Vemurafenib enhances MHC induction inBRAFV600Ehomozygous melanoma cells

Sapkota, Bishu; Hill, Charles E.; Pollack, Brian P.

doi:10.4161/onci.22890

Cited by 130 publications

(118 citation statements)

References 44 publications

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“…Therapeutics augmenting NLRC5 activity could compensate for this deficit by breaking cancer immune evasion in a broad range of tumor types. Interestingly, it has been reported that currently used therapies, such as an EGF receptor inhibitor (cetuximab) or a B-Raf inhibitor (vemurafenib), enhance MHC class I expression via IFN-γ (35,36). Therefore, these currently available therapies, originally designed to disrupt oncogenic signaling, may mediate their effects in part via the NLRC5-dependent MHC class I pathway.…”

Section: Discussionmentioning

confidence: 99%

NLRC5/MHC class I transactivator is a target for immune evasion in cancer

Yoshihama

Roszik

Downs

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

221

242

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Cancer cells develop under immune surveillance, thus necessitating immune escape for successful growth. Loss of MHC class I expression provides a key immune evasion strategy in many cancers, although the molecular mechanisms remain elusive. MHC class I transactivator (CITA), known as "NLRC5" [NOD-like receptor (NLR) family, caspase recruitment (CARD) domain containing 5], has recently been identified as a critical transcriptional coactivator of MHC class I gene expression. Here we show that the MHC class I transactivation pathway mediated by CITA/NLRC5 constitutes a target for cancer immune evasion. In all the 21 tumor types we examined, NLRC5 expression was highly correlated with the expression of MHC class I, with cytotoxic T-cell markers, and with genes in the MHC class I antigen-presentation pathway, including LMP2/LMP7, TAP1, and β2-microglobulin. Epigenetic and genetic alterations in cancers, including promoter methylation, copy number loss, and somatic mutations, were most prevalent in NLRC5 among all MHC class I-related genes and were associated with the impaired expression of components of the MHC class I pathway. Strikingly, NLRC5 expression was significantly associated with the activation of CD8 + cytotoxic T cells and patient survival in multiple cancer types. Thus, NLRC5 constitutes a novel prognostic biomarker and potential therapeutic target of cancers.MHC class I | CITA | cancer | immune evasion | NLRC5

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Section: Discussionmentioning

confidence: 99%

NLRC5/MHC class I transactivator is a target for immune evasion in cancer

Yoshihama

Roszik

Downs

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

221

242

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“…Molecularly targeted agents are also being combined with immune checkpoint inhibitors. BRAF inhibition, which is FDA-approved for the treatment of metastatic melanoma expressing the activating BRAF V600E mutation, has been shown to increase MHC expression, tumor antigen presentation, and T-cell infiltration (98)(99)(100)(101)(102). Similarly, MEK inhibitors have been shown to improve CD8+ T-cell activity in preclinical models in combination with PD-1 blockade (103).…”

Section: Future Directionsmentioning

confidence: 99%

Immune Checkpoint Inhibitors in the Treatment of Melanoma: From Basic Science to Clinical Application

Rausch¹,

Hastings

2017

Cutaneous Melanoma: Etiology and Therapy

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Abstract:Immune checkpoint blockade has revolutionized the treatment of patients with advanced melanoma and many other cancers. Blockade of inhibitory receptors, CTLA-4 and PD-1, enhances T-cell-mediated antitumor immune responses, leading to improved survival and durable responses in patients. Based on their mechanism of action, immune checkpoint inhibitors can also induce immune-related adverse events that require careful monitoring and prompt treatment. Despite these successes, only a fraction of patients benefit from immune checkpoint blockade. Basic science approaches and clinical experience are defining predictive biomarkers to identify patients most likely to respond to therapy as well as mechanisms of resistance that limit responses in certain tumors or shorten the duration of response. New approaches and combination therapies are under development to broaden the clinical impact of immune checkpoint blockade by overcoming resistance to therapy and limiting adverse events.

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“…C recurrent Grade II gliomas (NCT02193347); (6) the safety and efficacy of peptides derived from indoleamine 2,3-dioxygenase 1 (IDO1) [202][203][204][205][206] combined with the FDA-approved immune checkpoint blocker ipilimumab (also known as Yervoy TM ) [207][208][209][210][211][212] and vemurafenib (an FDA-approved inhibitor of mutant BRAF) [213][214][215][216][217] are being evaluated in melanoma patients (NCT02077114); (7) the therapeutic profile of a CMP targeting ganglioside GD2 and the so-called Lewis Y antigen (2 non-peptide TAAs), [218][219][220] employed as a PADRE-and Montanide ISA-51-adjuvanted intervention in combination with standard chemotherapy, is being assessed in breast carcinoma patients (NCT02229084); (8) full-length, recombinant cancer/ testis antigen 1B (CTAG1B, best known as NY-ESO-1)…”

Section: Gm-csf-adjuvanted Standalone Interventions In Subjects Bearimentioning

confidence: 99%