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Randomized Controlled Trial
. 2025 Mar:194:41-47.
doi: 10.1016/j.ygyno.2025.01.015. Epub 2025 Feb 13.

A clinical study of tremelimumab, alone or in combination with olaparib, for recurrent epithelial ovarian cancer

Stéphanie Gaillard  1 Neha Verma  2 Maureen Berg  2 Jeanne Harrison  2 Peng Huang  3 James M Leatherman  2 Michele Doucet  2 Rupashree Sen  2 Aditya Suru  2 Hongyan Cai  2 Jennifer Durham  2 Danijela Jelovac  2 Ashley Cimino-Mathews  4 Christopher Cherry  2 Sudipto Ganguly  2 Leisha A Emens  2
Affiliations
Randomized Controlled Trial

A clinical study of tremelimumab, alone or in combination with olaparib, for recurrent epithelial ovarian cancer

Stéphanie Gaillard et al. Gynecol Oncol. 2025 Mar.

Abstract

Objective: PARP inhibitors may work synergistically to improve the efficacy of immunotherapy in patients with epithelial ovarian cancer (EOC). We performed a parallel-arm study of tremelimumab, alone or with olaparib, in patients with recurrent EOC.

Methods: Eligibility criteria included measurable disease and progression <12 months from last platinum. Participants were randomized to Arm A (tremelimumab monotherapy, 10 mg/kg/dose intravenously [IV]) or Arm B (dose level 1 [DL1] olaparib orally 150 mg twice daily with tremelimumab IV 3 mg/kg/dose and DL2 olaparib orally 150 mg twice daily with tremelimumab IV 10 mg/kg/dose). Primary objectives were safety, change in peripheral ICOS+ T cells, and identification of optimal dose combination.

Results: Among 24 total patients (12 on Arm A, 6 on Arm B-DL1, 6 on Arm B-DL2), the most common grade 3 toxicities were rash (13 %), immune-mediated hepatitis (8 %), and colitis (8 %). No grade ≥ 4 toxicities were identified. No dose-limiting toxicities were identified. One patient (Arm B-DL2) experienced a partial response; no complete responses were observed. Ten patients (7 on Arm A, 2 on Arm B-DL2, and 1 on Arm B-DL1) had a best response of stable disease. There was a significant increase in CD4+ICOS+ and CD8+ICOS+ T cells at both C1D15 and C1D22 in groups treated with tremelimumab IV 10 mg/kg/dose, but not in those treated with tremelimumab 3 mg/kg/dose.

Conclusions: Tremelimumab IV 10 mg/kg/dose with olaparib 150 mg orally twice daily was safe and feasible. Tremelimumab 10 mg/kg/dose (as opposed to 3 mg/kg/dose) was required for immune activation, although this did not translate into clinical responses.

Keywords: Epithelial ovarian cancer; Immune activation; Olaparib; PARP inhibitor; Tremelimumab.

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Conflict of interest statement

Declaration of competing interest As above, funding was provided by AstraZeneca to the institution in support of this study. Unrelated to this manuscript: Stephanie Gaillard has received research funding to institution from Compugen, Genentech/Roche, Clovis/Pharma&, Iovance, Tempest, Tesaro/GSK, Blueprint, Immunogen, Volastra, Beigene, GOG-Foundation, served as a consultant for Immunogen, Novartis, Verastem, and Compugen, participated on an Advisory Board for SignPath Pharma, and serves as a Phase I subcommittee chair for NRG Oncology. Ashley Cimino-Mathews has received research funding to institution from Bristol-Myers Squibb. Christopher Cherry is the owner of CMCC Consulting LLC. Leisha A. Emens is a former employee of Ankyra Therapeutics, has received research funding to institution from AbbVie, AstraZeneca, Bolt Therapeutics, Bristol Meyers Squibb, Compugen, Corvus, CytomX, EMD Serono, Genentech, F Hoffman La Roche, Immune Onc, Merck, Next Cure, Silverback, Takeda, and Tempest, served as a consultant/advisor/speaker for AstraZeneca, BioLineRx, DNAMx, Genentech, F Hoffman La Roche, GPCR, Gilead, Immune Onc, Immunitas, Immutep, Lilly, Macrogenics, Mersana, and Shionogi, is a royalty and patent beneficiary with potential for royalties in the future from Molecuvax, and has publicly traded stocks/stock options from Ankyra Therapeutics. The authors otherwise declare no conflicts of interest.

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