Mutations Associated with Acquired Resistance to PD-1 Blockade in Melanoma

Zaretsky, Jesse M.; García-Díaz, Ángel; Shin, Daniel Sanghoon; Escuin-Ordinas, Helena; Hugo, Willy; Hu‐Lieskovan, Siwen; Torrejon, Davis Y.; Abril-Rodríguez, Gabriel; Sandoval, Salemiz; Barthly, Lucas; Saco, Justin D.; Moreno, Blanca Homet; Mezzadra, Riccardo; Chmielowski, Bartosz; Ruchalski, Kathleen; Shintaku, I. Peter; Sanchez, Phillip J.; Puig-Saus, Cristina; Cherry, Grace; Seja, Elizabeth; Kong, Xiangju; Pang, Jinfeng; Berent-Maoz, Beata; Comı́n-Anduix, Begoña; Graeber, Thomas G.; Tumeh, Paul C.; Schumacher, Ton N.; Lo, Roger S.; Ribas, Antoni

doi:10.1056/nejmoa1604958

Cited by 2,485 publications

(2,324 citation statements)

References 38 publications

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“…Similarly, blocking PD‐1 in patients with non‐small‐cell lung cancer prolonged progression‐free survival, but cancer nevertheless progressed in almost all patients 25. The most direct consistency with the present study's demonstration of a transient immunological response to PD‐1 blockade is demonstration of acquired resistance to PD‐1 antibody treatment in melanoma patients 43. This development of resistance was shown to be associated with alterations interferon receptor signaling and in antigen presentation.…”

Section: Discussionsupporting

confidence: 85%

Transient immunological and clinical effectiveness of treating mice bearing premalignant oral lesions with PD‐1 antibodies

Levingston

Young

2017

Intl Journal of Cancer

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A carcinogen‐induced premalignant oral lesion model that progresses to oral cancer was used to examine the impact of blocking PD‐1 on cytokine expression and on progression of lesions to cancer. The results of this study show increased production of IL‐2 and the inflammatory cytokines IL‐6, IL‐17 and TNF‐α by spleen cells of lesion‐bearing mice that were treated with PD‐1 antibody for 1 week compared to cytokine production by spleen cells of lesion‐bearing mice treated with control antibody. Production of IFN‐γ increased at 3 weeks of PD‐1 antibody treatment, although production of the other Th1 and inflammatory mediators declined. By 5 weeks, levels of these cytokines declined for both control and PD‐1 antibody‐treated mice. Flow cytometric analysis for IFN‐γ‐expressing cells showed shifts in CD4+ cells expressing IFN‐γ consistent with the changes in cytokine secretion. Whether or not treatment generated reactivity to lesions or HNSCC was determined. Spleen cells from PD‐1 antibody‐treated mice were stimulated by lysates of premalignant lesion and HNSCC tongue tissues to produce increased levels of Th1 and select inflammatory cytokines early in the course of PD‐1 antibody treatment. However, with continued treatment, reactivity to lesion and HNSCC lysates declined. Analysis of clinical response to treatment suggested an early delay in lesion progression but, with continued treatment, lesions in PD‐1 antibody‐treated mice progressed to the same degree as in control antibody‐treated mice. Overall, these results show an early beneficial response to PD‐1 antibody treatment, which then fails with continued treatment and lesion progression.

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Section: Discussionsupporting

confidence: 85%

Transient immunological and clinical effectiveness of treating mice bearing premalignant oral lesions with PD‐1 antibodies

Levingston

Young

2017

Intl Journal of Cancer

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“…A recent study found that mutations that affected the antigen presentation and the sensitivity of tumor cells to T cell-derived IFNs could cause acquired resistance to anti-PD1 therapy. 4,48 To overcome, or potentially prevent, the development of acquired immunotherapeutic resistance, a very large number of trials are now underway that combine checkpoint blockade with a wide range of other agents. 10 In many cases, the combination under study appears to be lacking any strong mechanistic rationale for that particular combination.…”

Section: Discussionmentioning

confidence: 99%

Combination with SGT-53 overcomes tumor resistance to a checkpoint inhibitor

et al. 2018

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The tumor suppressor p53 responds to genotoxic and oncogenic stresses by inducing cell cycle arrest and apoptosis. Recent studies suggest that p53 also participates in the regulation of cellular immune responses. Here, we have investigated the potential of p53 gene therapy to augment immune checkpoint inhibition by combining an anti-programmed cell death protein 1 (PD1) antibody with SGT-53, our investigational nanomedicine carrying a plasmid encoding human wild-type p53. In three syngeneic mouse tumor models examined including a breast cancer, a non-small cell lung carcinoma, and a glioblastoma, SGT-53 sensitized otherwise refractory tumors to anti-PD1 antibody. The involvement of p53 in enhancing anti-PD1 immunotherapy appears to be multifaceted, since SGT-53 treatment increased tumor immunogenicity, enhanced both innate and adaptive immune responses, and reduced tumor-induced immunosuppression in a 4T1 breast tumor model. In addition, SGT-53 alleviates a fatal xenogeneic hypersensitivity associated with the anti-PD1 antibody in this model. Our data suggest that restoring p53 function by SGT-53 is able to boost anti-tumor immunity to augment anti-PD1 therapy by sensitizing tumors otherwise insensitive to anti-PD1 immunotherapy while reducing immune-related adverse events.

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“…Analyses of tumours with a very low IFNγ-associated geneexpression score, or a 'non-T-cell-inflamed' tumour microenvironment have revealed roles for activation of the WNT/β-catenin-signalling pathway 145 , and an enrichment for mutations in PTEN 146 in immune evasion. Deleterious mutations in the genes encoding JAK1 and JAK2 (which are involved in IFNγ signalling), or β 2 microglobulin (an MHC class I subunit), as well as loss of expression of interferon regulatory factor 1 (IRF1) have also been described in anti-PD-1-antibody-resistant patient samples and cell lines 147,148 . These intratumoural changes are associated with deficits in autophagy, antigen presentation, and the type I interferon response, suggesting that rational drug combinations should be explored to either suppress these pathways using β-catenin or PI3Kβ inhibitors, and/or amplify antigen presentation, perhaps via an approach such as FLT3-ligand agonism.…”

Section: Braf-mek-inhibitor Resistance and Biomarkersmentioning

confidence: 99%