npj Breast Cancer (Apr 2021)

Selective AKT kinase inhibitor capivasertib in combination with fulvestrant in PTEN-mutant ER-positive metastatic breast cancer

  • Lillian M. Smyth,
  • Gerald Batist,
  • Funda Meric-Bernstam,
  • Peter Kabos,
  • Iben Spanggaard,
  • Ana Lluch,
  • Komal Jhaveri,
  • Andrea Varga,
  • Andrea Wong,
  • Alison M. Schram,
  • Helen Ambrose,
  • T. Hedley Carr,
  • Elza C. de Bruin,
  • Carolina Salinas-Souza,
  • Andrew Foxley,
  • Joana Hauser,
  • Justin P. O. Lindemann,
  • Rhiannon Maudsley,
  • Robert McEwen,
  • Michele Moschetta,
  • Myria Nikolaou,
  • Gaia Schiavon,
  • Pedram Razavi,
  • Udai Banerji,
  • José Baselga,
  • David M. Hyman,
  • Sarat Chandarlapaty

DOI
https://doi.org/10.1038/s41523-021-00251-7
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 7

Abstract

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Abstract Five to ten percent of ER+ metastatic breast cancer (MBC) tumors harbor somatic PTEN mutations. Loss of function of this tumor-suppressor gene defines a highly aggressive, treatment-refractory disease for which new therapies are urgently needed. This Phase I multipart expansion study assessed oral capivasertib with fulvestrant in patients with PTEN-mutant ER+ MBC. Safety and tolerability were assessed by standard methods. Plasma and tumor were collected for NGS and immunohistochemistry analyses of PTEN protein expression. In 31 eligible patients (12 fulvestrant naive; 19 fulvestrant pretreated), the 24-week clinical benefit rate was 17% in fulvestrant-naive and 42% in fulvestrant-pretreated patients, with objective response rate of 8% and 21%, respectively. Non-functional PTEN was centrally confirmed in all cases by NGS or immunohistochemistry. Co­mutations occurred in PIK3CA (32%), with less ESR1 (10% vs 72%) and more TP53 (40% vs 28%) alterations in fulvestrant-naive versus fulvestrant-pretreated patients, respectively. PTEN was clonally dominant in most patients. Treatment-related grade ≥3 adverse events occurred in 32% of patients, most frequently diarrhea and maculopapular rash (both n = 2). In this clinical study, which selectively targeted the aggressive PTEN-mutant ER+ MBC, capivasertib plus fulvestrant was tolerable and clinically active. Phenotypic and genomic differences were apparent between fulvestrant-naive and -pretreated patients. Trial registration number for the study is NCT01226316.