Phase II Randomized Study of MK-2206 and Bicalutamide in Prostate Cancer Patients With Rising PSA After Primary Therapy (ECOG-ACRIN E2809).
2/5 보강
PICO 자동 추출 (휴리스틱, conf 2/4)
유사 논문P · Population 대상 환자/모집단
추출되지 않음
I · Intervention 중재 / 시술
AKT inhibitor MK-2206 200 mg 2x/week, arm-A was observation; second phase, bicalutamide (Bic), 50 mg daily, was added to each arm
C · Comparison 대조 / 비교
추출되지 않음
O · Outcome 결과 / 결론
[CLINICAL TRIAL REGISTRATION] ClinicalTrials. gov number, NCT01251861.
OpenAlex 토픽 ·
Prostate Cancer Treatment and Research
Cancer, Lipids, and Metabolism
Prostate Cancer Diagnosis and Treatment
[BACKGROUND] Combined inhibition of AKT and the androgen receptor (AR) might be more efficacious than AR inhibition alone in biochemical recurrence (BCR) of prostate cancer (PC) by additive effects on
- p-value p = 0.02
- p-value p = 0.04
APA
Anna C. Ferrari, Yuhui Chen, et al. (2026). Phase II Randomized Study of MK-2206 and Bicalutamide in Prostate Cancer Patients With Rising PSA After Primary Therapy (ECOG-ACRIN E2809).. The Prostate, 86(6), 697-709. https://doi.org/10.1002/pros.70125
MLA
Anna C. Ferrari, et al.. "Phase II Randomized Study of MK-2206 and Bicalutamide in Prostate Cancer Patients With Rising PSA After Primary Therapy (ECOG-ACRIN E2809).." The Prostate, vol. 86, no. 6, 2026, pp. 697-709.
PMID
41609418
Abstract
[BACKGROUND] Combined inhibition of AKT and the androgen receptor (AR) might be more efficacious than AR inhibition alone in biochemical recurrence (BCR) of prostate cancer (PC) by additive effects on the two effector pathways.
[PATIENTS AND METHODS] E2809 assigned 108 high-risk BCR patients (1:1, arm-A: arm-B) to two phases with 4-week cycles: first (PreBic) phase (3 cycles), arm-B received AKT inhibitor MK-2206 200 mg 2x/week, arm-A was observation; second phase, bicalutamide (Bic), 50 mg daily, was added to each arm. The PreBic phase assessed whether AKT inhibition changed PSA, reflecting AR activation. Exploratory primary endpoint (EP1) at 6-8 Bic cycles and secondary EP2 at cycle 14 compared the proportion of cases with ≥stable disease (SD) or progressive disease (PD).
[RESULTS] PreBic phase: 70% arm-B vs 32% arm-A patients had a ≥ 60% PSA rise (p = 0.02). MK-2206 skin toxicity (38% grade ≥ 3) drove high withdrawal prior to EP1. Bic phase: at EP1, inter-arm PSA response (81%/82%) or PD (19%/18%) was equal. At EP2, PD was greater in arm-A than arm B (36% vs 11%; p = 0.04). In subgroups defined by PreBic phase PD (PBPD; PSA rise ≥ 25%), 9/16 arm-A vs 0/7 arm-B cases experienced PD at EP2 (p = 0.02); overall between PBPD-subgroups, 73% arm-A vs 27% arm-B experienced PD.
[CONCLUSIONS] The results suggest that latent improved outcome of high-risk BCR patients (mean PSA doubling time 4.4 months) on combined MK-2206+Bic versus Bic alone was attributable to a subgroup identified by crosstalk AR activation secondary to inhibition of AKT. Toxicity may affect tolerance of sustained AKT-AR inhibition.
[CLINICAL TRIAL REGISTRATION] ClinicalTrials. gov number, NCT01251861.
[PATIENTS AND METHODS] E2809 assigned 108 high-risk BCR patients (1:1, arm-A: arm-B) to two phases with 4-week cycles: first (PreBic) phase (3 cycles), arm-B received AKT inhibitor MK-2206 200 mg 2x/week, arm-A was observation; second phase, bicalutamide (Bic), 50 mg daily, was added to each arm. The PreBic phase assessed whether AKT inhibition changed PSA, reflecting AR activation. Exploratory primary endpoint (EP1) at 6-8 Bic cycles and secondary EP2 at cycle 14 compared the proportion of cases with ≥stable disease (SD) or progressive disease (PD).
[RESULTS] PreBic phase: 70% arm-B vs 32% arm-A patients had a ≥ 60% PSA rise (p = 0.02). MK-2206 skin toxicity (38% grade ≥ 3) drove high withdrawal prior to EP1. Bic phase: at EP1, inter-arm PSA response (81%/82%) or PD (19%/18%) was equal. At EP2, PD was greater in arm-A than arm B (36% vs 11%; p = 0.04). In subgroups defined by PreBic phase PD (PBPD; PSA rise ≥ 25%), 9/16 arm-A vs 0/7 arm-B cases experienced PD at EP2 (p = 0.02); overall between PBPD-subgroups, 73% arm-A vs 27% arm-B experienced PD.
[CONCLUSIONS] The results suggest that latent improved outcome of high-risk BCR patients (mean PSA doubling time 4.4 months) on combined MK-2206+Bic versus Bic alone was attributable to a subgroup identified by crosstalk AR activation secondary to inhibition of AKT. Toxicity may affect tolerance of sustained AKT-AR inhibition.
[CLINICAL TRIAL REGISTRATION] ClinicalTrials. gov number, NCT01251861.
MeSH Terms
Male; Humans; Prostatic Neoplasms; Anilides; Tosyl Compounds; Nitriles; Prostate-Specific Antigen; Aged; Middle Aged; Heterocyclic Compounds, 3-Ring; Antineoplastic Combined Chemotherapy Protocols; Neoplasm Recurrence, Local; Proto-Oncogene Proteins c-akt; Androgen Antagonists