Targeting BCR-ABL-independent TKI resistance in chronic myeloid leukemia by mTOR and autophagy inhibition

Rebecca Mitchell; Lisa E.M. Hopcroft; Pablo Baquero; Elaine K. Allan; Kay Hewit; Daniel James; Graham Hamilton; Arunima Mukhopadhyay; Jim O'Prey; Alan Hair; Junia V. Melo; Edmond Chan; Kevin M. Ryan; Véronique Maguer-Satta; Brian J. Druker; Richard E. Clark; Subir Mitra; Pawel Herzyk; Franck E. Nicolini; Paolo Salomoni; Emma Shanks; Bruno Calabretta; Tessa L. Holyoake; G. Vignir Helgason

doi:10.1093/jnci/djx236

Targeting BCR-ABL-independent TKI resistance in chronic myeloid leukemia by mTOR and autophagy inhibition

Rebecca Mitchell, Lisa E.M. Hopcroft, Pablo Baquero, Elaine K. Allan, Kay Hewit, Daniel James, Graham Hamilton, Arunima Mukhopadhyay, Jim O'Prey, Alan Hair, Junia V. Melo, Edmond Chan, Kevin M. Ryan, Véronique Maguer-Satta, Brian J. Druker, Richard E. Clark, Subir Mitra, Pawel Herzyk, Franck E. Nicolini, Paolo SalomoniEmma Shanks, Bruno Calabretta, Tessa L. Holyoake, G. Vignir Helgason

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

74 Scopus citations

Abstract

Background: Imatinib and second-generation tyrosine kinase inhibitors (TKIs) nilotinib and dasatinib have statistically significantly improved the life expectancy of chronic myeloid leukemia (CML) patients; however, resistance to TKIs remains a major clinical challenge. Although ponatinib, a third-generation TKI, improves outcomes for patients with BCR-ABL-dependent mechanisms of resistance, including the T315I mutation, a proportion of patients may have or develop BCR-ABL-independent resistance and fail ponatinib treatment. By modeling ponatinib resistance and testing samples from these CML patients, it is hoped that an alternative drug target can be identified and inhibited with a novel compound. Methods: Two CML cell lines with acquired BCR-ABL-independent resistance were generated following culture in ponatinib. RNA sequencing and gene ontology (GO) enrichment were used to detect aberrant transcriptional response in ponatinib-resistant cells. A validated oncogene drug library was used to identify US Food and Drug Administration-approved drugs with activity against TKI-resistant cells. Validation was performed using bone marrow (BM)-derived cells from TKI-resistant patients (n = 4) and a human xenograft mouse model (n = 4-6 mice per group). All statistical tests were two-sided. Results: We show that ponatinib-resistant CML cells can acquire BCR-ABL-independent resistance mediated through alternative activation of mTOR. Following transcriptomic analysis and drug screening, we highlight mTOR inhibition as an alternative therapeutic approach in TKI-resistant CML cells. Additionally, we show that catalytic mTOR inhibitors induce autophagy and demonstrate that genetic or pharmacological inhibition of autophagy sensitizes ponatinib-resistant CML cells to death induced by mTOR inhibition in vitro (% number of colonies of control[SD], NVP-BEZ235 vs NVP-BEZ235+HCQ: 45.0[17.9]% vs 24.0[8.4]%, P = 002) and in vivo (median survival of NVP-BEZ235-vs NVP-BEZ235+HCQ-treated mice: 38.5 days vs 47.0 days, P = 04). Conclusion: Combined mTOR and autophagy inhibition may provide an attractive approach to target BCR-ABL-independent mechanism of resistance.

Original language	English (US)
Pages (from-to)	467-478
Number of pages	12
Journal	Journal of the National Cancer Institute
Volume	110
Issue number	5
DOIs	https://doi.org/10.1093/jnci/djx236
State	Published - May 1 2018

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1093/jnci/djx236

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Mitchell, R., Hopcroft, L. E. M., Baquero, P., Allan, E. K., Hewit, K., James, D., Hamilton, G., Mukhopadhyay, A., O'Prey, J., Hair, A., Melo, J. V., Chan, E., Ryan, K. M., Maguer-Satta, V., Druker, B. J., Clark, R. E., Mitra, S., Herzyk, P., Nicolini, F. E., ... Helgason, G. V. (2018). Targeting BCR-ABL-independent TKI resistance in chronic myeloid leukemia by mTOR and autophagy inhibition. Journal of the National Cancer Institute, 110(5), 467-478. https://doi.org/10.1093/jnci/djx236

Mitchell, R, Hopcroft, LEM, Baquero, P, Allan, EK, Hewit, K, James, D, Hamilton, G, Mukhopadhyay, A, O'Prey, J, Hair, A, Melo, JV, Chan, E, Ryan, KM, Maguer-Satta, V, Druker, BJ, Clark, RE, Mitra, S, Herzyk, P, Nicolini, FE, Salomoni, P, Shanks, E, Calabretta, B, Holyoake, TL & Helgason, GV 2018, 'Targeting BCR-ABL-independent TKI resistance in chronic myeloid leukemia by mTOR and autophagy inhibition', Journal of the National Cancer Institute, vol. 110, no. 5, pp. 467-478. https://doi.org/10.1093/jnci/djx236

@article{71bad4c0ba15439d84fe85e03897b044,

title = "Targeting BCR-ABL-independent TKI resistance in chronic myeloid leukemia by mTOR and autophagy inhibition",

abstract = "Background: Imatinib and second-generation tyrosine kinase inhibitors (TKIs) nilotinib and dasatinib have statistically significantly improved the life expectancy of chronic myeloid leukemia (CML) patients; however, resistance to TKIs remains a major clinical challenge. Although ponatinib, a third-generation TKI, improves outcomes for patients with BCR-ABL-dependent mechanisms of resistance, including the T315I mutation, a proportion of patients may have or develop BCR-ABL-independent resistance and fail ponatinib treatment. By modeling ponatinib resistance and testing samples from these CML patients, it is hoped that an alternative drug target can be identified and inhibited with a novel compound. Methods: Two CML cell lines with acquired BCR-ABL-independent resistance were generated following culture in ponatinib. RNA sequencing and gene ontology (GO) enrichment were used to detect aberrant transcriptional response in ponatinib-resistant cells. A validated oncogene drug library was used to identify US Food and Drug Administration-approved drugs with activity against TKI-resistant cells. Validation was performed using bone marrow (BM)-derived cells from TKI-resistant patients (n = 4) and a human xenograft mouse model (n = 4-6 mice per group). All statistical tests were two-sided. Results: We show that ponatinib-resistant CML cells can acquire BCR-ABL-independent resistance mediated through alternative activation of mTOR. Following transcriptomic analysis and drug screening, we highlight mTOR inhibition as an alternative therapeutic approach in TKI-resistant CML cells. Additionally, we show that catalytic mTOR inhibitors induce autophagy and demonstrate that genetic or pharmacological inhibition of autophagy sensitizes ponatinib-resistant CML cells to death induced by mTOR inhibition in vitro (% number of colonies of control[SD], NVP-BEZ235 vs NVP-BEZ235+HCQ: 45.0[17.9]% vs 24.0[8.4]%, P = 002) and in vivo (median survival of NVP-BEZ235-vs NVP-BEZ235+HCQ-treated mice: 38.5 days vs 47.0 days, P = 04). Conclusion: Combined mTOR and autophagy inhibition may provide an attractive approach to target BCR-ABL-independent mechanism of resistance.",

author = "Rebecca Mitchell and Hopcroft, {Lisa E.M.} and Pablo Baquero and Allan, {Elaine K.} and Kay Hewit and Daniel James and Graham Hamilton and Arunima Mukhopadhyay and Jim O'Prey and Alan Hair and Melo, {Junia V.} and Edmond Chan and Ryan, {Kevin M.} and V{\'e}ronique Maguer-Satta and Druker, {Brian J.} and Clark, {Richard E.} and Subir Mitra and Pawel Herzyk and Nicolini, {Franck E.} and Paolo Salomoni and Emma Shanks and Bruno Calabretta and Holyoake, {Tessa L.} and Helgason, {G. Vignir}",

note = "Publisher Copyright: {\textcopyright} The Author 2017. Published by Oxford University Press.",

year = "2018",

month = may,

day = "1",

doi = "10.1093/jnci/djx236",

language = "English (US)",

volume = "110",

pages = "467--478",

journal = "Journal of the National Cancer Institute",

issn = "0027-8874",

publisher = "Oxford University Press",

number = "5",

}

TY - JOUR

T1 - Targeting BCR-ABL-independent TKI resistance in chronic myeloid leukemia by mTOR and autophagy inhibition

AU - Mitchell, Rebecca

AU - Hopcroft, Lisa E.M.

AU - Baquero, Pablo

AU - Allan, Elaine K.

AU - Hewit, Kay

AU - James, Daniel

AU - Hamilton, Graham

AU - Mukhopadhyay, Arunima

AU - O'Prey, Jim

AU - Hair, Alan

AU - Melo, Junia V.

AU - Chan, Edmond

AU - Ryan, Kevin M.

AU - Maguer-Satta, Véronique

AU - Druker, Brian J.

AU - Clark, Richard E.

AU - Mitra, Subir

AU - Herzyk, Pawel

AU - Nicolini, Franck E.

AU - Salomoni, Paolo

AU - Shanks, Emma

AU - Calabretta, Bruno

AU - Holyoake, Tessa L.

AU - Helgason, G. Vignir

PY - 2018/5/1

Y1 - 2018/5/1

N2 - Background: Imatinib and second-generation tyrosine kinase inhibitors (TKIs) nilotinib and dasatinib have statistically significantly improved the life expectancy of chronic myeloid leukemia (CML) patients; however, resistance to TKIs remains a major clinical challenge. Although ponatinib, a third-generation TKI, improves outcomes for patients with BCR-ABL-dependent mechanisms of resistance, including the T315I mutation, a proportion of patients may have or develop BCR-ABL-independent resistance and fail ponatinib treatment. By modeling ponatinib resistance and testing samples from these CML patients, it is hoped that an alternative drug target can be identified and inhibited with a novel compound. Methods: Two CML cell lines with acquired BCR-ABL-independent resistance were generated following culture in ponatinib. RNA sequencing and gene ontology (GO) enrichment were used to detect aberrant transcriptional response in ponatinib-resistant cells. A validated oncogene drug library was used to identify US Food and Drug Administration-approved drugs with activity against TKI-resistant cells. Validation was performed using bone marrow (BM)-derived cells from TKI-resistant patients (n = 4) and a human xenograft mouse model (n = 4-6 mice per group). All statistical tests were two-sided. Results: We show that ponatinib-resistant CML cells can acquire BCR-ABL-independent resistance mediated through alternative activation of mTOR. Following transcriptomic analysis and drug screening, we highlight mTOR inhibition as an alternative therapeutic approach in TKI-resistant CML cells. Additionally, we show that catalytic mTOR inhibitors induce autophagy and demonstrate that genetic or pharmacological inhibition of autophagy sensitizes ponatinib-resistant CML cells to death induced by mTOR inhibition in vitro (% number of colonies of control[SD], NVP-BEZ235 vs NVP-BEZ235+HCQ: 45.0[17.9]% vs 24.0[8.4]%, P = 002) and in vivo (median survival of NVP-BEZ235-vs NVP-BEZ235+HCQ-treated mice: 38.5 days vs 47.0 days, P = 04). Conclusion: Combined mTOR and autophagy inhibition may provide an attractive approach to target BCR-ABL-independent mechanism of resistance.

AB - Background: Imatinib and second-generation tyrosine kinase inhibitors (TKIs) nilotinib and dasatinib have statistically significantly improved the life expectancy of chronic myeloid leukemia (CML) patients; however, resistance to TKIs remains a major clinical challenge. Although ponatinib, a third-generation TKI, improves outcomes for patients with BCR-ABL-dependent mechanisms of resistance, including the T315I mutation, a proportion of patients may have or develop BCR-ABL-independent resistance and fail ponatinib treatment. By modeling ponatinib resistance and testing samples from these CML patients, it is hoped that an alternative drug target can be identified and inhibited with a novel compound. Methods: Two CML cell lines with acquired BCR-ABL-independent resistance were generated following culture in ponatinib. RNA sequencing and gene ontology (GO) enrichment were used to detect aberrant transcriptional response in ponatinib-resistant cells. A validated oncogene drug library was used to identify US Food and Drug Administration-approved drugs with activity against TKI-resistant cells. Validation was performed using bone marrow (BM)-derived cells from TKI-resistant patients (n = 4) and a human xenograft mouse model (n = 4-6 mice per group). All statistical tests were two-sided. Results: We show that ponatinib-resistant CML cells can acquire BCR-ABL-independent resistance mediated through alternative activation of mTOR. Following transcriptomic analysis and drug screening, we highlight mTOR inhibition as an alternative therapeutic approach in TKI-resistant CML cells. Additionally, we show that catalytic mTOR inhibitors induce autophagy and demonstrate that genetic or pharmacological inhibition of autophagy sensitizes ponatinib-resistant CML cells to death induced by mTOR inhibition in vitro (% number of colonies of control[SD], NVP-BEZ235 vs NVP-BEZ235+HCQ: 45.0[17.9]% vs 24.0[8.4]%, P = 002) and in vivo (median survival of NVP-BEZ235-vs NVP-BEZ235+HCQ-treated mice: 38.5 days vs 47.0 days, P = 04). Conclusion: Combined mTOR and autophagy inhibition may provide an attractive approach to target BCR-ABL-independent mechanism of resistance.

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UR - http://www.scopus.com/inward/citedby.url?scp=85052853561&partnerID=8YFLogxK

U2 - 10.1093/jnci/djx236

DO - 10.1093/jnci/djx236

M3 - Article

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AN - SCOPUS:85052853561

SN - 0027-8874

VL - 110

SP - 467

EP - 478

JO - Journal of the National Cancer Institute

JF - Journal of the National Cancer Institute

IS - 5

ER -

Targeting BCR-ABL-independent TKI resistance in chronic myeloid leukemia by mTOR and autophagy inhibition

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