at tyrosine 371
Menée à l'aide de modèles murins et de données du projet "The Cancer Genome Atlas", cette étude met en évidence un mécanisme par lequel la phosphatase PRL2, via la déphosphorylation de l'ubiquitine ligase E3 CBL (Casitas B-lineage lymphoma) au niveau de la tyrosine 371, augmente la signalisation oncogène du récepteur FLT3
Acute myeloid leukemia (AML) is an aggressive blood cancer with poor prognosis. FLT3 is one of the major oncogenic receptor tyrosine kinases aberrantly activated in AML. While protein tyrosine phosphatase PRL2 is highly expressed in some subtypes of AML compared to normal human hematopoietic stem and progenitor cells (HSPCs), the mechanisms by which PRL2 promotes leukemogenesis are largely unknown. We discovered that genetic and pharmacological inhibition of PRL2 significantly reduce the burden of FLT3-ITD-driven leukemia and extend the survival of leukemic mice. Further, we found that PRL2 enhances oncogenic FLT3 signaling in leukemia cells, promoting their proliferation and survival. Mechanistically, PRL2 dephosphorylates the E3 ubiquitin ligase CBL at tyrosine 371 and attenuates CBL-mediated ubiquitination and degradation of FLT3, leading to enhanced FLT3 signaling in leukemia cells. Thus, our study reveals that PRL2 enhances oncogenic FLT3 signaling in leukemia cells through dephosphorylation of CBL and will likely establish PRL2 as a novel druggable target for AML.
Blood 2022