Capivasertib, an AKT Kinase Inhibitor, as Monotherapy or in Combination with Fulvestrant in Patients with AKT1E17K-Mutant, ER-Positive Metastatic Breast Cancer

被引：67

作者：

Smyth, Lillian M. ^{[1
,12
]}

Tamura, Kenji ^{[2
]}

Oliveira, Mafalda ^{[3
,4
]}

Ciruelos, Eva M. ^{[5
]}

Mayer, Ingrid A. ^{[6
]}

Sablin, Marie-Paule ^{[7
]}

Biganzoli, Laura ^{[8
]}

Ambrose, Helen J. ^{[9
]}

Ashton, Jack ^{[9
]}

Barnicle, Alan ^{[9
]}

Cashell, Des D. ^{[9
]}

Corcoran, Claire ^{[9
]}

de Bruin, Elza C. ^{[9
]}

Foxley, Andrew ^{[9
]}

Hauser, Joana ^{[9
]}

Lindemann, Justin P. O. ^{[9
]}

Maudsley, Rhiannon ^{[9
]}

McEwen, Robert ^{[9
]}

Moschetta, Michele ^{[9
]}

Pass, Martin ^{[9
]}

Rowlands, Vicky ^{[9
]}

Schiavon, Gaia ^{[9
]}

Banerji, Udai ^{[10
,11
]}

Scaltriti, Maurizio ^{[1
]}

Taylor, Barry S. ^{[1
]}

Chandarlapaty, Sarat ^{[1
]}

Baselga, Jose ^{[1
,13
]}

Hyman, David M. ^{[1
]}

机构：

[1] Mem Sloan Kettering Canc Ctr, 1275 York Ave, New York, NY 10021 USA

[2] Natl Canc Ctr, Tokyo, Japan

[3] Vall dHebron Univ Hosp, Barcelona, Spain

[4] Vall dHebron Inst Oncol, Barcelona, Spain

[5] Hosp Univ 12 Octubre, Madrid, Spain

[6] Vanderbilt Breast Ctr, Nashville, TN USA

[7] Inst Curie, Paris, France

[8] Hosp Prato, Breast Ctr, Oncol Dept, Prato, Italy

[9] AstraZeneca, R&D Oncol, Cambridge, England

[10] Inst Canc Res, London, England

[11] Royal Marsden NHS Fdn Trust, London, England

[12] St Vincents Univ Hosp, Elm Pk, Dublin D04 T6F4, Ireland

[13] AstraZeneca, Res & Dev Oncol, Gaithersburg, MD USA

来源：

CLINICAL CANCER RESEARCH | 2020年 / 26卷 / 15期

基金：

美国国家卫生研究院;

关键词：

MUTATIONS; THERAPY; AZD5363; COMMON; TUMORS;

D O I：

10.1158/1078-0432.CCR-19-3953

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Purpose: The activating mutation AKT1(E17K) occurs in approximately 7% of estrogen receptor-positive (ER+) metastatic breast cancer (MBC). We report, from a multipart, first-in-human, phase I study (NCT01226316), tolerability and activity of capivasertib, an oral AKT inhibitor, as monotherapy or combined with fulvestrant in expansion cohorts of patients with AKT1(E17K)-mutant ER+ MBC. Patients and Methods: Patients with an AKT1E17K mutation, detected by local (next-generation sequencing) or central (plasma-based BEAMing) testing, received capivasertib 480 mg twice daily, 4 days on, 3 days off, weekly or 400 mg twice daily combined with fulvestrant at the labeled dose. Study endpoints included safety, objective response rate (ORR; RECIST v1.1), progression-free survival (PFS), and clinical benefit rate at 24 weeks (CBR24). Biomarker analyses were conducted in the combination cohort. Results: From October 2013 to August 2018, 63 heavily pretreated patients received capivasertib (20 monotherapy, 43 combination). ORR was 20% with monotherapy, and within the combination cohort was 36% in fulvestrant-pretreated and 20% in fulvestrant-naive patients, although the latter group may have had more aggressive disease at baseline. AKT1(E17K) mutations were detectable in plasma by BEAMing (95%, 41/43), droplet digital PCR (80%, 33/41), and next-generation sequencing (76%, 31/41). A >= 50% decrease in AKT1(E17K) at cycle 2 day 1 was associated with improved PFS. Combination therapy appeared more tolerable than monotherapy [most frequent grade >= 3 adverse events: rash (9% vs. 20%), hyperglycemia (5% vs. 30%), diarrhea (5% vs. 10%)]. Conclusions: Capivasertib demonstrated clinically meaningful activity in heavily pretreated patients with AKT1(E17K)-mutant ER+ MBC, including those with prior disease progression on fulvestrant. Tolerability and activity appeared improved by the combination.

引用

页码：3947 / 3957

页数：11

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