Oral PD-L1 inhibitor GS-4224 selectively engages PD-L1 high cells and elicits pharmacodynamic responses in patients with advanced solid tumors

Nicholas Waldron; P Rod Dunbar; Sanjeev Deva; Oh Kyu Yoon; John Ling; Kai-Wen Lin; Dung Thai; Latesh Lad; Ahmed A Othman; Jared M Odegard; Adele Y Wang; Jonathan Nazareno; Edmond Ang

doi:10.1136/jitc-2023-008547

Journal for ImmunoTherapy of Cancer (Apr 2024)

Oral PD-L1 inhibitor GS-4224 selectively engages PD-L1 high cells and elicits pharmacodynamic responses in patients with advanced solid tumors

Nicholas Waldron,
P Rod Dunbar,
Sanjeev Deva,
Oh Kyu Yoon,
John Ling,
Kai-Wen Lin,
Dung Thai,
Latesh Lad,
Ahmed A Othman,
Jared M Odegard,
Adele Y Wang,
Jonathan Nazareno,
Edmond Ang

Affiliations

Nicholas Waldron: University of Auckland, Auckland, New Zealand
P Rod Dunbar: School of Biological Sciences and Maurice Wilkins Centre, The University of Auckland, Auckland, New Zealand
Sanjeev Deva: University of Auckland, Auckland, New Zealand
Oh Kyu Yoon: Gilead Sciences, Inc, Foster City, California, USA
John Ling: Gilead Sciences, Inc, Foster City, California, USA
Kai-Wen Lin: Gilead Sciences, Inc, Foster City, California, USA
Dung Thai: Gilead Sciences, Inc, Foster City, California, USA
Latesh Lad: Gilead Sciences, Inc, Foster City, California, USA
Ahmed A Othman: Clinical Pharmacology, Gilead Sciences Inc, Foster City, California, USA
Jared M Odegard: Biomarker Sciences, Gilead Sciences Inc, Seattle, Washington, USA
Adele Y Wang: Gilead Sciences, Inc, Foster City, California, USA
Jonathan Nazareno: Gilead Sciences, Inc, Foster City, California, USA
Edmond Ang: University of Auckland, Auckland, New Zealand

DOI: https://doi.org/10.1136/jitc-2023-008547
Journal volume & issue: Vol. 12, no. 4

Abstract

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Background Checkpoint inhibitors targeting the programmed cell death 1 (PD-1)/programmed cell death 1 ligand 1 (PD-L1) pathway are effective therapies in a range of immunogenic cancer types. Blocking this pathway with an oral therapy could benefit patients through greater convenience, particularly in combination regimens, and allow flexible management of immune-mediated toxicities.Methods PD-L1 binding activity was assessed in engineered dimerization and primary cell target occupancy assays. Preclinical antitumor activity was evaluated in ex vivo and in vivo human PD-L1-expressing tumor models. Human safety, tolerability, pharmacokinetics, and biomarker activity were evaluated in an open-label, multicenter, sequential dose-escalation study in patients with advanced solid tumors. Biomarkers evaluated included target occupancy, flow cytometric immunophenotyping, plasma cytokine measurements, and T-cell receptor sequencing.Results GS-4224 binding caused dimerization of PD-L1, blocking its interaction with PD-1 and leading to reversal of T-cell inhibition and increased tumor killing in vitro and in vivo. The potency of GS-4224 was dependent on the density of cell surface PD-L1, with binding being most potent on PD-L1–high cells. In a phase 1 dose-escalation study in patients with advanced solid tumors, treatment was well tolerated at doses of 400–1,500 mg once daily. Administration of GS-4224 was associated with a dose-dependent increase in plasma GS-4224 exposure and reduction in free PD-L1 on peripheral blood T cells, an increase in Ki67 among the PD-1-positive T-cell subsets, and elevated plasma cytokines and chemokines.Conclusions GS-4224 is a novel, orally bioavailable small molecule inhibitor of PD-L1. GS-4224 showed evidence of expected on-target biomarker activity, including engagement of PD-L1 and induction of immune-related pharmacodynamic responses consistent with PD-L1 blockade.Trial registration number NCT04049617.

Published in Journal for ImmunoTherapy of Cancer

ISSN: 2051-1426 (Online)
Publisher: BMJ Publishing Group
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://jitc.bmj.com

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