Proliferation and AKT Activity Biomarker Analyses after Capivasertib (AZD5363) Treatment of Patients with ER+ Invasive Breast Cancer (STAKT)

John F R Robertson; Robert E Coleman; Kwok-Leung Cheung; Abigail Evans; Chris Holcombe; Anthony Skene; Daniel Rea; Samreen Ahmed; Ali Jahan; Kieran Horgan; Petra Rauchhaus; Roberta Littleford; S Y Amy Cheung; Marie Cullberg; Elza C de Bruin; Loumpiana Koulai; Justin P O Lindemann; Martin Pass; Paul Rugman; Gaia Schiavon; Rahul Deb; Pauline Finlay; Andrew Foxley; Julia M W Gee

doi:10.1158/1078-0432.CCR-19-3053

Proliferation and AKT Activity Biomarker Analyses after Capivasertib (AZD5363) Treatment of Patients with ER+ Invasive Breast Cancer (STAKT)

John F R Robertson, Robert E Coleman, Kwok-Leung Cheung, Abigail Evans, Chris Holcombe, Anthony Skene, Daniel Rea, Samreen Ahmed, Ali Jahan, Kieran Horgan, Petra Rauchhaus, Roberta Littleford, S Y Amy Cheung, Marie Cullberg, Elza C de Bruin, Loumpiana Koulai, Justin P O Lindemann, Martin Pass, Paul Rugman, Gaia SchiavonRahul Deb, Pauline Finlay, Andrew Foxley, Julia M W Gee

Cancer Clinical Trials Unit

Research output: Contribution to journal › Article › peer-review

7 Citations (Scopus)

Abstract

PURPOSE: The STAKT study examined short-term exposure (4.5 days) to the oral selective pan-AKT inhibitor capivasertib (AZD5363) to determine if this drug can reach its therapeutic target in sufficient concentration to significantly modulate key biomarkers of the AKT pathway and tumor proliferation.

METHODS: STAKT was a two-stage, double-blind, randomized, placebo-controlled, "window-of-opportunity" study in patients with newly diagnosed ER+ invasive breast cancer. Stage 1 assessed capivasertib 480 mg b.i.d. (recommended monotherapy dose) and placebo, and stage 2 assessed capivasertib 360 and 240 mg b.i.d. Primary endpoints were changes from baseline in AKT pathway markers pPRAS40, pGSK3β, and proliferation protein Ki67. Pharmacologic and pharmacodynamic properties were analyzed from blood sampling, and tolerability by adverse-event monitoring.

RESULTS: After 4.5 days' exposure, capivasertib 480 mg b.i.d. (n = 17) produced significant decreases from baseline versus placebo (n = 11) in pGSK3β (H-score absolute change: -55.3, P = 0.006) and pPRAS40 (-83.8, P < 0.0001), and a decrease in Ki67 (absolute change in percentage positive nuclei: -9.6%, P = 0.031). Significant changes also occurred in secondary signaling biomarker pS6 (-42.3, P = 0.004), while pAKT (and nuclear FOXO3a) also increased in accordance with capivasertib's mechanism (pAKT: 81.3, P = 0.005). At doses of 360 mg b.i.d. (n = 5) and 240 mg b.i.d. (n = 6), changes in primary and secondary biomarkers were also observed, albeit of smaller magnitude. Biomarker modulation was dose and concentration dependent, and no new safety signals were evident.

CONCLUSIONS: Capivasertib 480 mg b.i.d. rapidly modulates key biomarkers of the AKT pathway and decreases proliferation marker Ki67, suggesting future potential as an effective therapy in AKT-dependent breast cancers.

Original language	English
Journal	Clinical Cancer Research
DOIs	https://doi.org/10.1158/1078-0432.CCR-19-3053
Publication status	E-pub ahead of print - 13 Dec 2019

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Robertson, J. F. R., Coleman, R. E., Cheung, K-L., Evans, A., Holcombe, C., Skene, A., Rea, D., Ahmed, S., Jahan, A., Horgan, K., Rauchhaus, P., Littleford, R., Cheung, S. Y. A., Cullberg, M., de Bruin, E. C., Koulai, L., Lindemann, J. P. O., Pass, M., Rugman, P., ... Gee, J. M. W. (2019). Proliferation and AKT Activity Biomarker Analyses after Capivasertib (AZD5363) Treatment of Patients with ER+ Invasive Breast Cancer (STAKT). Clinical Cancer Research. Advance online publication. https://doi.org/10.1158/1078-0432.CCR-19-3053

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title = "Proliferation and AKT Activity Biomarker Analyses after Capivasertib (AZD5363) Treatment of Patients with ER+ Invasive Breast Cancer (STAKT)",

abstract = "PURPOSE: The STAKT study examined short-term exposure (4.5 days) to the oral selective pan-AKT inhibitor capivasertib (AZD5363) to determine if this drug can reach its therapeutic target in sufficient concentration to significantly modulate key biomarkers of the AKT pathway and tumor proliferation.METHODS: STAKT was a two-stage, double-blind, randomized, placebo-controlled, {"}window-of-opportunity{"} study in patients with newly diagnosed ER+ invasive breast cancer. Stage 1 assessed capivasertib 480 mg b.i.d. (recommended monotherapy dose) and placebo, and stage 2 assessed capivasertib 360 and 240 mg b.i.d. Primary endpoints were changes from baseline in AKT pathway markers pPRAS40, pGSK3β, and proliferation protein Ki67. Pharmacologic and pharmacodynamic properties were analyzed from blood sampling, and tolerability by adverse-event monitoring.RESULTS: After 4.5 days' exposure, capivasertib 480 mg b.i.d. (n = 17) produced significant decreases from baseline versus placebo (n = 11) in pGSK3β (H-score absolute change: -55.3, P = 0.006) and pPRAS40 (-83.8, P < 0.0001), and a decrease in Ki67 (absolute change in percentage positive nuclei: -9.6%, P = 0.031). Significant changes also occurred in secondary signaling biomarker pS6 (-42.3, P = 0.004), while pAKT (and nuclear FOXO3a) also increased in accordance with capivasertib's mechanism (pAKT: 81.3, P = 0.005). At doses of 360 mg b.i.d. (n = 5) and 240 mg b.i.d. (n = 6), changes in primary and secondary biomarkers were also observed, albeit of smaller magnitude. Biomarker modulation was dose and concentration dependent, and no new safety signals were evident.CONCLUSIONS: Capivasertib 480 mg b.i.d. rapidly modulates key biomarkers of the AKT pathway and decreases proliferation marker Ki67, suggesting future potential as an effective therapy in AKT-dependent breast cancers.",

author = "Robertson, {John F R} and Coleman, {Robert E} and Kwok-Leung Cheung and Abigail Evans and Chris Holcombe and Anthony Skene and Daniel Rea and Samreen Ahmed and Ali Jahan and Kieran Horgan and Petra Rauchhaus and Roberta Littleford and Cheung, {S Y Amy} and Marie Cullberg and {de Bruin}, {Elza C} and Loumpiana Koulai and Lindemann, {Justin P O} and Martin Pass and Paul Rugman and Gaia Schiavon and Rahul Deb and Pauline Finlay and Andrew Foxley and Gee, {Julia M W}",

note = "{\textcopyright}2019 American Association for Cancer Research.",

year = "2019",

month = dec,

day = "13",

doi = "10.1158/1078-0432.CCR-19-3053",

language = "English",

journal = "Clinical Cancer Research",

issn = "1078-0432",

publisher = "American Association for Cancer Research",

}

Robertson, JFR, Coleman, RE, Cheung, K-L, Evans, A, Holcombe, C, Skene, A, Rea, D, Ahmed, S, Jahan, A, Horgan, K, Rauchhaus, P, Littleford, R, Cheung, SYA, Cullberg, M, de Bruin, EC, Koulai, L, Lindemann, JPO, Pass, M, Rugman, P, Schiavon, G, Deb, R, Finlay, P, Foxley, A & Gee, JMW 2019, 'Proliferation and AKT Activity Biomarker Analyses after Capivasertib (AZD5363) Treatment of Patients with ER+ Invasive Breast Cancer (STAKT)', Clinical Cancer Research. https://doi.org/10.1158/1078-0432.CCR-19-3053

TY - JOUR

T1 - Proliferation and AKT Activity Biomarker Analyses after Capivasertib (AZD5363) Treatment of Patients with ER+ Invasive Breast Cancer (STAKT)

AU - Robertson, John F R

AU - Coleman, Robert E

AU - Cheung, Kwok-Leung

AU - Evans, Abigail

AU - Holcombe, Chris

AU - Skene, Anthony

AU - Rea, Daniel

AU - Ahmed, Samreen

AU - Jahan, Ali

AU - Horgan, Kieran

AU - Rauchhaus, Petra

AU - Littleford, Roberta

AU - Cheung, S Y Amy

AU - Cullberg, Marie

AU - de Bruin, Elza C

AU - Koulai, Loumpiana

AU - Lindemann, Justin P O

AU - Pass, Martin

AU - Rugman, Paul

AU - Schiavon, Gaia

AU - Deb, Rahul

AU - Finlay, Pauline

AU - Foxley, Andrew

AU - Gee, Julia M W

PY - 2019/12/13

Y1 - 2019/12/13

N2 - PURPOSE: The STAKT study examined short-term exposure (4.5 days) to the oral selective pan-AKT inhibitor capivasertib (AZD5363) to determine if this drug can reach its therapeutic target in sufficient concentration to significantly modulate key biomarkers of the AKT pathway and tumor proliferation.METHODS: STAKT was a two-stage, double-blind, randomized, placebo-controlled, "window-of-opportunity" study in patients with newly diagnosed ER+ invasive breast cancer. Stage 1 assessed capivasertib 480 mg b.i.d. (recommended monotherapy dose) and placebo, and stage 2 assessed capivasertib 360 and 240 mg b.i.d. Primary endpoints were changes from baseline in AKT pathway markers pPRAS40, pGSK3β, and proliferation protein Ki67. Pharmacologic and pharmacodynamic properties were analyzed from blood sampling, and tolerability by adverse-event monitoring.RESULTS: After 4.5 days' exposure, capivasertib 480 mg b.i.d. (n = 17) produced significant decreases from baseline versus placebo (n = 11) in pGSK3β (H-score absolute change: -55.3, P = 0.006) and pPRAS40 (-83.8, P < 0.0001), and a decrease in Ki67 (absolute change in percentage positive nuclei: -9.6%, P = 0.031). Significant changes also occurred in secondary signaling biomarker pS6 (-42.3, P = 0.004), while pAKT (and nuclear FOXO3a) also increased in accordance with capivasertib's mechanism (pAKT: 81.3, P = 0.005). At doses of 360 mg b.i.d. (n = 5) and 240 mg b.i.d. (n = 6), changes in primary and secondary biomarkers were also observed, albeit of smaller magnitude. Biomarker modulation was dose and concentration dependent, and no new safety signals were evident.CONCLUSIONS: Capivasertib 480 mg b.i.d. rapidly modulates key biomarkers of the AKT pathway and decreases proliferation marker Ki67, suggesting future potential as an effective therapy in AKT-dependent breast cancers.

AB - PURPOSE: The STAKT study examined short-term exposure (4.5 days) to the oral selective pan-AKT inhibitor capivasertib (AZD5363) to determine if this drug can reach its therapeutic target in sufficient concentration to significantly modulate key biomarkers of the AKT pathway and tumor proliferation.METHODS: STAKT was a two-stage, double-blind, randomized, placebo-controlled, "window-of-opportunity" study in patients with newly diagnosed ER+ invasive breast cancer. Stage 1 assessed capivasertib 480 mg b.i.d. (recommended monotherapy dose) and placebo, and stage 2 assessed capivasertib 360 and 240 mg b.i.d. Primary endpoints were changes from baseline in AKT pathway markers pPRAS40, pGSK3β, and proliferation protein Ki67. Pharmacologic and pharmacodynamic properties were analyzed from blood sampling, and tolerability by adverse-event monitoring.RESULTS: After 4.5 days' exposure, capivasertib 480 mg b.i.d. (n = 17) produced significant decreases from baseline versus placebo (n = 11) in pGSK3β (H-score absolute change: -55.3, P = 0.006) and pPRAS40 (-83.8, P < 0.0001), and a decrease in Ki67 (absolute change in percentage positive nuclei: -9.6%, P = 0.031). Significant changes also occurred in secondary signaling biomarker pS6 (-42.3, P = 0.004), while pAKT (and nuclear FOXO3a) also increased in accordance with capivasertib's mechanism (pAKT: 81.3, P = 0.005). At doses of 360 mg b.i.d. (n = 5) and 240 mg b.i.d. (n = 6), changes in primary and secondary biomarkers were also observed, albeit of smaller magnitude. Biomarker modulation was dose and concentration dependent, and no new safety signals were evident.CONCLUSIONS: Capivasertib 480 mg b.i.d. rapidly modulates key biomarkers of the AKT pathway and decreases proliferation marker Ki67, suggesting future potential as an effective therapy in AKT-dependent breast cancers.

U2 - 10.1158/1078-0432.CCR-19-3053

DO - 10.1158/1078-0432.CCR-19-3053

M3 - Article

C2 - 31836609

SN - 1078-0432

JO - Clinical Cancer Research

JF - Clinical Cancer Research

ER -

Proliferation and AKT Activity Biomarker Analyses after Capivasertib (AZD5363) Treatment of Patients with ER+ Invasive Breast Cancer (STAKT)

Abstract

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