Therapeutic KRAS
            <sup>G12C</sup>
            inhibition drives effective interferon-mediated antitumor immunity in immunogenic lung cancers

Mugarza, Edurne; Maldegem, Febe van; Boumelha, Jesse; Moore, Christopher; Rana, Sareena; Llorian, Miriam; East, Philip; Ambler, Rachel; Anastasiou, Panayiotis; Romero-Clavijo, Pablo; Valand, Karishma; Cole, Megan; Molina‐Arcas, Míriam; Downward, Julian

doi:10.1126/sciadv.abm8780

Cited by 54 publications

(106 citation statements)

References 55 publications

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“…Similarly, in lung cancer, SHP2 inhibitors induce CXCR2 ligands that recruit myeloid derived suppressor cells and limit the response to this therapy 18 . Multiple groups including ours have recently demonstrated the involvement of anti-tumor immunity in the therapeutic response to KRAS G12C inhibitors 10,12,13,15 . We recently reported the involvement of adaptive immunity in the therapeutic response of murine lung cancer cells driven by oncogenic EGFR to the TKI, osimertinib 14 .…”

Section: Quantification Of Lymphocytes and Pmns In Alk+ Patient Biopsiesmentioning

confidence: 96%

“…Our recent published studies demonstrate that EGFR-targeted inhibitors induce an interferon (IFN) response program that varies markedly between distinct EGFR mutant lung cancer cell lines and positively associates with the duration of therapeutic response in EGFR-mutant lung cancer patients 7 . In fact, there is a growing literature supporting the role of host immune cells in overall therapeutic response to precision oncology agents and cytotoxic drugs [8][9][10][11][12][13][14][15][16][17][18][19] . However, the mechanisms whereby TKIs induce factors mediating paracrine signaling to the immune microenvironment, and the contribution to the overall therapeutic response are not well understood.…”

Section: Introductionmentioning

confidence: 99%

“…npj Precision Oncology (2023)15 Published in partnership with The Hormel Institute, University of Minnesota 1234567890():,;…”

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confidence: 99%

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Durable responses to alectinib in murine models of EML4-ALK lung cancer requires adaptive immunity

et al. 2023

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Lung cancers bearing oncogenic EML4-ALK fusions respond to targeted tyrosine kinase inhibitors (TKIs; e.g., alectinib), with variation in the degree of shrinkage and duration of treatment (DOT). However, factors that control this response are not well understood. While the contribution of the immune system in mediating the response to immunotherapy has been extensively investigated, less is known regarding the contribution of immunity to TKI therapeutic responses. We previously demonstrated a positive association of a TKI-induced interferon gamma (IFNγ) transcriptional response with DOT in EGFR-mutant lung cancers. Herein, we used three murine models of EML4-ALK lung cancer to test the role for host immunity in the alectinib therapeutic response. The cell lines (EA1, EA2, EA3) were propagated orthotopically in the lungs of immunocompetent and immunodeficient mice and treated with alectinib. Tumor volumes were serially measured by μCT and immune cell content was measured by flow cytometry and multispectral immunofluorescence. Transcriptional responses to alectinib were assessed by RNAseq and secreted chemokines were measured by ELISA. All cell lines were similarly sensitive to alectinib in vitro and as orthotopic tumors in immunocompetent mice, exhibited durable shrinkage. However, in immunodeficient mice, all tumor models rapidly progressed on TKI therapy. In immunocompetent mice, EA2 tumors exhibited a complete response, whereas EA1 and EA3 tumors retained residual disease that rapidly progressed upon termination of TKI treatment. Prior to treatment, EA2 tumors had greater numbers of CD8+ T cells and fewer neutrophils compared to EA1 tumors. Also, RNAseq of cancer cells recovered from untreated tumors revealed elevated levels of CXCL9 and 10 in EA2 tumors, and higher levels of CXCL1 and 2 in EA1 tumors. Analysis of pre-treatment patient biopsies from ALK+ tumors revealed an association of neutrophil content with shorter time to progression. Combined, these data support a role for adaptive immunity in durability of TKI responses and demonstrate that the immune cell composition of the tumor microenvironment is predictive of response to alectinib therapy.

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Section: Quantification Of Lymphocytes and Pmns In Alk+ Patient Biopsiesmentioning

confidence: 96%

Section: Introductionmentioning

confidence: 99%

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Durable responses to alectinib in murine models of EML4-ALK lung cancer requires adaptive immunity

et al. 2023

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“…However, KRAS G12C inhibition did not sensitize non-immunogenic murine models to immunotherapy. This preclinical finding may guide in selecting patients for combinational clinical trials [ 162 ]. Combinations of G12C inhibitors and immune checkpoint inhibitors are being studied in frontline and refractory settings in NSCLC (NCT04613596, NCT04185883, NCT03600883).…”

Section: Combinations With Immunotherapymentioning

confidence: 99%

Drugging KRAS: current perspectives and state-of-art review

et al. 2022

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After decades of efforts, we have recently made progress into targeting KRAS mutations in several malignancies. Known as the ‘holy grail’ of targeted cancer therapies, KRAS is the most frequently mutated oncogene in human malignancies. Under normal conditions, KRAS shuttles between the GDP-bound ‘off’ state and the GTP-bound ‘on’ state. Mutant KRAS is constitutively activated and leads to persistent downstream signaling and oncogenesis. In 2013, improved understanding of KRAS biology and newer drug designing technologies led to the crucial discovery of a cysteine drug-binding pocket in GDP-bound mutant KRAS G12C protein. Covalent inhibitors that block mutant KRAS G12C were successfully developed and sotorasib was the first KRAS G12C inhibitor to be approved, with several more in the pipeline. Simultaneously, effects of KRAS mutations on tumour microenvironment were also discovered, partly owing to the universal use of immune checkpoint inhibitors. In this review, we discuss the discovery, biology, and function of KRAS in human malignancies. We also discuss the relationship between KRAS mutations and the tumour microenvironment, and therapeutic strategies to target KRAS. Finally, we review the current clinical evidence and ongoing clinical trials of novel agents targeting KRAS and shine light on resistance pathways known so far.

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“…Within this group, the prevalence of targetable oncogenic drivers within the IS phenotype, such as KRAS G12C, may represent the potential for novel ICI combination therapies. 4 These findings further highlight the importance of adding TME analysis to comprehensive biomarker testing in NSCLC…”

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confidence: 90%

159 Xerna tumor microenvironment subtypes as a biomarker in lung cancer patients

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et al. 2022

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Therapeutic KRAS ^G12C inhibition drives effective interferon-mediated antitumor immunity in immunogenic lung cancers

Cited by 54 publications

References 55 publications

Durable responses to alectinib in murine models of EML4-ALK lung cancer requires adaptive immunity

Durable responses to alectinib in murine models of EML4-ALK lung cancer requires adaptive immunity

Drugging KRAS: current perspectives and state-of-art review

159 Xerna tumor microenvironment subtypes as a biomarker in lung cancer patients

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Therapeutic KRAS G12C inhibition drives effective interferon-mediated antitumor immunity in immunogenic lung cancers

Cited by 54 publications

References 55 publications

Durable responses to alectinib in murine models of EML4-ALK lung cancer requires adaptive immunity

Durable responses to alectinib in murine models of EML4-ALK lung cancer requires adaptive immunity

Drugging KRAS: current perspectives and state-of-art review

159 Xerna tumor microenvironment subtypes as a biomarker in lung cancer patients

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Therapeutic KRAS ^G12C inhibition drives effective interferon-mediated antitumor immunity in immunogenic lung cancers