Combining RAS(ON) G12C-selective inhibitor with SHP2 inhibition sensitises lung tumours to immune checkpoint blockade

Panayiotis Anastasiou; Christopher Moore; Sareena Rana; Mona Tomaschko; Claire E. Pillsbury; Andrea de Castro; Jesse Boumelha; Edurne Mugarza; Sophie de Carné Trécesson; Ania Mikolajczak; Cristina Blaj; Robert Goldstone; Jacqueline A. M. Smith; Elsa Quintana; Miriam Molina-Arcas; Julian Downward

doi:10.1038/s41467-024-52324-3

Nature Communications (Sep 2024)

Combining RAS(ON) G12C-selective inhibitor with SHP2 inhibition sensitises lung tumours to immune checkpoint blockade

Panayiotis Anastasiou,
Christopher Moore,
Sareena Rana,
Mona Tomaschko,
Claire E. Pillsbury,
Andrea de Castro,
Jesse Boumelha,
Edurne Mugarza,
Sophie de Carné Trécesson,
Ania Mikolajczak,
Cristina Blaj,
Robert Goldstone,
Jacqueline A. M. Smith,
Elsa Quintana,
Miriam Molina-Arcas,
Julian Downward

Affiliations

Panayiotis Anastasiou: Oncogene Biology Laboratory, Francis Crick Institute
Christopher Moore: Oncogene Biology Laboratory, Francis Crick Institute
Sareena Rana: Oncogene Biology Laboratory, Francis Crick Institute
Mona Tomaschko: Oncogene Biology Laboratory, Francis Crick Institute
Claire E. Pillsbury: Oncogene Biology Laboratory, Francis Crick Institute
Andrea de Castro: Oncogene Biology Laboratory, Francis Crick Institute
Jesse Boumelha: Oncogene Biology Laboratory, Francis Crick Institute
Edurne Mugarza: Oncogene Biology Laboratory, Francis Crick Institute
Sophie de Carné Trécesson: Oncogene Biology Laboratory, Francis Crick Institute
Ania Mikolajczak: Experimental Histopathology, Francis Crick Institute
Cristina Blaj: Revolution Medicines, Inc.
Robert Goldstone: Bioinformatics & Biostatistics Science Technology Platform, Francis Crick Institute
Jacqueline A. M. Smith: Revolution Medicines, Inc.
Elsa Quintana: Revolution Medicines, Inc.
Miriam Molina-Arcas: Oncogene Biology Laboratory, Francis Crick Institute
Julian Downward: Oncogene Biology Laboratory, Francis Crick Institute

DOI: https://doi.org/10.1038/s41467-024-52324-3
Journal volume & issue: Vol. 15, no. 1
pp. 1 – 17

Abstract

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Abstract Mutant selective drugs targeting the inactive, GDP-bound form of KRASG12C have been approved for use in lung cancer, but resistance develops rapidly. Here we use an inhibitor, (RMC-4998) that targets RASG12C in its active, GTP-bound form, to treat KRAS mutant lung cancer in various immune competent mouse models. RAS pathway reactivation after RMC-4998 treatment could be delayed using combined treatment with a SHP2 inhibitor, which not only impacts tumour cell RAS signalling but also remodels the tumour microenvironment to be less immunosuppressive. In an immune inflamed model, RAS and SHP2 inhibitors in combination drive durable responses by suppressing tumour relapse and inducing development of immune memory. In an immune excluded model, combined RAS and SHP2 inhibition sensitises tumours to immune checkpoint blockade, leading to efficient tumour immune rejection. These preclinical results demonstrate the potential of the combination of RAS(ON) G12C-selective inhibitors with SHP2 inhibitors to sensitize tumours to immune checkpoint blockade.

Published in Nature Communications

ISSN: 2041-1723 (Online)
Publisher: Nature Portfolio
Country of publisher: United Kingdom
LCC subjects: Science
Website: https://www.nature.com/ncomms/

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