TY - JOUR
T1 - A randomized, phase II study of pazopanib in castrate-sensitive prostate cancer
T2 - A University of Chicago Phase II Consortium/Department of Defense Prostate Cancer Clinical Trials Consortium study
AU - Ward, J. E.
AU - Karrison, T.
AU - Chatta, G.
AU - Hussain, M.
AU - Shevrin, D.
AU - Szmulewitz, R. Z.
AU - O'Donnell, P. H.
AU - Stadler, W. M.
AU - Posadas, E. M.
N1 - Funding Information:
This study was supported in part by the NCI Early Therapeutics Development with Phase II emphasis grant: N01-CM-62201 and DOD Prostate Cancer Training Award: W81XWH-08-PCRP-PRTA.
PY - 2012/3
Y1 - 2012/3
N2 - Background:Intermittent androgen suppression (IAS) is an increasingly popular treatment option for castrate-sensitive prostate cancer. On the basis of previous data with anti-angiogenic strategies, we hypothesized that pan-inhibition of the vascular endothelial growth factor receptor using pazopanib during the IAS off period would result in prolonged time to PSA failure.Methods:Men with biochemically recurrent prostate cancer, whose PSA was <0.5 ng ml -1 after 6 months of androgen deprivation therapy were randomized to pazopanib 800 mg daily or observation. The planned primary outcome was time to PSA progression >4.0 ng ml -1.Results:Thirty-seven patients were randomized. Of 18 patients randomized to pazopanib, at the time of study closure, 4 had progressive disease, 1 remained on treatment and 13 (72%) electively disenrolled, the most common reason being patient request due to grade 1/2 toxicity (8 patients). Two additional patients were removed from treatment due to adverse events. Of 19 patients randomized to observation, at the time of study closure, 4 had progressive disease, 7 remained under protocol-defined observation and 8 (42%) had disenrolled, most commonly due to non-compliance with protocol visits (3 patients). Because of high dropout rates in both arms, the study was halted.Conclusions:IAS is a treatment approach that may facilitate investigation of novel agents in the hormone-sensitive state. This trial attempted to investigate the role of antiangiogenic therapy in this setting, but encountered several barriers, including toxicities and patient non-compliance, which can make implementation of such a study difficult. Future investigative efforts in this arena should carefully consider drug toxicity and employ a design that maximizes patient convenience to reduce the dropout rate.
AB - Background:Intermittent androgen suppression (IAS) is an increasingly popular treatment option for castrate-sensitive prostate cancer. On the basis of previous data with anti-angiogenic strategies, we hypothesized that pan-inhibition of the vascular endothelial growth factor receptor using pazopanib during the IAS off period would result in prolonged time to PSA failure.Methods:Men with biochemically recurrent prostate cancer, whose PSA was <0.5 ng ml -1 after 6 months of androgen deprivation therapy were randomized to pazopanib 800 mg daily or observation. The planned primary outcome was time to PSA progression >4.0 ng ml -1.Results:Thirty-seven patients were randomized. Of 18 patients randomized to pazopanib, at the time of study closure, 4 had progressive disease, 1 remained on treatment and 13 (72%) electively disenrolled, the most common reason being patient request due to grade 1/2 toxicity (8 patients). Two additional patients were removed from treatment due to adverse events. Of 19 patients randomized to observation, at the time of study closure, 4 had progressive disease, 7 remained under protocol-defined observation and 8 (42%) had disenrolled, most commonly due to non-compliance with protocol visits (3 patients). Because of high dropout rates in both arms, the study was halted.Conclusions:IAS is a treatment approach that may facilitate investigation of novel agents in the hormone-sensitive state. This trial attempted to investigate the role of antiangiogenic therapy in this setting, but encountered several barriers, including toxicities and patient non-compliance, which can make implementation of such a study difficult. Future investigative efforts in this arena should carefully consider drug toxicity and employ a design that maximizes patient convenience to reduce the dropout rate.
KW - intermittent androgen suppression
KW - pazopanib randomized consortium trial
KW - tyrosine kinase inhibitors
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U2 - 10.1038/pcan.2011.49
DO - 10.1038/pcan.2011.49
M3 - Article
C2 - 22006050
AN - SCOPUS:84857046020
SN - 1365-7852
VL - 15
SP - 87
EP - 92
JO - Prostate Cancer and Prostatic Diseases
JF - Prostate Cancer and Prostatic Diseases
IS - 1
ER -