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

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

doi:10.1172/JCI68951

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

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. KlisovicJanelle 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

Research output: Contribution to journal › Article › peer-review

193 Scopus citations

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. TKIresistant 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.

Original language	English (US)
Pages (from-to)	4144-4157
Number of pages	14
Journal	Journal of Clinical Investigation
Volume	123
Issue number	10
DOIs	https://doi.org/10.1172/JCI68951
State	Published - Oct 1 2013
Externally published	Yes

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General Medicine

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Neviani, P., Harb, J. G., Oaks, J. J., Santhanam, R., Walker, C. J., Ellis, J. J., Ferenchak, G., Dorrance, A. M., Paisie, C. A., Eiring, A. M., Ma, Y., Mao, H. C., Zhang, B., Wunderlich, M., May, P. C., Sun, C., Saddoughi, S. A., Bielawski, J., Blum, W., ... Perrotti, D. (2013). PP2A-activating drugs selectively eradicate tki-resistant chronic myeloid leukemic stem cells. Journal of Clinical Investigation, 123(10), 4144-4157. https://doi.org/10.1172/JCI68951

Neviani, P, Harb, JG, Oaks, JJ, Santhanam, R, Walker, CJ, Ellis, JJ, Ferenchak, G, Dorrance, AM, Paisie, CA, Eiring, AM, Ma, Y, Mao, HC, Zhang, B, Wunderlich, M, May, PC, Sun, C, Saddoughi, SA, Bielawski, J, Blum, W, Klisovic, RB, Solt, JA, Byrd, JC, Volinia, S, Cortes, J, Huettner, CS, Koschmieder, S, Holyoake, TL, Devine, S, Caligiuri, MA, Croce, CM, Garzon, R, Ogretmen, B, Arlinghaus, RB, Chen, CS, Bittman, R, Hokland, P, Roy, DC, Milojkovic, D, Apperley, J, Goldman, JM, Reid, A, Mulloy, JC, Bhatia, R, Marcucci, G & Perrotti, D 2013, 'PP2A-activating drugs selectively eradicate tki-resistant chronic myeloid leukemic stem cells', Journal of Clinical Investigation, vol. 123, no. 10, pp. 4144-4157. https://doi.org/10.1172/JCI68951

@article{cd9285c1b2234e569d748460a6990f2e,

title = "PP2A-activating drugs selectively eradicate tki-resistant chronic myeloid leukemic stem cells",

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. TKIresistant 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.",

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

year = "2013",

month = oct,

day = "1",

doi = "10.1172/JCI68951",

language = "English (US)",

volume = "123",

pages = "4144--4157",

journal = "Journal of Clinical Investigation",

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publisher = "The American Society for Clinical Investigation",

number = "10",

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TY - JOUR

T1 - PP2A-activating drugs selectively eradicate tki-resistant chronic myeloid leukemic stem cells

AU - Neviani, Paolo

AU - Harb, Jason G.

AU - Oaks, Joshua J.

AU - Santhanam, Ramasamy

AU - Walker, Christopher J.

AU - Ellis, Justin J.

AU - Ferenchak, Gregory

AU - Dorrance, Adrienne M.

AU - Paisie, Carolyn A.

AU - Eiring, Anna M.

AU - Ma, Yihui

AU - Mao, Hsiaoyin C.

AU - Zhang, Bin

AU - Wunderlich, Mark

AU - May, Philippa C.

AU - Sun, Chaode

AU - Saddoughi, Sahar A.

AU - Bielawski, Jacek

AU - Blum, William

AU - Klisovic, Rebecca B.

AU - Solt, Janelle A.

AU - Byrd, John C.

AU - Volinia, Stefano

AU - Cortes, Jorge

AU - Huettner, Claudia S.

AU - Koschmieder, Steffen

AU - Holyoake, Tessa L.

AU - Devine, Steven

AU - Caligiuri, Michael A.

AU - Croce, Carlo M.

AU - Garzon, Ramiro

AU - Ogretmen, Besim

AU - Arlinghaus, Ralph B.

AU - Chen, Ching Shih

AU - Bittman, Robert

AU - Hokland, Peter

AU - Roy, Denis Claude

AU - Milojkovic, Dragana

AU - Apperley, Jane

AU - Goldman, John M.

AU - Reid, Alistair

AU - Mulloy, James C.

AU - Bhatia, Ravi

AU - Marcucci, Guido

AU - Perrotti, Danilo

PY - 2013/10/1

Y1 - 2013/10/1

N2 - 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. TKIresistant 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.

AB - 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. TKIresistant 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.

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AN - SCOPUS:84885085996

SN - 0021-9738

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SP - 4144

EP - 4157

JO - Journal of Clinical Investigation

JF - Journal of Clinical Investigation

IS - 10

ER -

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

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