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. 2020 Nov 9;22(Suppl 2):ii44. doi: 10.1093/neuonc/noaa215.179

CTNI-12. PRELIMINARY RESULTS OF THE ABEMACICLIB ARM IN THE INDIVIDUALIZED SCREENING TRIAL OF INNOVATIVE GLIOBLASTOMA THERAPY (INSIGHT): A PHASE II PLATFORM TRIAL USING BAYESIAN ADAPTIVE RANDOMIZATION

Patrick Wen 1, Lorenzo Trippa 1, Eudocia Lee 1, Geoffrey Fell 1, Rifaquat Rahman 2, Isabel Arrillaga-Romany 3, Mehdi Touat 4, Christine McCluskey 1, Jennifer Brunno 1, Sarah Gaffey 5, Jan Drappatz 6, Andrew Lassman 7, Evanthia Galanis 8, Manmeet Ahluwalia 9, Howard Colman 10, Louis Nabors 11, Jaroslaw Hepel 12, Heinrich Elinzano 12, David Schiff 13, Ugonma Chukwueke 1, Rameen Beroukhim 1, Lakshmi Nayak 1, Jose Mcfaline-Figueroa 1, Tracy Batchelor 14, Mikael Rinne 1, Thomas Kaley 15, Christine Lu-Emerson 16, Wenya Linda Bi 17, Omar Arnaout 17, Pier-Paolo Peruzzi 14, Lisa Doherty 3, Daphne Haas-Kogan 18, Shyam Tanguturi 1, Daniel Cagney 14, Ayal A Aizer 19, Mary Welch 20, Maria Lavallee 1, Brittany Fisher-Longden 1, Shanna Dowling 1, Jack Geduldig 1, Sandro Santagata 21, David Meredith 21, E Antonio Chiocca 22, David Reardon 23, Keith Ligon 21, Brian Alexander 1
PMCID: PMC7650442

Abstract

BACKGROUND

The cyclin D-CDK4/6-Rb pathway is activated in most glioblastomas. Abemaciclib is a potent CDK4/6 inhibitor with good brain penetration approved for ER/PR/HER2- breast cancer. In order to efficiently evaluate the potential impact of abemaciclib on overall survival (OS) in newly diagnosed glioblastoma and to simultaneously develop information regarding potential genomic biomarker associations, abemaciclib was included as an arm on the Individualized Screening Trial of Innovative Glioblastoma Therapy (INSIGhT) trial. INSIGhT is a phase II platform trial using response adaptive randomization and deep genomic profiling to more efficiently test experimental agents in MGMT unmethylated glioblastoma and potentially accelerate identification of novel therapies for phase III testing. Initial randomization was equal between abemaciclib, control, and two other experimental arms but subsequent randomization was adapted based on efficacy as determined by progression-free survival (PFS). Ineffective arms were discontinued and new arms added by protocol amendment. We report preliminary results for the abemaciclib arm which has completed accrual.

METHODS

Patients with newly diagnosed MGMT-unmethylated glioblastoma were randomized to receive either radiotherapy with concomitant and adjuvant temozolomide at standard doses or standard radiochemotherapy followed by adjuvant abemaciclib (150–200 mg orally BID) without temozolomide. Treatment continued until progression or development of unacceptable toxicities. The primary endpoint was OS. Association between abemaciclib efficacy and cyclin D-CDK4/6-Rb pathway genomic alterations was also investigated.

RESULTS

There were 123 patients (50 control; 73 treated with abemaciclib). Abemaciclib was generally well-tolerated with no new toxicity signals identified. PFS was significantly longer (p=0.03, logrank test) with abemaciclib (median 6.31 months 95% CI [5.29, 8.18]) compared to the control arm (5.16 months 95% CI [4.37, 6.28]). 28/50 control and 36/73 abemaciclib patients remain alive.

CONCLUSION

Preliminary analysis suggests that abemaciclib increases PFS compared to control. Updated toxicity, PFS and survival data and potential genomic biomarker associations will be presented.

Articles from Neuro-Oncology are provided here courtesy of Society for Neuro-Oncology and Oxford University Press

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