IFNγ-Dependent Tissue-Immune Homeostasis Is Co-opted in the Tumor Microenvironment

Nirschl, Christopher J.; Suárez‐Fariñas, Mayte; Izar, Benjamin; Prakadan, Sanjay M.; Dannenfelser, Ruth; Tirosh, Itay; Liu, Yong; Zhu, Qi; Devi, K. Sanjana P.; Carroll, Shaina L.; Chau, David; Rezaee, Mehrdad; Kim, Tae Kyun; Huang, Ruiqi; Fuentes‐Duculan, Judilyn; Song-Zhao, George X.; Gulati, Nicholas; Lowes, Michelle A.; King, Sandra L.; Quintana, Francisco J.; Lee, Young suk; Krueger, James G.; Sarin, Kavita Y.; Yoon, Charles H.; Garraway, Levi A.; Regev, Aviv; Shalek, Alex K.; Troyanskaya, Olga G.; Anandasabapathy, Niroshana

doi:10.1016/j.cell.2017.06.016

Cited by 142 publications

(123 citation statements)

References 52 publications

(67 reference statements)

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“…In accordance with the increased immunosuppressive landscape in melanoma, our study identified increased DCs expressing suppressive markers that have previously been associated with tolerogenic, immunoregulatory function. Similar to SOCS2, which was previously identified as a protein expressed by dendritic cells that is critical for limiting antitumor immune response in MM, SOCS3 is also a member of the suppressor of cytokine signalling (SOCS) proteins family. SOCS3 expression by dendritic cells has not previously been described in human melanoma.…”

Section: Discussionmentioning

confidence: 93%

Novel immune signatures associated with dysplastic naevi and primary cutaneous melanoma in human skin

Yan

Garcet

Gulati

et al. 2018

Experimental Dermatology

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Dysplastic nevi (DN) are benign lesions with atypical features intermediate between that of common melanocytic nevi (CMN) and malignant melanoma (MM). Debate remains over whether DN represent progressive lesions from CMN. Through gene expression profiling and analysis of molecular gene signatures, our study revealed progressive increases in immune activation and regulation, along with pathways implicated in melanomagenesis, from CMN to DN to MM. Using criteria of 1.5 fold change and false discovery rate ≤ 0.05, we found differential expression of 7,186 probes (6,370 unique genes) with the largest difference detected between DN and MM from the standpoint of genomic melanoma progression. Despite progressive increases in the T-helper type 1 (Th1) inducing gene (IL-12), RT-PCR indicated impaired Th1 or cytotoxic T-cell response (decreased IFN-γ) in MM. Concordantly, our results indicated progressive increases in molecular markers associated with regulatory T-cells, exhausted T-cells, and tolerogenic dendritic cells, including detection of increased expression of suppressor of cytokine signaling 3 (SOCS3) in dendritic cells associated with MM. All together, our findings suggest that the increased immunosuppressive microenvironment of melanoma may contribute to unhampered proliferation of neoplastic cells. In addition, the detection of increased markers associated with tolerogenic dendritic cells in MM suggest that targeting these suppressive immune cell types may represent an alternative avenue for future immunotherapy.

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Section: Discussionmentioning

confidence: 93%

Novel immune signatures associated with dysplastic naevi and primary cutaneous melanoma in human skin

Yan

Garcet

Gulati

et al. 2018

Experimental Dermatology

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“…The role of IFN‐γ in maintaining immune homeostasis is less well described. A recent study suggests that IFN‐γ regulates homeostasis in healthy tissue by upregulation of suppressor‐of‐cytokine‐2 (SOCS2) protein expressed by tissue phagocytes . Moreover, we previously described that IFN‐γ induces indoleamine 2, 3‐dioxygenase production from gingival fibroblast cells .…”

Section: Discussionmentioning

confidence: 95%

Memory T cell subsets in healthy gingiva and periodontitis tissues

Mahanonda

Champaiboon

Subbalekha

et al. 2018

Journal of Periodontology

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Our findings suggest that recirculating and gingiva-resident memory T cells could represent an important part of the immune surveillance network in the connective tissue, maintaining periodontal homeostasis. Imbalance of subgingival bacterial communities could damage gingival barrier allowing bacterial antigens to get access to the deeper connective tissue where they activate memory T cells leading to deleterious inflammation; a hallmark of periodontitis.

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“…IFNγ could induce expression of suppressor‐of‐cytokine‐2 (SOCS2) protein, a conserved program transcript, which is expressed by mononuclear phagocytes infiltrating primary melanoma. SOCS2 limits adaptive antitumor immunity and DC‐based priming of T cells in vivo . These results link immune homeostasis to key determinants of antitumor immunity and escape, uncovering the underlying mechanism by which IFNγ contributes to tumor escape in the tumor microenvironments.…”

Section: The Role Of Ifnγ In Tumor Escapementioning

confidence: 92%

Interferon gamma in cancer immunotherapy

2018

Cancer Medicine

254

162

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Immune system can recognize self vs transformed self. That is why cancer immunotherapy achieves notable benefits in a wide variety of cancers. Recently, several papers reported that immune checkpoint blockade therapy led to upregulation of IFNγ and in turn clearance of tumor cells. In this review, we conducted an extensive literature search of recent 5‐year studies about the roles of IFNγ signaling in both tumor immune surveillance and immune evasion. In addition to well‐known functions, IFNγ signaling also induces tumor ischemia and homeostasis program, resulting in tumor clearance and tumor escape, respectively. The yin and the yang of IFNγ signaling are summarized. Thus, this review helps us to comprehensively understand the roles of IFNγ in tumor immunity, which contributes to better design and management of clinical immunotherapy approaches.

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IFNγ-Dependent Tissue-Immune Homeostasis Is Co-opted in the Tumor Microenvironment

Cited by 142 publications

References 52 publications

Novel immune signatures associated with dysplastic naevi and primary cutaneous melanoma in human skin

Novel immune signatures associated with dysplastic naevi and primary cutaneous melanoma in human skin

Memory T cell subsets in healthy gingiva and periodontitis tissues

Interferon gamma in cancer immunotherapy

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