Combined Nivolumab and Ipilimumab or Monotherapy in Untreated Melanoma

Larkin, James; Chiarion-Sileni, Vanna; González, René; Grob, Jean-Jacques; Cowey, C. Lance; Lao, Christopher D.; Schadendorf, Dirk; Dummer, Reinhard; Smylie, Michael; Rutkowski, Piotr; Ferrucci, Pier Francesco; Hill, Andrew; Wagstaff, John; Carlino, Matteo S.; Haanen, John B.A.G.; Maio, Michele; Márquez-Rodas, Iván; McArthur, Grant A.; Ascierto, Paolo A.; Long, Georgina V.; Callahan, Margaret K.; Postow, Michael A.; Grossmann, Kenneth F.; Sznol, Mario; Dréno, Brigitte; Bastholt, Lars; Yang, Allison L.; Rollin, Linda; Horak, Christine E.; Hodi, F. Stephen; Wolchok, Jedd D.

doi:10.1056/nejmoa1504030

Cited by 6,694 publications

(5,653 citation statements)

References 21 publications

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“…Mirroring findings in the clinic, 4,10 some subjects (mice) did not respond to immunotherapy at all, while others experienced slower tumor growth or eradication of the tumor altogether. RON inhibition alone (RON i single agent) did not result in appreciable clinical benefit, and it did not significantly reduce tumor growth rate compared to the vehicle group (Figure 3a-c).…”

Section: Resultsmentioning

confidence: 93%

“…Unfortunately, grade 3 and 4 treatment-related adverse events were observed in 55% of patients, twice as frequently compared to single-treatment arms. 4 These data emphasize that discovering cooperating immune pathways that can be safely modulated to provide synergistic clinical benefit will be a key step in improving immunotherapy outcomes.…”

Section: Discussionmentioning

confidence: 99%

“…Blocking immune checkpoints with “checkpoint inhibitor” therapy was shown to be a powerful approach to release T cell inhibition in preclinical models and is now approved by the FDA for the treatment of certain cancers. 3,4 In some cases, long-term durable responses and complete remissions are achieved with checkpoint inhibition, but only a fraction of patients mount a productive anti-tumor immune response and benefit from the treatment. To this end, numerous approaches have been proposed to potentiate responses to immunotherapy including combination treatment with various immune-modulating drugs, or co-treatment with chemotherapy or radiotherapy.…”

Section: Introductionmentioning

confidence: 99%

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Inhibition of RON kinase potentiates anti-CTLA-4 immunotherapy to shrink breast tumors and prevent metastatic outgrowth

et al. 2018

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The advent of immune checkpoint blockade as a new strategy for immunotherapy has changed the outlook for many aggressive cancers. Although complete tumor eradication is attainable in some cases, durable clinical responses are observed only in a small fraction of patients, underlining urgent need for improvement. We previously showed that RON, a receptor tyrosine kinase expressed in macrophages, suppresses antitumor immune responses, and facilitates progression and metastasis of breast cancer. Here, we investigated the molecular changes that occur downstream of RON activation in macrophages, and whether inhibition of RON can cooperate with checkpoint immunotherapy to eradicate tumors. Activation of RON by its ligand, MSP, altered the gene expression profile of macrophages drastically and upregulated surface levels of CD80 and PD-L1, ligands for T-cell checkpoint receptors CTLA-4 and PD-1. Genetic deletion or pharmacological inhibition of RON in combination with anti-CTLA-4, but not with anti-PD-1, resulted in improved clinical responses against orthotopically transplanted tumors compared to single-agent treatment groups, resulting in complete tumor eradication in 46% of the animals. Positive responses to therapy were associated with higher levels of T-cell activation markers and tumor-infiltrating lymphocytes. Importantly, co-inhibition of RON and anti-CTLA-4 was also effective in clearing metastatic breast cancer cells in lungs, resulting in clinical responses in nearly 60% of the mice. These findings suggest that RON inhibition can be a novel approach to potentiate responses to checkpoint immunotherapy in breast cancer.

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Section: Resultsmentioning

confidence: 93%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Inhibition of RON kinase potentiates anti-CTLA-4 immunotherapy to shrink breast tumors and prevent metastatic outgrowth

et al. 2018

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“…However, studies with animal models and cancer patients have also shown that combining antibody blockade of the PD‐1/PD‐L1 axis with other forms of immunotherapy can lead to more meaningful clinical responses 32, 33, 34, 35. Approaches to block checkpoint signals have not been previously tested for their capacity to prevent premalignant lesion progression to cancer, despite indications of subjects with premalignant lesions having increased expression of PD‐L1 and PD‐1 + cells36, 37.…”

Section: Discussionmentioning

confidence: 99%

“…A murine model of cervical cancer that showed antibody treatment to block PD‐1 was not sufficient to stimulate T‐cell reactivity or to increase survival of tumor‐bearing mice, instead showed effectiveness when used in combination with agonistic antibody to the co‐stimulatory receptor OX40 33. Combining nivolumab (anti‐PD‐1) and ipilimumab (anti‐CTLA‐4) antibody treatments targeting two distinct immune checkpoints resulted in greater clinical response than when used alone 34, 35…”

Section: Introductionmentioning

confidence: 99%

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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Immune Checkpoint Blockade in Cancer Therapy

Allison

2015

JAMA

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While there are exciting examples of successful clinical strategies to mobilize the immune system to attack cancer cells, overall the results have been disappointing. One reason for less than optimal results is that until recently insufficient attention has been paid to multiple inhibitory mechanisms that serve to shape the immune response and minimize harm to normal tissues and can frustrate generation of effective anti-tumor responses. The prototype of these inhibitory pathways is CTLA-4, which upon engaging its ligands B7-1 and B7-2 limits T cell proliferation. We have shown that blockade of CTLA-4 can greatly enhance anti-tumor responses in a number of experimental tumors in mice. Recent studies of the mechanisms involved suggest that CTLA-blockade enhances anti-tumor responses by blocking a cell intrinsic inhibitory pathway in effector T cell, thus rendering them resistant to inhibition by Treg cells.Anti-CTLA-4 (MDX-010, Ipilimumab) is being co-developed by Medarex, Inc. and Bristol Meyers Squibb. The results of clinical trials in over 1700 patients have demonstrated objective, durable responses with manageable in a high fraction of melanoma, renal prostate, ovarian, and pancreatic cancer.More recently we and others have shown that there are additional B7 family members that limit T cell responses at distinct stages, and that at least three of these are also expressed by tumor cells. Thus the extended B7 family offers a number of targets for immune checkpoint blockade in the treatment of cancer. Finally, recent studies have shown that tumors multiple coding mutations which should result in generation of multiple neoantigens. I will discuss the implications for this to immunologically based as well as conventional cancer therapy.

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Combined Nivolumab and Ipilimumab or Monotherapy in Untreated Melanoma

Cited by 6,694 publications

References 21 publications

Inhibition of RON kinase potentiates anti-CTLA-4 immunotherapy to shrink breast tumors and prevent metastatic outgrowth

Inhibition of RON kinase potentiates anti-CTLA-4 immunotherapy to shrink breast tumors and prevent metastatic outgrowth

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

Immune Checkpoint Blockade in Cancer Therapy

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