MHC Class I Loss Is a Frequent Mechanism of Immune Escape in Papillary Thyroid Cancer That Is Reversed by Interferon and Selumetinib Treatment<i>In Vitro</i>

Angell, Trevor E.; Lechner, Melissa G.; Jang, Julie K.; LoPresti, Jonathan S.; Epstein, Alan L.

doi:10.1158/1078-0432.ccr-14-0879

Cited by 125 publications

(87 citation statements)

References 45 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Due to the complexity of the HLA genetic system and the difficulties in measuring the HLA-I expression in human tissue, the available information on tumor HLA-I expression does not always reflect the real pattern and the character of HLA-I alterations [15]. Additional detailed analysis is required to obtain a more accurate picture of HLA-I defects and the underlying molecular mechanisms in a given type of cancer.…”

Section: Tumor Immune Escape and Hla Class I Lossmentioning

confidence: 99%

The Escape of Cancer from T Cell-Mediated Immune Surveillance: HLA Class I Loss and Tumor Tissue Architecture

et al. 2017

View full text Add to dashboard Cite

Tumor immune escape is associated with the loss of tumor HLA class I (HLA-I) expression commonly found in malignant cells. Accumulating evidence suggests that the efficacy of immunotherapy depends on the expression levels of HLA class I molecules on tumors cells. It also depends on the molecular mechanism underlying the loss of HLA expression, which could be reversible/“soft” or irreversible/“hard” due to genetic alterations in HLA, β2-microglobulin or IFN genes. Immune selection of HLA-I negative tumor cells harboring structural/irreversible alterations has been demonstrated after immunotherapy in cancer patients and in experimental cancer models. Here, we summarize recent findings indicating that tumor HLA-I loss also correlates with a reduced intra-tumor T cell infiltration and with a specific reorganization of tumor tissue. T cell immune selection of HLA-I negative tumors results in a clear separation between the stroma and the tumor parenchyma with leucocytes, macrophages and other mononuclear cells restrained outside the tumor mass. Better understanding of the structural and functional changes taking place in the tumor microenvironment may help to overcome cancer immune escape and improve the efficacy of different immunotherapeutic strategies. We also underline the urgent need for designing strategies to enhance tumor HLA class I expression that could improve tumor rejection by cytotoxic T-lymphocytes (CTL).

show abstract

Section: Tumor Immune Escape and Hla Class I Lossmentioning

confidence: 99%

The Escape of Cancer from T Cell-Mediated Immune Surveillance: HLA Class I Loss and Tumor Tissue Architecture

et al. 2017

View full text Add to dashboard Cite

show abstract

“…35 In TC, type I and type II IFNs in vitro induced the expression of MHC-I molecules on human TC cell lines, thus impeding TC immunoevasion and potentiating TC susceptibility to immune destruction. 36 …”

Section: Cytokinesmentioning

confidence: 99%

The immune network in thyroid cancer

2016

View full text Add to dashboard Cite

The immune system plays critical roles in tumor prevention, but also in its initiation and progression. Tumors are subjected to immunosurveillance, but cancer cells generate an immunosuppressive microenvironment that favors their escape from immune-mediated elimination. During chronic inflammation, immune cells can contribute to the formation and progression of tumors by producing mitogenic, prosurvival, proangiogenic and lymphangiogenic factors. Thyroid cancer is the most frequent type of endocrine neoplasia and is the most rapidly increasing cancer in the US. In this review, we discuss recent findings on how different immune cells and mediators can contribute to thyroid cancer development and progression.

show abstract

“…Most of the studies have shown that MEK inhibition can increase the expression of intrinsic and IFN-γ-induced HLA/ MHC I/II in cancer cell lines, including melanoma, mesothelioma, prostate, gastric, and esophageal cancer cell lines [103][104][105]. Similarly to BRAF inhibition, treatment of mutant melanoma cell lines with MEK inhibition enhances the expression of melanoma-differentiation antigens [92] and decreases the production of IL-10, IL-6, and VEGF [91].…”

Section: Mek Inhibitionmentioning

confidence: 99%

The MAPK hypothesis: immune-regulatory effects of MAPK-pathway genetic dysregulations and implications for breast cancer immunotherapy

Bedognetti

Roelands

Decock

et al. 2017

Emerging Topics in Life Sciences

View full text Add to dashboard Cite

Correspondence: Davide Bedognetti (dbedognetti@sidra.org)With the advent of checkpoint inhibition, immunotherapy has revolutionized the clinical management of several cancers, but has demonstrated limited efficacy in mammary carcinoma. Transcriptomic profiling of cancer samples defined distinct immunophenotypic categories characterized by different prognostic and predictive connotations. In breast cancer, genomic alterations leading to the dysregulation of mitogen-activated protein kinase (MAPK) pathways have been linked to an immune-silent phenotype associated with poor outcome and treatment resistance. These aberrations include mutations of MAP3K1 and MAP2K4, amplification of KRAS, BRAF, and RAF1, and truncations of NF1. Anticancer therapies targeting MAPK signaling by BRAF and MEK inhibitors have demonstrated clear immunologic effects. These off-target properties could be exploited to convert the immune-silent tumor phenotype into an immune-active one. Preclinical evidence supports that MAPK-pathway inhibition can dramatically increase the efficacy of immunotherapy. In this review, we provide a detailed overview of the immunomodulatory impact of MAPK-pathway blockade through BRAF and MEK inhibitions. While BRAF inhibition might be relevant in melanoma only, MEK inhibition is potentially applicable to a wide range of tumors. Context-dependent similarities and differences of MAPK modulation will be dissected, in light of the complexity of the MAPK pathways. Therapeutic strategies combining the favorable effects of MAPK-oriented interventions on the tumor microenvironment while maintaining T-cell function will be presented. Finally, we will discuss recent studies highlighting the rationale for the implementation of MAPK-interference approaches in combination with checkpoint inhibitors and immune agonists in breast cancer.

show abstract

MHC Class I Loss Is a Frequent Mechanism of Immune Escape in Papillary Thyroid Cancer That Is Reversed by Interferon and Selumetinib TreatmentIn Vitro

Cited by 125 publications

References 45 publications

The Escape of Cancer from T Cell-Mediated Immune Surveillance: HLA Class I Loss and Tumor Tissue Architecture

The Escape of Cancer from T Cell-Mediated Immune Surveillance: HLA Class I Loss and Tumor Tissue Architecture

The immune network in thyroid cancer

The MAPK hypothesis: immune-regulatory effects of MAPK-pathway genetic dysregulations and implications for breast cancer immunotherapy

Contact Info

Product

Resources

About