Phase i trial of the combination of flavopiridol and imatinib mesylate in patients with Bcr-Abl + hematological malignancies

Prithviraj Bose; Edward B. Perkins; Connie Honeycut; Martha D. Wellons; Tammy Stefan; James W. Jacobberger; Emmanouil Kontopodis; Jan H. Beumer; Merrill J. Egorin; Chiyo K. Imamura; W. Douglas Figg; Judith E. Karp; Omer N. Koc; Brenda W. Cooper; Selina M. Luger; A. Dimitrios Colevas; John D. Roberts; Steven Grant

doi:10.1007/s00280-012-1839-5

Phase i trial of the combination of flavopiridol and imatinib mesylate in patients with Bcr-Abl ⁺ hematological malignancies

Prithviraj Bose, Edward B. Perkins, Connie Honeycut, Martha D. Wellons, Tammy Stefan, James W. Jacobberger, Emmanouil Kontopodis, Jan H. Beumer, Merrill J. Egorin, Chiyo K. Imamura, W. Douglas Figg, Judith E. Karp, Omer N. Koc, Brenda W. Cooper, Selina M. Luger, A. Dimitrios Colevas, John D. Roberts, Steven Grant

School of Medicine

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

16 Scopus citations

Abstract

Purpose: Imatinib is an inhibitor of the Bcr-Abl tyrosine kinase; however, resistance is common. Flavopiridol, a cyclin-dependent kinase (CDK) inhibitor, down-regulates short-lived anti-apoptotic proteins via inhibition of transcription. In preclinical studies, flavopiridol synergizes with imatinib to induce apoptosis. We investigated this novel combination regimen in patients with Bcr-Abl ⁺ malignancies. Methods: In a phase I dose-escalation study, imatinib was administered orally daily, and flavopiridol by 1 h intravenous infusion weekly for 3 weeks every 4 weeks. Adults with chronic myelogenous leukemia or Philadelphia chromosome- positive acute leukemia were eligible. Patients were divided into two strata based on peripheral blood and bone marrow blast counts. The primary objective was to identify the recommended phase II doses for the combination. Correlative pharmacokinetic and pharmacodynamic studies were also performed. Results: A total of 21 patients received study treatment. Four dose levels were evaluated before the study was closed following the approval of the second-generation Bcr-Abl tyrosine kinase inhibitors (TKIs). Five patients responded, including four sustained responses. Four patients had stable disease. All but one responder, and all patients with stable disease had previously been treated with imatinib. One patient had a complete response sustained for 30 months. Changes in expression of phospho-Bcr/Abl, -Stat5, and Mcl-1 were monitored. No major pharmacokinetic interaction was observed. Conclusions: This is the first study to evaluate the combination of a CDK inhibitor and a TKI in humans. The combination of flavopiridol and imatinib is tolerable and produces encouraging responses, including in some patients with imatinib-resistant disease.

Original language	English (US)
Pages (from-to)	1657-1667
Number of pages	11
Journal	Cancer Chemotherapy and Pharmacology
Volume	69
Issue number	6
DOIs	https://doi.org/10.1007/s00280-012-1839-5
State	Published - Jun 2012

Keywords

Alvocidib
Bcr-Abl
CDK inhibitor
Cyclin-dependent kinase inhibitor
Flavopiridol
Imatinib
Tyrosine kinase inhibitor

ASJC Scopus subject areas

Oncology
Toxicology
Pharmacology
Cancer Research
Pharmacology (medical)

Access to Document

10.1007/s00280-012-1839-5

Cite this

Bose, P., Perkins, E. B., Honeycut, C., Wellons, M. D., Stefan, T., Jacobberger, J. W., Kontopodis, E., Beumer, J. H., Egorin, M. J., Imamura, C. K., Figg, W. D., Karp, J. E., Koc, O. N., Cooper, B. W., Luger, S. M., Colevas, A. D., Roberts, J. D., & Grant, S. (2012). Phase i trial of the combination of flavopiridol and imatinib mesylate in patients with Bcr-Abl ⁺ hematological malignancies. Cancer Chemotherapy and Pharmacology, 69(6), 1657-1667. https://doi.org/10.1007/s00280-012-1839-5

Bose, P, Perkins, EB, Honeycut, C, Wellons, MD, Stefan, T, Jacobberger, JW, Kontopodis, E, Beumer, JH, Egorin, MJ, Imamura, CK, Figg, WD, Karp, JE, Koc, ON, Cooper, BW, Luger, SM, Colevas, AD, Roberts, JD & Grant, S 2012, 'Phase i trial of the combination of flavopiridol and imatinib mesylate in patients with Bcr-Abl ⁺ hematological malignancies', Cancer Chemotherapy and Pharmacology, vol. 69, no. 6, pp. 1657-1667. https://doi.org/10.1007/s00280-012-1839-5

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title = "Phase i trial of the combination of flavopiridol and imatinib mesylate in patients with Bcr-Abl + hematological malignancies",

abstract = "Purpose: Imatinib is an inhibitor of the Bcr-Abl tyrosine kinase; however, resistance is common. Flavopiridol, a cyclin-dependent kinase (CDK) inhibitor, down-regulates short-lived anti-apoptotic proteins via inhibition of transcription. In preclinical studies, flavopiridol synergizes with imatinib to induce apoptosis. We investigated this novel combination regimen in patients with Bcr-Abl + malignancies. Methods: In a phase I dose-escalation study, imatinib was administered orally daily, and flavopiridol by 1 h intravenous infusion weekly for 3 weeks every 4 weeks. Adults with chronic myelogenous leukemia or Philadelphia chromosome- positive acute leukemia were eligible. Patients were divided into two strata based on peripheral blood and bone marrow blast counts. The primary objective was to identify the recommended phase II doses for the combination. Correlative pharmacokinetic and pharmacodynamic studies were also performed. Results: A total of 21 patients received study treatment. Four dose levels were evaluated before the study was closed following the approval of the second-generation Bcr-Abl tyrosine kinase inhibitors (TKIs). Five patients responded, including four sustained responses. Four patients had stable disease. All but one responder, and all patients with stable disease had previously been treated with imatinib. One patient had a complete response sustained for 30 months. Changes in expression of phospho-Bcr/Abl, -Stat5, and Mcl-1 were monitored. No major pharmacokinetic interaction was observed. Conclusions: This is the first study to evaluate the combination of a CDK inhibitor and a TKI in humans. The combination of flavopiridol and imatinib is tolerable and produces encouraging responses, including in some patients with imatinib-resistant disease.",

keywords = "Alvocidib, Bcr-Abl, CDK inhibitor, Cyclin-dependent kinase inhibitor, Flavopiridol, Imatinib, Tyrosine kinase inhibitor",

author = "Prithviraj Bose and Perkins, {Edward B.} and Connie Honeycut and Wellons, {Martha D.} and Tammy Stefan and Jacobberger, {James W.} and Emmanouil Kontopodis and Beumer, {Jan H.} and Egorin, {Merrill J.} and Imamura, {Chiyo K.} and Figg, {W. Douglas} and Karp, {Judith E.} and Koc, {Omer N.} and Cooper, {Brenda W.} and Luger, {Selina M.} and Colevas, {A. Dimitrios} and Roberts, {John D.} and Steven Grant",

note = "Funding Information: Acknowledgments The authors would like to acknowledge Mary Beth Tombes, R. N., M. N. for assistance in preparing the manuscript tables, Lora Kramer for the Western blot figure, Sookyung Woo and Shawn Spencer for the manuscript and supplemental sections on flavopiridol pharmacokinetics and Brian J. Druker, Director, Knight Cancer Institute, Oregon Health and Science University, for performing correlative studies on characterization of mechanisms of resistance to imatinib in patients previously treated with imatinib. This work was supported by the following NIH grants: R01 CA93738-05, CA 100866, and R21 CA106139, NCI Cooperative Agreement U01 CA70095, Massey Cancer Center Support Grant P30 CA016059, General Clinical Research Center Grant M01 RR00065, Leukemia and Lymphoma Society of America award 6181-10, Multiple Myeloma Research Foundation, Myeloma SPORE award 1P50CA142509, and Lymphoma SPORE award 1P50CA130805. EK was supported by a scholarship from the Hellenic Society of Medical Oncology. JHB and MJE were supported by grant P30-CA47904 from the National Cancer Institute. MJE was the recipient of an American Society of Clinical Oncology Cancer Foundation Translational Research Professorship.",

year = "2012",

month = jun,

doi = "10.1007/s00280-012-1839-5",

language = "English (US)",

volume = "69",

pages = "1657--1667",

journal = "Cancer Chemotherapy and Pharmacology",

issn = "0344-5704",

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number = "6",

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TY - JOUR

T1 - Phase i trial of the combination of flavopiridol and imatinib mesylate in patients with Bcr-Abl + hematological malignancies

AU - Bose, Prithviraj

AU - Perkins, Edward B.

AU - Honeycut, Connie

AU - Wellons, Martha D.

AU - Stefan, Tammy

AU - Jacobberger, James W.

AU - Kontopodis, Emmanouil

AU - Beumer, Jan H.

AU - Egorin, Merrill J.

AU - Imamura, Chiyo K.

AU - Figg, W. Douglas

AU - Karp, Judith E.

AU - Koc, Omer N.

AU - Cooper, Brenda W.

AU - Luger, Selina M.

AU - Colevas, A. Dimitrios

AU - Roberts, John D.

AU - Grant, Steven

N1 - Funding Information: Acknowledgments The authors would like to acknowledge Mary Beth Tombes, R. N., M. N. for assistance in preparing the manuscript tables, Lora Kramer for the Western blot figure, Sookyung Woo and Shawn Spencer for the manuscript and supplemental sections on flavopiridol pharmacokinetics and Brian J. Druker, Director, Knight Cancer Institute, Oregon Health and Science University, for performing correlative studies on characterization of mechanisms of resistance to imatinib in patients previously treated with imatinib. This work was supported by the following NIH grants: R01 CA93738-05, CA 100866, and R21 CA106139, NCI Cooperative Agreement U01 CA70095, Massey Cancer Center Support Grant P30 CA016059, General Clinical Research Center Grant M01 RR00065, Leukemia and Lymphoma Society of America award 6181-10, Multiple Myeloma Research Foundation, Myeloma SPORE award 1P50CA142509, and Lymphoma SPORE award 1P50CA130805. EK was supported by a scholarship from the Hellenic Society of Medical Oncology. JHB and MJE were supported by grant P30-CA47904 from the National Cancer Institute. MJE was the recipient of an American Society of Clinical Oncology Cancer Foundation Translational Research Professorship.

PY - 2012/6

Y1 - 2012/6

N2 - Purpose: Imatinib is an inhibitor of the Bcr-Abl tyrosine kinase; however, resistance is common. Flavopiridol, a cyclin-dependent kinase (CDK) inhibitor, down-regulates short-lived anti-apoptotic proteins via inhibition of transcription. In preclinical studies, flavopiridol synergizes with imatinib to induce apoptosis. We investigated this novel combination regimen in patients with Bcr-Abl + malignancies. Methods: In a phase I dose-escalation study, imatinib was administered orally daily, and flavopiridol by 1 h intravenous infusion weekly for 3 weeks every 4 weeks. Adults with chronic myelogenous leukemia or Philadelphia chromosome- positive acute leukemia were eligible. Patients were divided into two strata based on peripheral blood and bone marrow blast counts. The primary objective was to identify the recommended phase II doses for the combination. Correlative pharmacokinetic and pharmacodynamic studies were also performed. Results: A total of 21 patients received study treatment. Four dose levels were evaluated before the study was closed following the approval of the second-generation Bcr-Abl tyrosine kinase inhibitors (TKIs). Five patients responded, including four sustained responses. Four patients had stable disease. All but one responder, and all patients with stable disease had previously been treated with imatinib. One patient had a complete response sustained for 30 months. Changes in expression of phospho-Bcr/Abl, -Stat5, and Mcl-1 were monitored. No major pharmacokinetic interaction was observed. Conclusions: This is the first study to evaluate the combination of a CDK inhibitor and a TKI in humans. The combination of flavopiridol and imatinib is tolerable and produces encouraging responses, including in some patients with imatinib-resistant disease.

AB - Purpose: Imatinib is an inhibitor of the Bcr-Abl tyrosine kinase; however, resistance is common. Flavopiridol, a cyclin-dependent kinase (CDK) inhibitor, down-regulates short-lived anti-apoptotic proteins via inhibition of transcription. In preclinical studies, flavopiridol synergizes with imatinib to induce apoptosis. We investigated this novel combination regimen in patients with Bcr-Abl + malignancies. Methods: In a phase I dose-escalation study, imatinib was administered orally daily, and flavopiridol by 1 h intravenous infusion weekly for 3 weeks every 4 weeks. Adults with chronic myelogenous leukemia or Philadelphia chromosome- positive acute leukemia were eligible. Patients were divided into two strata based on peripheral blood and bone marrow blast counts. The primary objective was to identify the recommended phase II doses for the combination. Correlative pharmacokinetic and pharmacodynamic studies were also performed. Results: A total of 21 patients received study treatment. Four dose levels were evaluated before the study was closed following the approval of the second-generation Bcr-Abl tyrosine kinase inhibitors (TKIs). Five patients responded, including four sustained responses. Four patients had stable disease. All but one responder, and all patients with stable disease had previously been treated with imatinib. One patient had a complete response sustained for 30 months. Changes in expression of phospho-Bcr/Abl, -Stat5, and Mcl-1 were monitored. No major pharmacokinetic interaction was observed. Conclusions: This is the first study to evaluate the combination of a CDK inhibitor and a TKI in humans. The combination of flavopiridol and imatinib is tolerable and produces encouraging responses, including in some patients with imatinib-resistant disease.

KW - Alvocidib

KW - Bcr-Abl

KW - CDK inhibitor

KW - Cyclin-dependent kinase inhibitor

KW - Flavopiridol

KW - Imatinib

KW - Tyrosine kinase inhibitor

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