Phase i studies of AZD1208, a proviral integration Moloney virus kinase inhibitor in solid and haematological cancers

Jorge Cortes; Kenji Tamura; Daniel J. Deangelo; Johann De Bono; David Lorente; Mark Minden; Geoffrey L. Uy; Hagop Kantarjian; Lisa S. Chen; Varsha Gandhi; Robert Godin; Karen Keating; Kristen McEachern; Karthick Vishwanathan; Janet Elizabeth Pease; Emma Dean

doi:10.1038/s41416-018-0082-1

Phase i studies of AZD1208, a proviral integration Moloney virus kinase inhibitor in solid and haematological cancers

Jorge Cortes, Kenji Tamura, Daniel J. Deangelo, Johann De Bono, David Lorente, Mark Minden, Geoffrey L. Uy, Hagop Kantarjian, Lisa S. Chen, Varsha Gandhi, Robert Godin, Karen Keating, Kristen McEachern, Karthick Vishwanathan, Janet Elizabeth Pease, Emma Dean

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

67 Scopus citations

Abstract

Background: Proviral integration Moloney virus (PIM) kinases (PIM1, 2 and 3) are overexpressed in several tumour types and contribute to oncogenesis. AZD1208 is a potent ATP-competitive PIM kinase inhibitor investigated in patients with recurrent or refractory acute myeloid leukaemia (AML) or advanced solid tumours. Methods: Two dose-escalation studies were performed to evaluate the safety and tolerability, and to define the maximum tolerated dose (MTD), of AZD1208 in AML and solid tumours. Secondary objectives were to evaluate the pharmacokinetics, pharmacodynamics (PD) and preliminary efficacy of AZD1208. Results: Sixty-seven patients received treatment: 32 in the AML study over a 120-900 mg dose range, and 25 in the solid tumour study over a 120-800 mg dose range. Nearly all patients (98.5%) in both studies experienced adverse events, mostly gastrointestinal (92.5%). Dose-limiting toxicities included rash, fatigue and vomiting. AZD1208 was not tolerated at 900 mg, and the protocol-defined MTD was not confirmed. AZD1208 increased CYP3A4 activity after multiple dosing, resulting in increased drug clearance. There were no clinical responses; PD analysis showed biological activity of AZD1208. Conclusions: Despite the lack of single-agent clinical efficacy with AZD1208, PIM kinase inhibition may hold potential as an anticancer treatment, perhaps in combination with other agents.

Original language	English (US)
Pages (from-to)	1425-1433
Number of pages	9
Journal	British Journal of Cancer
Volume	118
Issue number	11
DOIs	https://doi.org/10.1038/s41416-018-0082-1
State	Published - May 1 2018
Externally published	Yes

ASJC Scopus subject areas

Oncology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1038/s41416-018-0082-1

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Cortes, J., Tamura, K., Deangelo, D. J., De Bono, J., Lorente, D., Minden, M., Uy, G. L., Kantarjian, H., Chen, L. S., Gandhi, V., Godin, R., Keating, K., McEachern, K., Vishwanathan, K., Pease, J. E., & Dean, E. (2018). Phase i studies of AZD1208, a proviral integration Moloney virus kinase inhibitor in solid and haematological cancers. British Journal of Cancer, 118(11), 1425-1433. https://doi.org/10.1038/s41416-018-0082-1

Cortes, J, Tamura, K, Deangelo, DJ, De Bono, J, Lorente, D, Minden, M, Uy, GL, Kantarjian, H, Chen, LS, Gandhi, V, Godin, R, Keating, K, McEachern, K, Vishwanathan, K, Pease, JE & Dean, E 2018, 'Phase i studies of AZD1208, a proviral integration Moloney virus kinase inhibitor in solid and haematological cancers', British Journal of Cancer, vol. 118, no. 11, pp. 1425-1433. https://doi.org/10.1038/s41416-018-0082-1

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title = "Phase i studies of AZD1208, a proviral integration Moloney virus kinase inhibitor in solid and haematological cancers",

abstract = "Background: Proviral integration Moloney virus (PIM) kinases (PIM1, 2 and 3) are overexpressed in several tumour types and contribute to oncogenesis. AZD1208 is a potent ATP-competitive PIM kinase inhibitor investigated in patients with recurrent or refractory acute myeloid leukaemia (AML) or advanced solid tumours. Methods: Two dose-escalation studies were performed to evaluate the safety and tolerability, and to define the maximum tolerated dose (MTD), of AZD1208 in AML and solid tumours. Secondary objectives were to evaluate the pharmacokinetics, pharmacodynamics (PD) and preliminary efficacy of AZD1208. Results: Sixty-seven patients received treatment: 32 in the AML study over a 120-900 mg dose range, and 25 in the solid tumour study over a 120-800 mg dose range. Nearly all patients (98.5%) in both studies experienced adverse events, mostly gastrointestinal (92.5%). Dose-limiting toxicities included rash, fatigue and vomiting. AZD1208 was not tolerated at 900 mg, and the protocol-defined MTD was not confirmed. AZD1208 increased CYP3A4 activity after multiple dosing, resulting in increased drug clearance. There were no clinical responses; PD analysis showed biological activity of AZD1208. Conclusions: Despite the lack of single-agent clinical efficacy with AZD1208, PIM kinase inhibition may hold potential as an anticancer treatment, perhaps in combination with other agents.",

author = "Jorge Cortes and Kenji Tamura and Deangelo, {Daniel J.} and {De Bono}, Johann and David Lorente and Mark Minden and Uy, {Geoffrey L.} and Hagop Kantarjian and Chen, {Lisa S.} and Varsha Gandhi and Robert Godin and Karen Keating and Kristen McEachern and Karthick Vishwanathan and Pease, {Janet Elizabeth} and Emma Dean",

note = "Funding Information: Medical writing support, under the direction of the authors, was provided by Thomas Owens, PhD, of CMC CONNECT, a division of Complete Medical Communications Ltd, Macclesfield, UK, funded by AstraZeneca, Cambridge, UK, in accordance with Good Publication Practice (GPP3) guidelines. This study was funded by AstraZeneca. Funding Information: Funding: This study was funded by AstraZeneca. This work was also supported in part by Cancer Center Support Grant (CCSG) P30 CA016672 and by the Translational Research Program of the Leukemia and Lymphoma Society of America (R6011-14). Funding Information: Competing interests: J.C. has received research support from, and served as a consultant for, AstraZeneca. D.J.D. has received honoraria from AstraZeneca for participation in advisory boards. Jde.B. has served on AstraZeneca advisory boards. L.S.C. has received honoraria from AstraZeneca for participation in advisory boards. V.G. has received research support and honoraria from AstraZeneca for participation in advisory boards. R.G., K.V. and J.E.P. are employees of, and hold stock in, AstraZeneca. K.K. and K.M. are former employees of AstraZeneca. E.D. is currently employed by AstraZeneca but for the duration of the study was affiliated to The Christie NHS Foundation Trust and The University of Manchester. E.D.{\textquoteright}s former institution—The Christie NHS Foundation Trust—has received commercial income from AstraZeneca. The clinical research was supported by Experimental Cancer Medicine grant award C1467/A15578. K.T., D.L., M.M., G.L.U. and H.K. have no conflicts of interest or disclosures to declare. Publisher Copyright: {\textcopyright} 2018 The Author(s).",

year = "2018",

month = may,

day = "1",

doi = "10.1038/s41416-018-0082-1",

language = "English (US)",

volume = "118",

pages = "1425--1433",

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T1 - Phase i studies of AZD1208, a proviral integration Moloney virus kinase inhibitor in solid and haematological cancers

AU - Cortes, Jorge

AU - Tamura, Kenji

AU - Deangelo, Daniel J.

AU - De Bono, Johann

AU - Lorente, David

AU - Minden, Mark

AU - Uy, Geoffrey L.

AU - Kantarjian, Hagop

AU - Chen, Lisa S.

AU - Gandhi, Varsha

AU - Godin, Robert

AU - Keating, Karen

AU - McEachern, Kristen

AU - Vishwanathan, Karthick

AU - Pease, Janet Elizabeth

AU - Dean, Emma

N1 - Funding Information: Medical writing support, under the direction of the authors, was provided by Thomas Owens, PhD, of CMC CONNECT, a division of Complete Medical Communications Ltd, Macclesfield, UK, funded by AstraZeneca, Cambridge, UK, in accordance with Good Publication Practice (GPP3) guidelines. This study was funded by AstraZeneca. Funding Information: Funding: This study was funded by AstraZeneca. This work was also supported in part by Cancer Center Support Grant (CCSG) P30 CA016672 and by the Translational Research Program of the Leukemia and Lymphoma Society of America (R6011-14). Funding Information: Competing interests: J.C. has received research support from, and served as a consultant for, AstraZeneca. D.J.D. has received honoraria from AstraZeneca for participation in advisory boards. Jde.B. has served on AstraZeneca advisory boards. L.S.C. has received honoraria from AstraZeneca for participation in advisory boards. V.G. has received research support and honoraria from AstraZeneca for participation in advisory boards. R.G., K.V. and J.E.P. are employees of, and hold stock in, AstraZeneca. K.K. and K.M. are former employees of AstraZeneca. E.D. is currently employed by AstraZeneca but for the duration of the study was affiliated to The Christie NHS Foundation Trust and The University of Manchester. E.D.’s former institution—The Christie NHS Foundation Trust—has received commercial income from AstraZeneca. The clinical research was supported by Experimental Cancer Medicine grant award C1467/A15578. K.T., D.L., M.M., G.L.U. and H.K. have no conflicts of interest or disclosures to declare. Publisher Copyright: © 2018 The Author(s).

PY - 2018/5/1

Y1 - 2018/5/1

N2 - Background: Proviral integration Moloney virus (PIM) kinases (PIM1, 2 and 3) are overexpressed in several tumour types and contribute to oncogenesis. AZD1208 is a potent ATP-competitive PIM kinase inhibitor investigated in patients with recurrent or refractory acute myeloid leukaemia (AML) or advanced solid tumours. Methods: Two dose-escalation studies were performed to evaluate the safety and tolerability, and to define the maximum tolerated dose (MTD), of AZD1208 in AML and solid tumours. Secondary objectives were to evaluate the pharmacokinetics, pharmacodynamics (PD) and preliminary efficacy of AZD1208. Results: Sixty-seven patients received treatment: 32 in the AML study over a 120-900 mg dose range, and 25 in the solid tumour study over a 120-800 mg dose range. Nearly all patients (98.5%) in both studies experienced adverse events, mostly gastrointestinal (92.5%). Dose-limiting toxicities included rash, fatigue and vomiting. AZD1208 was not tolerated at 900 mg, and the protocol-defined MTD was not confirmed. AZD1208 increased CYP3A4 activity after multiple dosing, resulting in increased drug clearance. There were no clinical responses; PD analysis showed biological activity of AZD1208. Conclusions: Despite the lack of single-agent clinical efficacy with AZD1208, PIM kinase inhibition may hold potential as an anticancer treatment, perhaps in combination with other agents.

AB - Background: Proviral integration Moloney virus (PIM) kinases (PIM1, 2 and 3) are overexpressed in several tumour types and contribute to oncogenesis. AZD1208 is a potent ATP-competitive PIM kinase inhibitor investigated in patients with recurrent or refractory acute myeloid leukaemia (AML) or advanced solid tumours. Methods: Two dose-escalation studies were performed to evaluate the safety and tolerability, and to define the maximum tolerated dose (MTD), of AZD1208 in AML and solid tumours. Secondary objectives were to evaluate the pharmacokinetics, pharmacodynamics (PD) and preliminary efficacy of AZD1208. Results: Sixty-seven patients received treatment: 32 in the AML study over a 120-900 mg dose range, and 25 in the solid tumour study over a 120-800 mg dose range. Nearly all patients (98.5%) in both studies experienced adverse events, mostly gastrointestinal (92.5%). Dose-limiting toxicities included rash, fatigue and vomiting. AZD1208 was not tolerated at 900 mg, and the protocol-defined MTD was not confirmed. AZD1208 increased CYP3A4 activity after multiple dosing, resulting in increased drug clearance. There were no clinical responses; PD analysis showed biological activity of AZD1208. Conclusions: Despite the lack of single-agent clinical efficacy with AZD1208, PIM kinase inhibition may hold potential as an anticancer treatment, perhaps in combination with other agents.

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JO - British Journal of Cancer

JF - British Journal of Cancer

IS - 11

ER -

Phase i studies of AZD1208, a proviral integration Moloney virus kinase inhibitor in solid and haematological cancers

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