Supplementary Figure 2 from Capivasertib, an AKT Kinase Inhibitor, as Monotherapy or in Combination with Fulvestrant in Patients with AKT1E17K-Mutant, ER-Positive Metastatic Breast Cancer

Smyth, Lillian M.; Tamura, Kenji; Oliveira, Mafalda; Ciruelos, Eva M.; Mayer, Ingrid A.; Sablin, Marie-Paule; Biganzoli, Laura; Ambrose, Helen J.; Ashton, Jack; Barnicle, Alan; Cashell, Des D.; Corcoran, Claire; de Bruin, Elza C.; Foxley, Andrew; Hauser, Joana; Lindemann, Justin P.O.; Maudsley, Rhiannon; McEwen, Robert; Moschetta, Michele; Pass, Martin; Rowlands, Vicky; Schiavon, Gaia; Banerji, Udai; Scaltriti, Maurizio; Taylor, Barry S.; Chandarlapaty, Sarat; Baselga, José; Hyman, David M.

doi:10.1158/1078-0432.22476297.v1

10780432ccr193953-sup-233401_2_supp_6216549_q8h3gs.pdf (325.43 kB)

Supplementary Figure 2 from Capivasertib, an AKT Kinase Inhibitor, as Monotherapy or in Combination with Fulvestrant in Patients with AKT1^E17K-Mutant, ER-Positive Metastatic Breast Cancer

journal contribution

posted on 2023-03-31, 22:01 authored by Lillian M. Smyth, Kenji Tamura, Mafalda Oliveira, Eva M. Ciruelos, Ingrid A. Mayer, Marie-Paule Sablin, Laura Biganzoli, Helen J. Ambrose, Jack Ashton, Alan Barnicle, Des D. Cashell, Claire Corcoran, Elza C. de Bruin, Andrew Foxley, Joana Hauser, Justin P.O. Lindemann, Rhiannon Maudsley, Robert McEwen, Michele Moschetta, Martin Pass, Vicky Rowlands, Gaia Schiavon, Udai Banerji, Maurizio Scaltriti, Barry S. Taylor, Sarat Chandarlapaty, José Baselga, David M. Hyman

Supplementary Figure 2. PFS Association With {greater than or equal to}50% Decrease from Baseline in AKT1E17K at Cycle 2 Day 1 in ctDNA

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National Institutes of Health

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AstraZeneca

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ARTICLE ABSTRACT

The activating mutation AKT1E17K 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 AKT1E17K-mutant ER+ MBC. 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. 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-naïve patients, although the latter group may have had more aggressive disease at baseline. AKT1E17K 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 AKT1E17K 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%)]. Capivasertib demonstrated clinically meaningful activity in heavily pretreated patients with AKT1E17K-mutant ER+ MBC, including those with prior disease progression on fulvestrant. Tolerability and activity appeared improved by the combination.

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Breast Cancer Small Molecule Agents Kinase inhibitors

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