Capivasertib plus abiraterone in PTEN-deficient metastatic hormone-sensitive prostate cancer: CAPItello-281 phase III study☆

Simple item page
dc.contributor.authorFizazi K.
dc.contributor.authorClarke N.W.
dc.contributor.authorDe Santis M.
dc.contributor.authorUemura H.
dc.contributor.authorFay A.P.
dc.contributor.authorKaradurmus N.
dc.contributor.authorKwiatkowski M.
dc.contributor.authorAlvarez-Fernandez C.
dc.contributor.authorJiang S.
dc.contributor.authorSotelo M.
dc.contributor.authorParslow D.
dc.contributor.authorOliveira N.
dc.contributor.authorKwon T.G.
dc.contributor.authorYe D.
dc.contributor.authorBoudewijns S.
dc.contributor.authorDanchaivijitr P.
dc.contributor.authorRooney C.
dc.contributor.authorGresty C.
dc.contributor.authorYeste-Velasco M.
dc.contributor.authorLogan J.
dc.contributor.authorGeorge D.J.
dc.contributor.correspondenceFizazi K.
dc.contributor.otherMahidol University
dc.date.accessioned2025-12-20T18:17:30Z
dc.date.available2025-12-20T18:17:30Z
dc.date.issued2025-01-01
dc.description.abstractBackground: In metastatic hormone-sensitive prostate cancer (mHSPC), phosphatase and tensin homolog (PTEN) deficiency results in phosphoinositide 3-kinase (PI3K)/protein kinase B (AKT) pathway activation, providing an independent proliferative drive, which cannot be suppressed by androgen receptor pathway inhibitors (ARPIs), resulting in worse outcomes. Dual inhibition of PI3K/AKT and AR pathways with capivasertib and abiraterone may delay progression and improve disease outcomes. Patients and methods: In CAPItello-281 (NCT04493853), patients with PTEN-deficient mHSPC (diagnostic cut-off: ≥90% viable malignant cells with no specific cytoplasmic PTEN immunohistochemistry staining) received capivasertib or placebo (1 : 1) plus abiraterone, prednisone/prednisolone, and androgen deprivation therapy (ADT). The primary endpoint was investigator-assessed radiographic progression-free survival (rPFS); overall survival (OS) was a key secondary endpoint. Post hoc exploratory subgroups at increasing PTEN cut-off thresholds were also assessed. Results: 25.3% (1519/6003) of patients with valid tumor test results had PTEN-deficient tumors. In the randomized PTEN-deficient population, a statistically significant improvement in rPFS was observed with capivasertib plus abiraterone (n = 507, median 33.2 months) versus placebo plus abiraterone [n = 505, 25.7 months; hazard ratio (HR) 0.81, 95% confidence interval (CI) 0.66-0.98, P = 0.034]. Post hoc rPFS analyses for loss of PTEN cut-offs of ≥95%, ≥99%, and 100% showed that the capivasertib plus abiraterone arm performed consistently across cut-offs, but the placebo plus abiraterone arm performed progressively worse as the cut-off for the degree of PTEN loss was increased, resulting in a numerically improved treatment effect. In the overall population studied, the HR for OS (26.4% maturity) was 0.90, 95% CI 0.71-1.15, P = 0.401. The most common adverse events (AEs) for capivasertib plus abiraterone were diarrhea (51.9%; 8.0% placebo plus abiraterone), hyperglycemia (38.0%; 12.9%), and rash (35.4%; 7.0%). Deaths associated with an AE were reported in 36 (7.2%) and 26 (5.2%) patients in the capivasertib plus abiraterone and placebo plus abiraterone arms, respectively. Conclusions: Capivasertib plus abiraterone improves rPFS versus placebo plus abiraterone in PTEN-deficient mHSPC, on a background of ADT, with a 7.5-month improvement in median rPFS. AE profile was consistent with that of the individual agents. Patients with PTEN-deficient mHSPC benefit from dual blockade of the PI3K/AKT and AR pathways with capivasertib plus abiraterone.
dc.identifier.citationAnnals of Oncology (2025)
dc.identifier.doi10.1016/j.annonc.2025.10.004
dc.identifier.eissn15698041
dc.identifier.issn09237534
dc.identifier.pmid41120017
dc.identifier.scopus2-s2.0-105024661258
dc.identifier.urihttps://repository.li.mahidol.ac.th/handle/123456789/113599
dc.rights.holderSCOPUS
dc.subjectMedicine
dc.titleCapivasertib plus abiraterone in PTEN-deficient metastatic hormone-sensitive prostate cancer: CAPItello-281 phase III study☆
dc.typeArticle
mu.datasource.scopushttps://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=105024661258&origin=inward
oaire.citation.titleAnnals of Oncology
oairecerif.author.affiliationThe University of Manchester
oairecerif.author.affiliationThe University of Queensland
oairecerif.author.affiliationDuke University
oairecerif.author.affiliationCharité – Universitätsmedizin Berlin
oairecerif.author.affiliationMedizinische Universität Wien
oairecerif.author.affiliationInstitut de Cancerologie Gustave Roussy
oairecerif.author.affiliationAstraZeneca
oairecerif.author.affiliationPontifícia Universidade Católica do Rio Grande do Sul
oairecerif.author.affiliationSiriraj Hospital
oairecerif.author.affiliationGülhane Eğitim ve Araştırma Hastanesi
oairecerif.author.affiliationFudan University Shanghai Cancer Center
oairecerif.author.affiliationHospital Universitario Central de Asturias
oairecerif.author.affiliationThe Affiliated Cancer Hospital of Xiangya School of Medicine, Central South University
oairecerif.author.affiliationDerriford Hospital
oairecerif.author.affiliationInstituto de Investigación Sanitaria del Principado de Asturias
oairecerif.author.affiliationKyungpook National University Chilgok Hospital
oairecerif.author.affiliationKindai University Hospital
oairecerif.author.affiliationMater Hospital Brisbane
oairecerif.author.affiliationHospital María Auxiliadora
oairecerif.author.affiliationBravis Ziekenhuis
oairecerif.author.affiliationSzpital Wojewodzki

Files

Collections

Scopus 2025