High-Dose Abiraterone Acetate in Men With Castration Resistant Prostate Cancer

Terence W. Friedlander; Julie N. Graff; Kreshnik Zejnullahu; Archana Anantharaman; Li Zhang; Rosa Paz; Gayatri Premasekharan; Carly Russell; Yong Huang; Won Kim; Rahul R. Aggarwal; Amy M. Lin; Lawrence Fong; Joshi J. Alumkal; Tomasz M. Beer; Nima Sharifi; Mohammad Alyamani; Ryan Dittamore; Eric J. Small; Pamela L. Paris; Charles J. Ryan

doi:10.1016/j.clgc.2017.05.026

High-Dose Abiraterone Acetate in Men With Castration Resistant Prostate Cancer

Terence W. Friedlander, Julie N. Graff, Kreshnik Zejnullahu, Archana Anantharaman, Li Zhang, Rosa Paz, Gayatri Premasekharan, Carly Russell, Yong Huang, Won Kim, Rahul R. Aggarwal, Amy M. Lin, Lawrence Fong, Joshi J. Alumkal, Tomasz M. Beer, Nima Sharifi, Mohammad Alyamani, Ryan Dittamore, Eric J. Small, Pamela L. ParisCharles J. Ryan

Internal Medicine

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

18 Scopus citations

Abstract

Micro-Abstract Abiraterone acetate with prednisone prolongs progression-free and overall survival in men with advanced prostate cancer, but most eventually acquire resistance to treatment. In this study we evaluated the clinical benefit of increasing the dose of abiraterone acetate in patients who develop acquired resistance to standard-dose therapy while exploring the pharmacokinetics and pharmacodynamics of resistance. Background Abiraterone acetate (AA) inhibits androgen biosynthesis and prolongs survival in men with metastatic castration-resistant prostate cancer (mCRPC) when combined with prednisone (P). Resistance to therapy remains incompletely understood. In this open-label, single-arm, multicenter phase II study we investigated the clinical benefit of increasing the dose of AA at the time of resistance to standard-dose therapy. Patients and Methods Eligible patients had progressive mCRPC and started AA 1000 mg daily and P 5 mg twice daily. Patients who achieved any prostate-specific antigen (PSA) decline after 12 weeks of therapy continued AA with P until PSA or radiographic progression. At progression, AA was increased to 1000 mg twice daily with unchanged P dosing. Patients were monitored for response to therapy for a minimum of 12 weeks or until PSA or radiographic progression. The primary end point was PSA decline of at least 30% after 12 weeks of therapy at the increased dose of AA. Results Forty-one patients were enrolled from March 2013 through March 2014. Thirteen men experienced disease progression during standard-dose therapy and were subsequently treated with AA 1000 mg twice per day. Therapy was well tolerated. No PSA declines ≥ 30% nor radiographic responses were observed after 12 weeks of dose-escalated therapy. Higher baseline dehydroepiandrosterone levels, lower circulating tumor cell burden, and higher pharmacokinetic levels of abiraterone and abiraterone metabolites were associated with response to standard-dose therapy. Conclusion Increasing the dose of abiraterone at the time of resistance has limited clinical utility and cannot be recommended. Lower baseline circulating androgen levels and interpatient pharmacokinetic variance appear to be associated with primary resistance to AA with P.

Original language	English (US)
Pages (from-to)	733-741.e1
Journal	Clinical Genitourinary Cancer
Volume	15
Issue number	6
DOIs	https://doi.org/10.1016/j.clgc.2017.05.026
State	Published - Dec 2017

Keywords

Acquired resistance
Androgen receptor
Androgens
Hormonal therapy
Primary resistance

ASJC Scopus subject areas

Oncology
Urology

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10.1016/j.clgc.2017.05.026

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Friedlander, T. W., Graff, J. N., Zejnullahu, K., Anantharaman, A., Zhang, L., Paz, R., Premasekharan, G., Russell, C., Huang, Y., Kim, W., Aggarwal, R. R., Lin, A. M., Fong, L., Alumkal, J. J., Beer, T. M., Sharifi, N., Alyamani, M., Dittamore, R., Small, E. J., ... Ryan, C. J. (2017). High-Dose Abiraterone Acetate in Men With Castration Resistant Prostate Cancer. Clinical Genitourinary Cancer, 15(6), 733-741.e1. https://doi.org/10.1016/j.clgc.2017.05.026

Friedlander, TW, Graff, JN, Zejnullahu, K, Anantharaman, A, Zhang, L, Paz, R, Premasekharan, G, Russell, C, Huang, Y, Kim, W, Aggarwal, RR, Lin, AM, Fong, L, Alumkal, JJ, Beer, TM, Sharifi, N, Alyamani, M, Dittamore, R, Small, EJ, Paris, PL & Ryan, CJ 2017, 'High-Dose Abiraterone Acetate in Men With Castration Resistant Prostate Cancer', Clinical Genitourinary Cancer, vol. 15, no. 6, pp. 733-741.e1. https://doi.org/10.1016/j.clgc.2017.05.026

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title = "High-Dose Abiraterone Acetate in Men With Castration Resistant Prostate Cancer",

abstract = "Micro-Abstract Abiraterone acetate with prednisone prolongs progression-free and overall survival in men with advanced prostate cancer, but most eventually acquire resistance to treatment. In this study we evaluated the clinical benefit of increasing the dose of abiraterone acetate in patients who develop acquired resistance to standard-dose therapy while exploring the pharmacokinetics and pharmacodynamics of resistance. Background Abiraterone acetate (AA) inhibits androgen biosynthesis and prolongs survival in men with metastatic castration-resistant prostate cancer (mCRPC) when combined with prednisone (P). Resistance to therapy remains incompletely understood. In this open-label, single-arm, multicenter phase II study we investigated the clinical benefit of increasing the dose of AA at the time of resistance to standard-dose therapy. Patients and Methods Eligible patients had progressive mCRPC and started AA 1000 mg daily and P 5 mg twice daily. Patients who achieved any prostate-specific antigen (PSA) decline after 12 weeks of therapy continued AA with P until PSA or radiographic progression. At progression, AA was increased to 1000 mg twice daily with unchanged P dosing. Patients were monitored for response to therapy for a minimum of 12 weeks or until PSA or radiographic progression. The primary end point was PSA decline of at least 30% after 12 weeks of therapy at the increased dose of AA. Results Forty-one patients were enrolled from March 2013 through March 2014. Thirteen men experienced disease progression during standard-dose therapy and were subsequently treated with AA 1000 mg twice per day. Therapy was well tolerated. No PSA declines ≥ 30% nor radiographic responses were observed after 12 weeks of dose-escalated therapy. Higher baseline dehydroepiandrosterone levels, lower circulating tumor cell burden, and higher pharmacokinetic levels of abiraterone and abiraterone metabolites were associated with response to standard-dose therapy. Conclusion Increasing the dose of abiraterone at the time of resistance has limited clinical utility and cannot be recommended. Lower baseline circulating androgen levels and interpatient pharmacokinetic variance appear to be associated with primary resistance to AA with P.",

keywords = "Acquired resistance, Androgen receptor, Androgens, Hormonal therapy, Primary resistance",

author = "Friedlander, {Terence W.} and Graff, {Julie N.} and Kreshnik Zejnullahu and Archana Anantharaman and Li Zhang and Rosa Paz and Gayatri Premasekharan and Carly Russell and Yong Huang and Won Kim and Aggarwal, {Rahul R.} and Lin, {Amy M.} and Lawrence Fong and Alumkal, {Joshi J.} and Beer, {Tomasz M.} and Nima Sharifi and Mohammad Alyamani and Ryan Dittamore and Small, {Eric J.} and Paris, {Pamela L.} and Ryan, {Charles J.}",

note = "Publisher Copyright: {\textcopyright} 2017 Elsevier Inc.",

year = "2017",

month = dec,

doi = "10.1016/j.clgc.2017.05.026",

language = "English (US)",

volume = "15",

pages = "733--741.e1",

journal = "Clinical Genitourinary Cancer",

issn = "1558-7673",

publisher = "Elsevier",

number = "6",

}

TY - JOUR

T1 - High-Dose Abiraterone Acetate in Men With Castration Resistant Prostate Cancer

AU - Friedlander, Terence W.

AU - Graff, Julie N.

AU - Zejnullahu, Kreshnik

AU - Anantharaman, Archana

AU - Zhang, Li

AU - Paz, Rosa

AU - Premasekharan, Gayatri

AU - Russell, Carly

AU - Huang, Yong

AU - Kim, Won

AU - Aggarwal, Rahul R.

AU - Lin, Amy M.

AU - Fong, Lawrence

AU - Alumkal, Joshi J.

AU - Beer, Tomasz M.

AU - Sharifi, Nima

AU - Alyamani, Mohammad

AU - Dittamore, Ryan

AU - Small, Eric J.

AU - Paris, Pamela L.

AU - Ryan, Charles J.

PY - 2017/12

Y1 - 2017/12

N2 - Micro-Abstract Abiraterone acetate with prednisone prolongs progression-free and overall survival in men with advanced prostate cancer, but most eventually acquire resistance to treatment. In this study we evaluated the clinical benefit of increasing the dose of abiraterone acetate in patients who develop acquired resistance to standard-dose therapy while exploring the pharmacokinetics and pharmacodynamics of resistance. Background Abiraterone acetate (AA) inhibits androgen biosynthesis and prolongs survival in men with metastatic castration-resistant prostate cancer (mCRPC) when combined with prednisone (P). Resistance to therapy remains incompletely understood. In this open-label, single-arm, multicenter phase II study we investigated the clinical benefit of increasing the dose of AA at the time of resistance to standard-dose therapy. Patients and Methods Eligible patients had progressive mCRPC and started AA 1000 mg daily and P 5 mg twice daily. Patients who achieved any prostate-specific antigen (PSA) decline after 12 weeks of therapy continued AA with P until PSA or radiographic progression. At progression, AA was increased to 1000 mg twice daily with unchanged P dosing. Patients were monitored for response to therapy for a minimum of 12 weeks or until PSA or radiographic progression. The primary end point was PSA decline of at least 30% after 12 weeks of therapy at the increased dose of AA. Results Forty-one patients were enrolled from March 2013 through March 2014. Thirteen men experienced disease progression during standard-dose therapy and were subsequently treated with AA 1000 mg twice per day. Therapy was well tolerated. No PSA declines ≥ 30% nor radiographic responses were observed after 12 weeks of dose-escalated therapy. Higher baseline dehydroepiandrosterone levels, lower circulating tumor cell burden, and higher pharmacokinetic levels of abiraterone and abiraterone metabolites were associated with response to standard-dose therapy. Conclusion Increasing the dose of abiraterone at the time of resistance has limited clinical utility and cannot be recommended. Lower baseline circulating androgen levels and interpatient pharmacokinetic variance appear to be associated with primary resistance to AA with P.

AB - Micro-Abstract Abiraterone acetate with prednisone prolongs progression-free and overall survival in men with advanced prostate cancer, but most eventually acquire resistance to treatment. In this study we evaluated the clinical benefit of increasing the dose of abiraterone acetate in patients who develop acquired resistance to standard-dose therapy while exploring the pharmacokinetics and pharmacodynamics of resistance. Background Abiraterone acetate (AA) inhibits androgen biosynthesis and prolongs survival in men with metastatic castration-resistant prostate cancer (mCRPC) when combined with prednisone (P). Resistance to therapy remains incompletely understood. In this open-label, single-arm, multicenter phase II study we investigated the clinical benefit of increasing the dose of AA at the time of resistance to standard-dose therapy. Patients and Methods Eligible patients had progressive mCRPC and started AA 1000 mg daily and P 5 mg twice daily. Patients who achieved any prostate-specific antigen (PSA) decline after 12 weeks of therapy continued AA with P until PSA or radiographic progression. At progression, AA was increased to 1000 mg twice daily with unchanged P dosing. Patients were monitored for response to therapy for a minimum of 12 weeks or until PSA or radiographic progression. The primary end point was PSA decline of at least 30% after 12 weeks of therapy at the increased dose of AA. Results Forty-one patients were enrolled from March 2013 through March 2014. Thirteen men experienced disease progression during standard-dose therapy and were subsequently treated with AA 1000 mg twice per day. Therapy was well tolerated. No PSA declines ≥ 30% nor radiographic responses were observed after 12 weeks of dose-escalated therapy. Higher baseline dehydroepiandrosterone levels, lower circulating tumor cell burden, and higher pharmacokinetic levels of abiraterone and abiraterone metabolites were associated with response to standard-dose therapy. Conclusion Increasing the dose of abiraterone at the time of resistance has limited clinical utility and cannot be recommended. Lower baseline circulating androgen levels and interpatient pharmacokinetic variance appear to be associated with primary resistance to AA with P.

KW - Acquired resistance

KW - Androgen receptor

KW - Androgens

KW - Hormonal therapy

KW - Primary resistance

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High-Dose Abiraterone Acetate in Men With Castration Resistant Prostate Cancer

Abstract

Keywords

ASJC Scopus subject areas

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