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  • PP2A-activating drugs selectively eradicate TKI-resistant chronic myeloid leukemic stem cells.

PP2A-activating drugs selectively eradicate TKI-resistant chronic myeloid leukemic stem cells.

The Journal of clinical investigation (2013-09-04)
Paolo Neviani, Jason G Harb, Joshua J Oaks, Ramasamy Santhanam, Christopher J Walker, Justin J Ellis, Gregory Ferenchak, Adrienne M Dorrance, Carolyn A Paisie, Anna M Eiring, Yihui Ma, Hsiaoyin C Mao, Bin Zhang, Mark Wunderlich, Philippa C May, Chaode Sun, Sahar A Saddoughi, Jacek Bielawski, William Blum, Rebecca B Klisovic, Janelle A Solt, John C Byrd, Stefano Volinia, Jorge Cortes, Claudia S Huettner, Steffen Koschmieder, Tessa L Holyoake, Steven Devine, Michael A Caligiuri, Carlo M Croce, Ramiro Garzon, Besim Ogretmen, Ralph B Arlinghaus, Ching-Shih Chen, Robert Bittman, Peter Hokland, Denis-Claude Roy, Dragana Milojkovic, Jane Apperley, John M Goldman, Alistair Reid, James C Mulloy, Ravi Bhatia, Guido Marcucci, Danilo Perrotti
ABSTRACT

The success of tyrosine kinase inhibitors (TKIs) in treating chronic myeloid leukemia (CML) depends on the requirement for BCR-ABL1 kinase activity in CML progenitors. However, CML quiescent HSCs are TKI resistant and represent a BCR-ABL1 kinase-independent disease reservoir. Here we have shown that persistence of leukemic HSCs in BM requires inhibition of the tumor suppressor protein phosphatase 2A (PP2A) and expression--but not activity--of the BCR-ABL1 oncogene. Examination of HSCs from CML patients and healthy individuals revealed that PP2A activity was suppressed in CML compared with normal HSCs. TKI-resistant CML quiescent HSCs showed increased levels of BCR-ABL1, but very low kinase activity. BCR-ABL1 expression, but not kinase function, was required for recruitment of JAK2, activation of a JAK2/β-catenin survival/self-renewal pathway, and inhibition of PP2A. PP2A-activating drugs (PADs) markedly reduced survival and self-renewal of CML quiescent HSCs, but not normal quiescent HSCs, through BCR-ABL1 kinase-independent and PP2A-mediated inhibition of JAK2 and β-catenin. This led to suppression of human leukemic, but not normal, HSC/progenitor survival in BM xenografts and interference with long-term maintenance of BCR-ABL1-positive HSCs in serial transplantation assays. Targeting the JAK2/PP2A/β-catenin network in quiescent HSCs with PADs (e.g., FTY720) has the potential to treat TKI-refractory CML and relieve lifelong patient dependence on TKIs.

MATERIALS
Product Number
Brand
Product Description

Sigma-Aldrich
FTY720, ≥98% (HPLC)
Sigma-Aldrich
D-Sphingosine, synthetic
Sigma-Aldrich
D-Sphingosine, ≥98.0% (TLC)