Number-needed-to-treat analysis of clinical progression in patients with metastatic castration-resistant prostate cancer in the STRIVE and TERRAIN trials

Background

This analysis estimated the number needed to treat with enzalutamide versus bicalutamide to achieve one additional patient with chemotherapy-naïve metastatic castration-resistant prostate cancer who would obtain clinical benefit regarding progression-free survival, radiographic progression-free survival, or no prostate-specific antigen progression at 1 and 2 years following treatment initiation.

Methods

Clinical event rates were obtained from the STRIVE (NCT01664923) and TERRAIN (NCT01288911) trials, and the number needed to treat was the inverse of the absolute rate difference between the event rates of enzalutamide and bicalutamide. The 95% Confidence Interval of the number needed to treat was derived from the 95% Confidence Interval of the event rate difference.

Results

Using STRIVE data (patients with metastatic disease: n = 128 enzalutamide; n = 129 bicalutamide) comparing enzalutamide with bicalutamide at 1 and 2 years, the numbers needed to treat to achieve one additional patient with chemotherapy-naïve metastatic castration-resistant prostate cancer with progression-free survival were 2.0 and 2.8, respectively; with radiographic progression-free survival, 2.6 and 3.0, respectively; and without prostate-specific antigen progression, 1.8 and 2.4, respectively. Using TERRAIN data (n = 184 enzalutamide; n = 191 bicalutamide) comparing enzalutamide with bicalutamide at 1 and 2 years, the numbers needed to treat to achieve one additional patient with progression-free survival were 4.3 and 3.7, respectively; with radiographic progression-free survival, 10.0 and 2.8, respectively; and without prostate-specific antigen progression, 2.1 and 3.2, respectively.

Conclusions

The combined data from TERRAIN and STRIVE demonstrated that treating chemotherapy-naïve metastatic castration-resistant prostate cancer with enzalutamide leads to more patients without clinical progression at 1 and 2 years than with bicalutamide.

Trial registration

STRIVE (NCT01664923; registration date: August 10, 2012) and TERRAIN (NCT01288911; registration date: February 1, 2011).

Prostate cancer (PC) is the second leading cause of cancer-related deaths and the most commonly diagnosed cancer among men worldwide [1, 2]. Castration-resistant prostate cancer (CRPC) is characterized by a castrate level of testosterone and either rising prostate-specific antigen (PSA) or radiographic disease progression [3]. CRPC may account for approximately 10–20% of PC cases, with over 84% of these cases demonstrating radiographic findings of metastatic CRPC (mCRPC) [4].

Until 2010, treatment for mCRPC was largely limited to taxane chemotherapy (docetaxel) or the oral non-steroidal antiandrogen bicalutamide plus luteinizing hormone-releasing hormone (LHRH) analogs [5]. Bicalutamide is a partial androgen receptor (AR) antagonist approved by the United States Food and Drug Administration (FDA) in 1995 as a 50 mg daily tablet for the treatment of metastatic androgen-sensitive PC, in combination with an LHRH analog [5, 6]. However, bicalutamide has been frequently used to treat various stages of mCRPC as monotherapy or as combination therapy with androgen-deprivation therapy despite a void of Category 1 evidence for its use in this patient population [7]. Until recently, median overall survival, depending on symptomatology and tumor burden, was estimated to be 9–18 months for those with mCRPC [4]. However, since 2010, the approval of new treatments for mCRPC has resulted in increases in median overall survival ranging from 16 to 35 months [7, 8].

One of these new therapies is the AR antagonist enzalutamide (Xtandi®; Astellas Pharma, Inc., IL, and Medivation, Inc., CA, which was acquired by Pfizer, Inc. in September 2016), which was approved by the FDA in 2012 [9]. Enzalutamide, with an approved dose of 160 mg daily for the treatment of mCRPC [9], is shown to have a five- to eight-fold higher AR binding affinity compared to bicalutamide in a preclinical test [10]. Enzalutamide targets three aspects of the AR signaling pathway: blocking androgen binding to ARs; inhibiting nuclear translocation of ARs; and inhibiting binding of ARs to DNA [11]. In contrast to bicalutamide, enzalutamide has received a Category 1 evidence recommendation for mCRPC in multiple US clinical guidelines [7, 12, 13].

Enzalutamide and bicalutamide have been directly compared in patients with chemotherapy-naïve CRPC in two randomized clinical trials: STRIVE and TERRAIN [14, 15]. In TERRAIN, enzalutamide and bicalutamide were compared in patients with chemotherapy-naïve asymptomatic or minimally symptomatic mCRPC [15]. The primary outcome of the TERRAIN trial was significantly improved progression-free survival (PFS) in patients receiving enzalutamide compared to patients receiving bicalutamide (15.7 months vs. 5.8 months, respectively). Median radiographic PFS (rPFS) was not reached for enzalutamide and was 16.4 months for bicalutamide, and median time to PSA progression was 19.4 months and 5.8 months, respectively. The STRIVE trial compared these two therapies in chemotherapy-naïve non-metastatic CRPC patients and mCRPC patients [14]. In patients with mCRPC, the trial reported a longer median PFS with enzalutamide than with bicalutamide (16.5 months vs. 5.5 months, respectively), and median rPFS was not reached with enzalutamide and was 8.3 months with bicalutamide. Median time to PSA progression was 24.9 months with enzalutamide and 5.7 months with bicalutamide. With respect to the incidence of serious adverse events, in the TERRAIN trial, patients treated with enzalutamide were more likely to experience a serious adverse event than patients treated with bicalutamide (31% vs. 23%, respectively); however, in the STRIVE trial, the rates were similar between the two treatment groups (29% vs. 28%, respectively) [14, 15].

The outcomes data from TERRAIN and STRIVE can be used to generate additional comparative efficacy evidence for enzalutamide versus bicalutamide that is applicable to mCRPC clinical practice and treatment decision-making. A useful and broadly used measure of treatment effect is the number needed to treat (NNT) to avoid a clinical progression event. The NNT is defined as the inverse of the absolute risk reduction [16] and reports the number of patients who need to be treated with one therapy versus an alternative therapy to achieve one additional clinical response or outcome. This approach has been previously used by the FDA to aid benefit-risk treatment comparisons [17] and is widely used in medical literature for its ease of interpretation. Thus, this analysis used outcomes data from the STRIVE and TERRAIN trials to calculate the NNT to avoid a clinical progression event (PFS, rPFS, or PSA progression) in patients with chemotherapy-naïve mCRPC receiving enzalutamide versus bicalutamide at 1 and 2 years.

Study population

This analysis reviewed data from patients with chemotherapy-naïve mCRPC in the STRIVE [14] (NCT01664923) and TERRAIN [15] (NCT01288911) trials. The definition of mCRPC was confirmed adenocarcinoma of the prostate, serum testosterone level less than 50 ng/dL, disease progression on androgen-deprivation therapy, and bone or soft tissue metastases in both trials [14, 15]. Approximately 65% of patients in the STRIVE trial had radiographic documentation of metastatic disease and all patients in the TERRAIN trial had mCRPC.

Baseline patient characteristics

Baseline demographic categories of the study populations (age, race, weight, and body mass index) were reported. Clinical characteristics including Eastern Cooperative Oncology Group (ECOG) performance status score [18] and serum PSA levels were also summarized [14, 15].

Clinical progression outcomes

Clinical progression events have been previously reported and included PFS, rPFS, and PSA progression at 1 and 2 years. These events were evaluated using end points defined in the STRIVE [14] and TERRAIN [15] trials that were similar but not identical (Table 1).

NNT analysis

The NNT to achieve one additional patient free from clinical progression was calculated as the reciprocal of the rate difference between enzalutamide and bicalutamide at 1 and 2 years. The 95% Confidence Interval (CI) of the NNT was calculated as the inverse of the 95% CI of the rate difference when comparing enzalutamide with bicalutamide. In this analysis, the NNT value represents the number of patients who needed to be treated with enzalutamide versus bicalutamide to achieve one additional patient with PFS, rPFS, or no PSA progression. Lower NNT values indicate greater benefit of enzalutamide over bicalutamide. The time points at 1 and 2 years were selected because the median follow-up was 17 months for both the enzalutamide and bicalutamide arms in the STRIVE trial and 20 and 17 months for the enzalutamide and bicalutamide arms, respectively, in the TERRAIN trial. In the TERRAIN trial at 2 years, the median time to events was reached for the majority of the evaluated clinical progression events (except rPFS).

NNT analyses were conducted separately from the STRIVE and TERRAIN trial data. For STRIVE, one- and two-year rates and standard errors of PFS, rPFS, and freedom from PSA progression with enzalutamide and bicalutamide were derived from the available clinical study report [11]. For TERRAIN, one- and two-year rates of PFS, rPFS, and no PSA progression with enzalutamide and bicalutamide were derived from the digitized Kaplan-Meier curves. Pseudo-individual patient data were generated from the digitized Kaplan-Meier curves according to the algorithm described in Guyot et al. [15, 19] were used to estimate the standard errors of the one- and two-year rates of the end point outcomes using Greenwood’s formula [20]. The 95% CIs of the rate difference were estimated based on the point estimate and standard error of each individual rate.

Baseline characteristics

A total of 257 (128 enzalutamide, 129 bicalutamide) patients with chemotherapy-naïve mCRPC in STRIVE [14] and 375 (184 enzalutamide, 191 bicalutamide) patients in TERRAIN [15] were included in the analysis. At baseline, the median ages of the STRIVE patients receiving enzalutamide or bicalutamide were 71 and 72 years, respectively; in TERRAIN, the median age of patients receiving either treatment was 71 years. The majority of patients in both trials were white. The distribution of ECOG scores was similar in both trials for patients receiving enzalutamide or bicalutamide, and median serum PSA levels were higher in TERRAIN than in STRIVE (Table 2).

Rates of clinical progression in STRIVE

At 1 year, PFS rates were 59.5% for enzalutamide patients and 9.4% for bicalutamide patients in STRIVE, a difference of 50.1% (95% CI 39.5–60.7) [Table 3]. rPFS rates at 1 year were 74.0 and 35.1% for enzalutamide and bicalutamide patients, respectively, a difference of 38.9% (95% CI 24.7–53.1). At 1 year, 69.4 and 12.9% of enzalutamide and bicalutamide patients, respectively, were free from PSA progression, a difference of 56.5% (95% CI 45.4–67.7).

Similar to the 1-year results in STRIVE, enzalutamide resulted in superior outcomes relative to bicalutamide at 2 years (Table 3). At 2 years, PFS rates were 40.0% for enzalutamide patients and 4.1% for bicalutamide patients, a difference of 35.9% (95% CI 23.4–48.4). rPFS rates at 2 years were 56.4 and 23.2% for enzalutamide and bicalutamide patients, respectively, a difference of 33.1% (95% CI 13.9–52.4). At 2 years, 50.3 and 8.1% of enzalutamide and bicalutamide patients, respectively, were free from PSA progression, a difference of 42.2% (95% CI 27.0–57.4).

NNT in STRIVE

For STRIVE, the NNT for PFS was 2.0 (upper, lower limits: 1.6, 2.5) when comparing enzalutamide and bicalutamide; thus, treating two patients with enzalutamide resulted in one additional patient with PFS at 1 year versus treating with bicalutamide (Fig. 1). At 2 years, the NNT for PFS was 2.8 (upper, lower limits: 2.1, 4.3) when comparing enzalutamide and bicalutamide. The NNT for rPFS at 2 year was 2.6 (upper, lower limits: 1.9, 4.0) and at 2 years was 3.0 (1.9, 7.2) when comparing enzalutamide and bicalutamide. Lastly, the NNT for freedom from PSA progression was 1.8 (upper, lower limits: 1.5, 2.2) at 1 year and 2.4 (1.7, 3.7) at 2 years when comparing enzalutamide and bicalutamide.

NNT for PFS, rPFS, and freedom from PSA progression comparing enzalutamide with bicalutamide. NNT for the STRIVE (a) and TERRAIN (b) trials at 1 and 2 years. The lower limit of NNT for rPFS at 1 year was not reported, as the rate difference between enzalutamide with bicalutamide covers the 0, and it is not meaningful to report a negative NNT value. NNT number needed to treat, PFS progression-free survival, PSA prostate-specific antigen, rPFS radiographic progression-free survival

Full size image

Rates of clinical progression in TERRAIN

At 1 year, PFS rates were 55.0% for enzalutamide patients and 31.7% for bicalutamide patients in TERRAIN, a difference of 23.3% (95% CI 12.6–34.0) [Table 3]. rPFS rates at 1 year were 68.2 and 58.1% for enzalutamide and bicalutamide patients, respectively, a difference of 10.1% (95% CI − 2.6-22.7). At 1 year, 65.1 and 18.6% of enzalutamide and bicalutamide patients, respectively, were free from PSA progression, a difference of 46.5% (95% CI 34.6–58.5).

Similar to the one-year results in TERRAIN, enzalutamide also resulted in superior outcomes relative to bicalutamide at 2 years (Table 3). At 2 years, PFS rates were 37.8% for enzalutamide patients and 11.0% for bicalutamide patients, a difference of 26.8% (95% CI 15.0–38.7). rPFS rates at 2 years were 61.3 and 25.6% for enzalutamide and bicalutamide patients, respectively, a difference of 35.7% (95% CI 18.3–53.0). Lastly, 41.3% and 10.3% of enzalutamide and bicalutamide patients, respectively, were free from PSA progression at 2 years, a difference of 31.0% (95% CI 16.9–45.1).

NNT in TERRAIN

For TERRAIN, the NNT for PFS at 1 year was 4.3 (upper, lower limits: 2.9, 8.0) and at 2 years was 3.7 (2.6, 6.7) when comparing enzalutamide with bicalutamide (Fig. 1). The NNT for rPFS at 1 year was 10.0 (upper, lower limits: 4.4, not evaluable) and at 2 years was 2.8 (1.9, 5.5) when comparing enzalutamide with bicalutamide. The NNT for freedom from PSA progression was 2.1 (upper, lower limits: 1.7, 2.9) at 1 year and 3.2 (2.2, 5.9) at 2 years when comparing enzalutamide with bicalutamide.

This analysis used data from the STRIVE [14] and TERRAIN [15] clinical trials comparing two AR inhibitor therapies – enzalutamide and bicalutamide – for the treatment of chemotherapy-naïve patients with mCRPC to calculate NNT to avoid clinical progression. The outcomes reported in the trials were translated into NNTs, a metric of comparative efficacy that can be utilized to inform decision-making in clinical practice. The results show that at 1 year, the NNTs when comparing enzalutamide with bicalutamide in STRIVE and TERRAIN were 2.0 and 4.3, respectively for PFS; 2.6 and 10.0, respectively, for rPFS; and 1.8 and 2.1, respectively, for no PSA progression. At 2 years, the NNTs comparing enzalutamide with bicalutamide in STRIVE and TERRAIN were 2.8 and 3.7, respectively, for PFS; 3.0 and 2.8, respectively, for rPFS; and 2.4 and 3.2, respectively, for no PSA progression.

It is important to consider that NNT values estimated from the STRIVE and TERRAIN trials are generally consistent across time points and across the different clinical trial populations, with the exception of rPFS at 1 year. The NNT of rPFS at 1 year estimated from the TERRAIN trial was 10.0 and the CI of the rPFS rate difference crossed 0; however, the respective NNT value estimated from the STRIVE trial was 2.6. At 2 years, the NNTs for rPFS were similar across the trials, with the values estimated at 3.0 (upper, lower limits: 1.9, 7.2) and 2.8 (upper, lower limits: 1.9, 5.5) for STRIVE and TERRAIN, respectively. This difference indicates that the uncertainties associated with the benefit of enzalutamide versus bicalutamide decreased over the long term. Thus, the numerically lower NNT values for enzalutamide versus those for bicalutamide demonstrate that enzalutamide for mCRPC leads to more patients free from disease progression or death (i.e. PFS), radiographic disease progression, and PSA progression compared with bicalutamide at 1 and 2 years.

NNT analysis was selected to compare enzalutamide with bicalutamide for the treatment of mCRPC because it is an established and interpretable measure that can be used in clinical practice to illustrate treatment effectiveness. This approach has been previously applied in evaluating treatments in PC [21, 22]. For example, Massoudi et al. [22] compared enzalutamide with abiraterone plus prednisone using data from the PREVAIL [23] and COU-AA-302 [24, 25] clinical trials. They reported an NNT of 14 for rPFS, indicating that treating 14 patients with enzalutamide instead of abiraterone plus prednisone would yield one extra patient free of radiographic progression or death at 1 year. When comparing therapies on efficacy outcomes, in general, lower NNTs indicate treatment superiority. The smallest possible NNT is 1; a value that translates for every patient treated with a therapy, there would be a benefit that would not be reached with the comparative treatment. However, values can range widely across NNT comparisons and there is no established threshold for an NNT value to be considered clinically meaningful.

Hildebrandt et al. [26] conducted a literature review of the use of NNT calculations alongside randomized controlled trials (2003 to 2005) and noted that 62 of 734 eligible trials reported NNTs with values ranging from 2 to 325.7. Therefore, each individual NNT measure needs to be evaluated for its clinical interpretation based on the disease and outcomes used for the evaluation. That being said, the value of NNT is evident based on the emerging number of recent publications using this methodology when evaluating oncology treatment options [27,28,29,30,31]. In addition, the 2018 National Comprehensive Cancer Network (NCCN) guidelines for prostate cancer cite studies that report NNT estimates in the discussion of active surveillance and radical prostatectomy [7]. Furthermore, the NNT methodology provides a transparent interpretation of the relative risk for a particular outcome that can be utilized in clinical practice decision-making.

The value of the present analysis is to translate the statistically significant outcome rate differences reported in STRIVE and TERRAIN into a clear effect-size measure relevant to real-world clinical practice and treatment choice when considering enzalutamide versus bicalutamide. With the exception of the NNT for rPFS at 1 year in TERRAIN, all of the NNTs were similar and demonstrated a robust effect size and clinical benefit of enzalutamide over bicalutamide and overall agreement among the robust Phase II trials.

Historically, bicalutamide has been commonly used in the treatment of various stages of PC due to its global accessibility, relatively low cost, once-daily dosing formulation, well-established safety profile, and ability to reduce PSA levels [5, 32, 33]. Bicalutamide can be used as monotherapy or combination therapy (approved in the United States at 50 mg once daily), and its efficacy in PC has been reported in several studies. For example, a 1996 randomized, double-blind, multicenter study compared 50 mg once-daily bicalutamide plus LHRH with 250 mg (3 times a day) flutamide plus LHRH in patients with untreated metastatic PC and reported that bicalutamide was better tolerated than flutamide, although efficacy was similar [33]. Additionally, Klotz et al. [32] reported a 20% reduction in risk of death in metastatic PC patients receiving 50 mg once-daily bicalutamide compared with castration alone.

However, the recent availability of several new therapies for chemotherapy-naïve mCRPC presents opportunities for physicians and patients to optimize treatment decision-making in consideration of all approved therapeutic options and current association guidelines. In particular, among the FDA-approved treatments for chemotherapy-naïve mCRPC, enzalutamide has received recommendations in the NCCN guidelines based on Category 1 evidence, and these recommendations have been adopted in clinical practice [7, 34]. The pivotal trial of enzalutamide (PREVAIL) [23] compared the drug with placebo among chemotherapy-naïve patients and observed improved overall survival (median survival of 32.4 months vs. 30.2 months, respectively) and rPFS (65% vs. 14% at 12 months). The AFFIRM trial [35] assessed patients previously treated with docetaxel-based chemotherapy and also found improved overall survival for enzalutamide versus placebo (median survival of 18.4 months vs. 13.6 months, respectively) and improved rPFS (median of 8.3 months vs. 2.9 months, respectively). As currently discussed, both STRIVE and TERRAIN reinforced the superiority of enzalutamide over bicalutamide for chemotherapy-naïve mCRPC [14, 15]. In addition, in comparison with the PREVAIL and AFFIRM trials which allowed progression on previous bicalutamide, progression on prior bicalutamide was not allowed in the STRIVE and TERRAIN trials [14, 15, 23, 35]. Therefore, these four clinical trials showed clinical efficacy for enzalutamide among patient populations with diverse treatment history (e.g. chemotherapy-naïve, post chemotherapy, bicalutamide-naïve, and bicalutamide-experienced).

The availability of evidence from STRIVE and TERRAIN, as well as this NNT comparison, help establish optimal treatment strategies for mCRPC and may result in a change in the use of enzalutamide and bicalutamide in clinical practice. Future studies could use similar NNT methodology to indirectly compare enzalutamide with other existing and emerging hormonal therapies for the treatment of chemotherapy-naïve mCRPC. In addition, NNT analyses based on follow-up data beyond 2 years from STRIVE and TERRAIN would provide additional value.

Limitations

In addition to the previous comments regarding NNT analyses, this research is subject to the following limitations. First, patients enrolled in clinical trials might not be representative of the overall mCRPC population in real-world clinical practice. Trial-specific events and case report forms may assess outcomes more rigorously than real-world practice. Second, overall survival was not evaluated in the current analysis because the STRIVE and TERRAIN trials did not include it as a standalone end point; therefore the overall survival rate was not reported in the publications [14, 15]. Third, in this analysis, evaluations of clinical progression outcomes were limited to 1 and 2 years due to the availability of the data; however, NNT can be evaluated at additional time points. Fourth, the current NNT analysis focused on clinical efficacy; NNTs related to safety or quality-of-life outcomes were not examined, although future studies evaluating this topic would be valuable. Lastly, while this study focused on NNT comparing these two treatments, future studies should also consider evaluating the cost and cost-efficacy of these two therapies in the mCRPC population.

The results from the current NNT analysis of chemotherapy-naïve mCRPC patients in STRIVE and TERRAIN indicate that treatment with enzalutamide will lead to more patients free from disease progression or death (i.e. PFS), radiographic disease progression, and PSA progression compared with bicalutamide at 1 and 2 years. In addition to the results of STRIVE and TERRAIN, this analysis may assist physicians and patients in choosing the optimal treatment for mCRPC.

• 01 October 2018

  It has been highlighted that in the original article [1] there was a typesetting mistake in the Results – NNT in Strive section. This Correction article states the incorrect and correct sentence.

AR:

Androgen receptor

CI:

Confidence Interval

CRPC:

Castration-resistant prostate cancer

ECOG:

Eastern Cooperative Oncology Group

FDA:

United States Food and Drug Administration

LHRH:

Luteinizing hormone-releasing hormone

mCRPC:

Metastatic castration-resistant prostate cancer

NCCN:

National Comprehensive Cancer Network

NNT:

Number needed to treat

PC:

Prostate cancer

PFS:

Progression-free survival

PSA:

Prostate-specific antigen

rPFS:

Radiographic progression-free survival

Medical writing assistance was provided by Shelley Batts, PhD, an employee of Analysis Group, Inc. Editorial assistance was provided by Lauren Smith, from Complete HealthVizion, and funded by the study sponsors.

Funding

This research was funded by Astellas Pharma, Inc. and Medivation, Inc., which was acquired by Pfizer, Inc. in September 2016, the co-developers of enzalutamide. Medical writing and editing were funded by the study sponsors.

Availability of data and materials

All data generated or analyzed during this study are included in this published article.

Authors and Affiliations

1. Astellas Pharma, Inc., 1 Astellas Way, Northbrook, IL, 60062, USA

   Neil M. Schultz, Bruce A. Brown & Scott C. Flanders

2. Carolina Urologic Research Center, Myrtle Beach, SC, USA

   Neal D. Shore

3. Guy’s, King’s, and St. Thomas’ Hospitals, London, UK

   Simon Chowdhury

4. Sunnybrook Health Sciences Centre, University of Toronto, Toronto, ON, Canada

   Laurence H. Klotz

5. Urology Associates, P.C, Nashville, TN, USA

   Raoul S. Concepcion

6. Vanderbilt University Medical Center, Nashville, TN, USA

   David F. Penson

7. The Urology Center of Colorado, Denver, CO, USA

   Lawrence I. Karsh

8. Analysis Group, Inc., Boston, MA, USA

   Hongbo Yang

9. Medivation, Inc., San Francisco, CA, USA

   Arie Barlev

10. Pfizer, Inc., New York, NY, USA

    Arie Barlev

Contributions

The study sponsor was involved in all stages of the study research and manuscript preparation, but all authors participated in the design of the study, contributed to manuscript development, and made the decision to submit the work for publication. Data were extracted from the STRIVE and TERRAIN trial publications by Analysis Group, Inc. and analyzed and interpreted in collaboration with all other authors. Manuscript drafts were prepared by the authors, with editorial assistance from a professional medical writer. All the authors vouch for the accuracy and completeness of the data reported.

Corresponding author

Correspondence to Neil M. Schultz.

Ethics approval and consent to participate

Not applicable.

Consent for publication

Not applicable.

Competing interests

NMS, SCF and BAB are employees of Astellas and own stock/stock options at the time of this manuscript, however, SCF and BAB are no longer employees presently of Astellas. AB was an employee of Medivation at the time of the study and owns stock/stock options. NDS has been a consultant/advisor for Amgen, Astellas, Bayer, Dendreon, Ferring, Janssen, Medivation, Sanofi, Takeda, and Inovio and has participated in speaker bureaus for Janssen, Bayer, and Dendreon. SC has acted as a consultant/advisor for Astellas and Janssen and has participated in speaker bureaus for Janssen, Sanofi, Clovis Oncology, and Astellas. LHK reports honoraria for advisory board participation from Astellas, Medivation, Janssen, Amgen, Genomic Health, and AbbVie, outside the submitted work. RSC has been a consultant/advisor for CUSP, Integra Connect, and Dendreon and reports honoraria for participation in speaker bureaus for Astellas, Medivation, Janssen, Bayer, and Sanofi. DFP has been a consultant for Astellas, Medivation, and Dendreon. LIK has been a consultant for 3DBiopsy, Argos, Tokai, Takeda, Heat Biologics, Augmenix, Dendreon, Astellas, Bayer, Janssen, Medivation, and Sanofi, has participated in speaker bureaus for Astellas, Bayer, Janssen, Medivation, Amgen, and Dendreon, has received research funding from Astellas, Bayer, Janssen, Medivation, Sanofi, Spectrum, Ferring, Precision Biopsy, 3DBiopsy, Argos, Tokai, Takeda, Heat Biologics, Augmenix, and Dendreon through his institution, and owns stock options with Swan Valley Medical. HY is an employee of Analysis Group Inc., which has received consultancy fees from Astellas and Medivation.

Publisher’s Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.

Reprints and permissions