Background
Androgen receptor pathway inhibitors (ARPIs) may have distinct central nervous system (CNS) penetration and differential effects on cognition or quality of life (QOL). AFT-47, “ARACOG” is a prospective, randomized open-label phase 2 trial comparing objective and patient-reported cognitive and QOL outcomes between patients with metastatic hormone sensitive prostate cancer (mHSPC), metastatic castration-resistant prostate cancer (mCRPC) or non-metastatic castration-resistant prostate cancer (nmCRPC) treated with darolutamide (DAR) or enzalutamide (ENZ).
Methods
Between 8/17/2021 and 3/11/2025, 111 pts were enrolled and randomized 1:1 to treatment with ENZ or DAR. CANTAB, a validated computer-based platform evaluating 5 cognitive domains (PALFAM-memory recall, SWM- spatial working memory, SSP-short-term visual memory, working memory, RVP-rapid visual processing, and OTSMCC- executive function), was performed at baseline, 12, 24, and 48 weeks. Crossover (Xover) was allowed at 12 or 24 weeks for significant pre-specified decline in cognitive testing or patient reported outcome measures (PROMs), or for CNS-associated adverse events, including falls. The primary endpoint was the percent change in the maximally changed cognitive domain (MCCD) from baseline to 24 weeks and was compared between groups with the Wilcoxon rank sum statistic. Patients crossing over prior to 24 weeks were evaluated at the time of Xover and analyzed with their randomized arm. Secondary endpoints included comparison of Xover rates.
Results
Among 111 pts, 55 received DAR and 56 received ENZ; median age was 71, 83% White. 95 pts (48 DAR, 47 ENZ) were evaluable for the primary endpoint. Baseline CANTAB was similar between groups. Median cognitive change in MCCD between baseline and 24 weeks was -15.8% and -36.1% for the DAR and ENZ pts, respectively (p = 0.009) (Table). Individual cognitive domains suggest possible learning effect (increased scores) for DAR and are stable or show mild decline for ENZ treated patients at 24 weeks. 32 DAR (58%) and 33 ENZ (59%) participants were eligible for Xover by 24 weeks, and 23 pts crossed over by 24 weeks. All Xover was pts randomized to ENZ (crossed to DAR), with the most common causes being decline in objective (N = 14) or subjective (N = 11) cognitive testing.
Conclusions
In this US randomized trial comparing DAR to ENZ, the primary endpoint of differential cognitive effects was met. ENZ showed significantly greater cognitive score decline than DAR at 24 weeks in the MCCD after treatment initiation. Learning effect was seen with DAR but not ENZ. Longer term follow-up of cognitive change and PROM analyses are ongoing.
Percent change in maximally changed cognitive domain by treatment.