Resistance to checkpoint blockade therapy through inactivation of antigen presentation

Sade-Feldman, Moshe; Jiao, Yunxin; Chen, Jonathan; Rooney, Michael S.; Barzily-Rokni, Michal; Eliane, Jean Pierre; Bjorgaard, Stacey L.; Hammond, Marc R.; Vitzthum, Hans; Blackmon, Shauna; Frederick, Dennie T.; Hazar-Rethinam, Mehlika; Nadres, Brandon; Seventer, Emily E. Van; Shukla, Sachet A.; Yizhak, Keren; Ray, John J.; Rosebrock, Daniel; Livitz, Dimitri; Adalsteinsson, Viktor A.; Getz, Gad; Duncan, Lyn M.; Li, Bo; Corcoran, Ryan B.; Lawrence, Donald P.; Stemmer‐Rachamimov, Anat; Boland, Genevieve M.; Landau, Dan A.; Flaherty, Keith T.; Sullivan, Ryan J.; Hacohen, Nir

doi:10.1038/s41467-017-01062-w

Cited by 708 publications

(598 citation statements)

References 44 publications

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“…Among the cancer‐related markers, we observed the expression of β2M, STAT3, STING, and β‐catenin (Figure B). The expression of β2M suggests that tumour antigens are presented via HLA‐A in these tumour areas, thus supporting the efficacy of ICI . Total levels of STAT3 were elevated, but not in its activated phosphorylated form (pY705), which regulates gene transcription for modulation of immunosuppressive factors .…”

Section: Resultsmentioning

confidence: 88%

Loss of BAP1 expression is associated with an immunosuppressive microenvironment in uveal melanoma, with implications for immunotherapy development

Figueiredo

Kalirai

Sacco

et al. 2020

The Journal of Pathology

101

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Immunotherapy using immune checkpoint inhibitors (ICIs) induces durable responses in many metastatic cancers. Metastatic uveal melanoma (mUM), typically occurring in the liver, is one of the most refractory tumours to ICIs and has dismal outcomes. Monosomy 3 (M3), polysomy 8q, and BAP1 loss in primary uveal melanoma (pUM) are associated with poor prognoses. The presence of tumour‐infiltrating lymphocytes (TILs) within pUM and surrounding mUM – and some evidence of clinical responses to adoptive TIL transfer – strongly suggests that UMs are indeed immunogenic despite their low mutational burden. The mechanisms that suppress TILs in pUM and mUM are unknown. We show that BAP1 loss is correlated with upregulation of several genes associated with suppressive immune responses, some of which build an immune suppressive axis, including HLA‐DR, CD38, and CD74. Further, single‐cell analysis of pUM by mass cytometry confirmed the expression of these and other markers revealing important functions of infiltrating immune cells in UM, most being regulatory CD8+ T lymphocytes and tumour‐associated macrophages (TAMs). Transcriptomic analysis of hepatic mUM revealed similar immune profiles to pUM with BAP1 loss, including the expression of IDO1. At the protein level, we observed TAMs and TILs entrapped within peritumoural fibrotic areas surrounding mUM, with increased expression of IDO1, PD‐L1, and β‐catenin (CTNNB1), suggesting tumour‐driven immune exclusion and hence the immunotherapy resistance. These findings aid the understanding of how the immune response is organised in BAP1 − mUM, which will further enable functional validation of detected biomarkers and the development of focused immunotherapeutic approaches. © 2020 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland.

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Section: Resultsmentioning

confidence: 88%

Loss of BAP1 expression is associated with an immunosuppressive microenvironment in uveal melanoma, with implications for immunotherapy development

Figueiredo

Kalirai

Sacco

et al. 2020

The Journal of Pathology

101

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“…12,13,27 Mutations in JAK1 and JAK2 and defects in INF-c signaling have been implicated in resistance to anti-CTLA-4 and anti-PD-1 therapy. 10 Glucocorticoids extensively modify cytokine signaling and can inhibit the interleukin-2 and INF-c pathways. 28 Mutations in b-2 microglobulin also appear to impart resistance to treatment with CTLA-4 and PD-1 antibodies.…”

Section: Discussionmentioning

confidence: 99%

“…[6][7][8] Optimal management strategies for patients with primary hypophysitis and checkpoint inhibitor (CPI)-associated hypophysitis are poorly defined; therefore, treatment patterns, including glucocorticoid dosages, vary. [10][11][12] High doses of glucocorticoids inhibit the immune response, including some pathways linked to CPI resistance. 9 Defects in the immune response are associated with primary and acquired resistance to CPIs.…”

Section: Introductionmentioning

confidence: 99%

High‐dose glucocorticoids for the treatment of ipilimumab‐induced hypophysitis is associated with reduced survival in patients with melanoma

Faje

Lawrence

Flaherty

et al. 2018

Cancer

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351

293

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“…This group found β2‐microglobulin gene mutations and loss of heterozygosity (LOH) at baseline in a cohort of melanoma samples taken from patients with intrinsic resistance to anti‐CTLA‐4 and anti‐PD‐1 therapy . β2‐microglobulin mutations have commonly been observed enriched in patients with disease relapse . Other study found enriched cellular ( FYB , CXCL9, CD69, CD8A, CARD11 , and CD5 ) and humoral (immunoglobulin heavy chain variants) immune responses in the group with clinical benefit to ipilimumab therapy …”

Section: Genomic Signatures Predicting Response To Anti‐ctla‐4 and Pdmentioning

confidence: 99%

OMIC signatures to understand cancer immunosurveillance and immunoediting: Melanoma and immune cells interplay in immunotherapy

León‐Letelier

Bonifaz

Fuentes‐Pananá

2019

Journal of Leukocyte Biology

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Melanoma is the deadliest form of skin cancer. Cutaneous melanomas usually originate from exposure to the mutagenic effects of ultraviolet radiation, and as such they exhibit the highest rate of somatic mutations than any other human cancer, and an extensive expression of neoantigens concurrently with a dense infiltrate of immune cells. The coexistence of high immunogenicity and high immune cell infiltration may sound contradictory for cancers carrying a gloomy outcome. However, recent studies have unveiled a variety of immunosuppressive mechanisms that often permeate the tumor microenvironment and that are responsible for tumor escaping from immunosurveillance mechanisms. Nonetheless, this particular immune profile has opened a new window of treatments based on immunotherapy that have significantly improved the clinical outcome of melanoma patients. Still, positive and complete therapy responses have been limited, and this particular cancer continues to be a major clinical challenge. The transcriptomic signatures of those patients with clinical benefit and those with progressive disease have provided a more complete picture of the universe of interactions between the tumor and the immune system. In this review, we integrate the results of the immunotherapy clinical trials to discuss a novel understanding of the mechanisms guiding cancer immunosurveillance and immunoediting. A clear notion of the cellular and molecular processes shaping how the immune system and the tumor are continuously coevolving would result in the rational design of combinatory therapies aiming to counteract the signaling pathways and cellular processes responsible for immunoescape mechanisms and provide clinical benefit to immunotherapy nonresponsive patients.

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Resistance to checkpoint blockade therapy through inactivation of antigen presentation

Cited by 708 publications

References 44 publications

Loss of BAP1 expression is associated with an immunosuppressive microenvironment in uveal melanoma, with implications for immunotherapy development

Loss of BAP1 expression is associated with an immunosuppressive microenvironment in uveal melanoma, with implications for immunotherapy development

High‐dose glucocorticoids for the treatment of ipilimumab‐induced hypophysitis is associated with reduced survival in patients with melanoma

OMIC signatures to understand cancer immunosurveillance and immunoediting: Melanoma and immune cells interplay in immunotherapy

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