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Research ArticleArticle

Clinical Pharmacokinetics, Metabolism, and Drug-Drug Interaction of Carfilzomib

Zhengping Wang, Jinfu Yang, Christopher Kirk, Ying Fang, Melissa Alsina, Ashraf Badros, Kyriakos Papadopoulos, Alvin Wong, Tina Woo, Darrin Bomba, Jin Li and Jeffrey R. Infante
Drug Metabolism and Disposition January 2013, 41 (1) 230-237; DOI: https://doi.org/10.1124/dmd.112.047662
Zhengping Wang
Onyx Pharmaceuticals, South San Francisco, California (Z.W., J.Y., C.K., Y.F., A.W., T.W., D.B., J.L.); H. Lee Moffitt Cancer and Research Center, Tampa, Florida (M.A.); Greenebaum Cancer Center, University of Maryland, Baltimore, Maryland (A.B.); The START (South Texas Accelerated Research Therapeutics) Center for Cancer Care, San Antonio, Texas (K.P.); and Sarah Cannon Research Institute, Nashville, Tennessee (J.R.I.)
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Jinfu Yang
Onyx Pharmaceuticals, South San Francisco, California (Z.W., J.Y., C.K., Y.F., A.W., T.W., D.B., J.L.); H. Lee Moffitt Cancer and Research Center, Tampa, Florida (M.A.); Greenebaum Cancer Center, University of Maryland, Baltimore, Maryland (A.B.); The START (South Texas Accelerated Research Therapeutics) Center for Cancer Care, San Antonio, Texas (K.P.); and Sarah Cannon Research Institute, Nashville, Tennessee (J.R.I.)
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Christopher Kirk
Onyx Pharmaceuticals, South San Francisco, California (Z.W., J.Y., C.K., Y.F., A.W., T.W., D.B., J.L.); H. Lee Moffitt Cancer and Research Center, Tampa, Florida (M.A.); Greenebaum Cancer Center, University of Maryland, Baltimore, Maryland (A.B.); The START (South Texas Accelerated Research Therapeutics) Center for Cancer Care, San Antonio, Texas (K.P.); and Sarah Cannon Research Institute, Nashville, Tennessee (J.R.I.)
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Ying Fang
Onyx Pharmaceuticals, South San Francisco, California (Z.W., J.Y., C.K., Y.F., A.W., T.W., D.B., J.L.); H. Lee Moffitt Cancer and Research Center, Tampa, Florida (M.A.); Greenebaum Cancer Center, University of Maryland, Baltimore, Maryland (A.B.); The START (South Texas Accelerated Research Therapeutics) Center for Cancer Care, San Antonio, Texas (K.P.); and Sarah Cannon Research Institute, Nashville, Tennessee (J.R.I.)
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Melissa Alsina
Onyx Pharmaceuticals, South San Francisco, California (Z.W., J.Y., C.K., Y.F., A.W., T.W., D.B., J.L.); H. Lee Moffitt Cancer and Research Center, Tampa, Florida (M.A.); Greenebaum Cancer Center, University of Maryland, Baltimore, Maryland (A.B.); The START (South Texas Accelerated Research Therapeutics) Center for Cancer Care, San Antonio, Texas (K.P.); and Sarah Cannon Research Institute, Nashville, Tennessee (J.R.I.)
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Ashraf Badros
Onyx Pharmaceuticals, South San Francisco, California (Z.W., J.Y., C.K., Y.F., A.W., T.W., D.B., J.L.); H. Lee Moffitt Cancer and Research Center, Tampa, Florida (M.A.); Greenebaum Cancer Center, University of Maryland, Baltimore, Maryland (A.B.); The START (South Texas Accelerated Research Therapeutics) Center for Cancer Care, San Antonio, Texas (K.P.); and Sarah Cannon Research Institute, Nashville, Tennessee (J.R.I.)
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Kyriakos Papadopoulos
Onyx Pharmaceuticals, South San Francisco, California (Z.W., J.Y., C.K., Y.F., A.W., T.W., D.B., J.L.); H. Lee Moffitt Cancer and Research Center, Tampa, Florida (M.A.); Greenebaum Cancer Center, University of Maryland, Baltimore, Maryland (A.B.); The START (South Texas Accelerated Research Therapeutics) Center for Cancer Care, San Antonio, Texas (K.P.); and Sarah Cannon Research Institute, Nashville, Tennessee (J.R.I.)
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Alvin Wong
Onyx Pharmaceuticals, South San Francisco, California (Z.W., J.Y., C.K., Y.F., A.W., T.W., D.B., J.L.); H. Lee Moffitt Cancer and Research Center, Tampa, Florida (M.A.); Greenebaum Cancer Center, University of Maryland, Baltimore, Maryland (A.B.); The START (South Texas Accelerated Research Therapeutics) Center for Cancer Care, San Antonio, Texas (K.P.); and Sarah Cannon Research Institute, Nashville, Tennessee (J.R.I.)
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Tina Woo
Onyx Pharmaceuticals, South San Francisco, California (Z.W., J.Y., C.K., Y.F., A.W., T.W., D.B., J.L.); H. Lee Moffitt Cancer and Research Center, Tampa, Florida (M.A.); Greenebaum Cancer Center, University of Maryland, Baltimore, Maryland (A.B.); The START (South Texas Accelerated Research Therapeutics) Center for Cancer Care, San Antonio, Texas (K.P.); and Sarah Cannon Research Institute, Nashville, Tennessee (J.R.I.)
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Darrin Bomba
Onyx Pharmaceuticals, South San Francisco, California (Z.W., J.Y., C.K., Y.F., A.W., T.W., D.B., J.L.); H. Lee Moffitt Cancer and Research Center, Tampa, Florida (M.A.); Greenebaum Cancer Center, University of Maryland, Baltimore, Maryland (A.B.); The START (South Texas Accelerated Research Therapeutics) Center for Cancer Care, San Antonio, Texas (K.P.); and Sarah Cannon Research Institute, Nashville, Tennessee (J.R.I.)
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Jin Li
Onyx Pharmaceuticals, South San Francisco, California (Z.W., J.Y., C.K., Y.F., A.W., T.W., D.B., J.L.); H. Lee Moffitt Cancer and Research Center, Tampa, Florida (M.A.); Greenebaum Cancer Center, University of Maryland, Baltimore, Maryland (A.B.); The START (South Texas Accelerated Research Therapeutics) Center for Cancer Care, San Antonio, Texas (K.P.); and Sarah Cannon Research Institute, Nashville, Tennessee (J.R.I.)
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Jeffrey R. Infante
Onyx Pharmaceuticals, South San Francisco, California (Z.W., J.Y., C.K., Y.F., A.W., T.W., D.B., J.L.); H. Lee Moffitt Cancer and Research Center, Tampa, Florida (M.A.); Greenebaum Cancer Center, University of Maryland, Baltimore, Maryland (A.B.); The START (South Texas Accelerated Research Therapeutics) Center for Cancer Care, San Antonio, Texas (K.P.); and Sarah Cannon Research Institute, Nashville, Tennessee (J.R.I.)
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Abstract

Carfilzomib, an irreversible proteasome inhibitor, has a favorable safety profile and significant antitumor activity in patients with relapsed and refractory multiple myeloma (MM). Here we summarize the clinical pharmacokinetics (PK), metabolism, and drug-drug interaction (DDI) profile of carfilzomib. The PK of carfilzomib, infused over 2–10 minutes, was evaluated in patients with solid tumors or MM. Metabolites of carfilzomib were characterized in patient plasma and urine samples. In vitro drug metabolism and DDI studies were conducted in human liver microsomes and hepatocytes. A clinical DDI study was conducted in patients with solid tumors to evaluate the effect of carfilzomib on CYP3A activity. Plasma concentrations of carfilzomib declined rapidly and in a biphasic manner after intravenous administration. The systemic half-life was short and the systemic clearance rate was higher than hepatic blood flow. Carfilzomib was cleared largely extrahepatically via peptidase cleavage and epoxide hydrolysis. Cytochrome P450–mediated metabolism played a minor role, suggesting that coadministration of P450 inhibitors or inducers is unlikely to change its PK profile. Carfilzomib showed direct and time-dependent inhibition of CYP3A in human liver microsome preparations and exposure to carfilzomib resulted in reductions in CYP3A and 1A2 gene expression in cultured human hepatocytes. However, administration of carfilzomib did not affect the PK of midazolam in patients with solid tumors, and there were no safety signals indicative of potential drug interactions. We conclude that the rapid systemic clearance and short half-life of carfilzomib limit clinically significant DDI.

Footnotes

  • Funding for this study and manuscript was provided by Onyx Pharmaceuticals. K.P. discloses that he is an advisory board member for conflict of interest and received funding support for clinical trial conduct.

  • ↵Embedded ImageThis article has supplemental material available at dmd.aspetjournals.org.

  • dx.doi.org/10.1124/dmd.112.047662.

  • Received July 24, 2012.
  • Accepted November 1, 2012.
  • Copyright © 2013 by The American Society for Pharmacology and Experimental Therapeutics
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Drug Metabolism and Disposition: 41 (1)
Drug Metabolism and Disposition
Vol. 41, Issue 1
1 Jan 2013
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Research ArticleArticle

PK, Metabolism, and Drug-Drug Interaction of Carfilzomib

Zhengping Wang, Jinfu Yang, Christopher Kirk, Ying Fang, Melissa Alsina, Ashraf Badros, Kyriakos Papadopoulos, Alvin Wong, Tina Woo, Darrin Bomba, Jin Li and Jeffrey R. Infante
Drug Metabolism and Disposition January 1, 2013, 41 (1) 230-237; DOI: https://doi.org/10.1124/dmd.112.047662

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Research ArticleArticle

PK, Metabolism, and Drug-Drug Interaction of Carfilzomib

Zhengping Wang, Jinfu Yang, Christopher Kirk, Ying Fang, Melissa Alsina, Ashraf Badros, Kyriakos Papadopoulos, Alvin Wong, Tina Woo, Darrin Bomba, Jin Li and Jeffrey R. Infante
Drug Metabolism and Disposition January 1, 2013, 41 (1) 230-237; DOI: https://doi.org/10.1124/dmd.112.047662
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