Loss of Optineurin Drives Cancer Immune Evasion via Palmitoylation-Dependent IFNGR1 Lysosomal Sorting and Degradation

Mutations in IFN and MHC signaling genes endow immunotherapy resistance. Patients with colorectal cancer infrequently exhibit IFN and MHC signaling gene mutations and are generally resistant to immunotherapy. In exploring the integrity of IFN and MHC signaling in colorectal cancer, we found that opt...

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Bibliographic Details
Published in:Cancer discovery 2021-07, Vol.11 (7), p.1826-1843
Main Authors: Du, Wan, Hua, Fang, Li, Xiong, Zhang, Jian, Li, Shasha, Wang, Weichao, Zhou, Jiajia, Wang, Weimin, Liao, Peng, Yan, Yijian, Li, Gaopeng, Wei, Shuang, Grove, Sara, Vatan, Linda, Zgodziński, Witold, Majewski, Marek, Wallner, Grzegorz, Chen, Haoyan, Kryczek, Ilona, Fang, Jing-Yuan, Zou, Weiping
Format: Article
Language:English
Subjects:
Animals
Cell Cycle Proteins - metabolism
Colorectal Neoplasms - genetics
Colorectal Neoplasms - metabolism
Colorectal Neoplasms - therapy
Female
Histocompatibility Antigens Class I - metabolism
Humans
Interferon gamma Receptor
Interferon-gamma - metabolism
Lipoylation
Male
Membrane Transport Proteins - metabolism
Mice
Mice, Inbred C57BL
Mice, Inbred Strains
Protein Transport
Receptors, Interferon - metabolism
Specific Pathogen-Free Organisms
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Summary:Mutations in IFN and MHC signaling genes endow immunotherapy resistance. Patients with colorectal cancer infrequently exhibit IFN and MHC signaling gene mutations and are generally resistant to immunotherapy. In exploring the integrity of IFN and MHC signaling in colorectal cancer, we found that optineurin was a shared node between the two pathways and predicted colorectal cancer patient outcome. Loss of optineurin occurs in early-stage human colorectal cancer. Immunologically, optineurin deficiency was shown to attenuate IFNGR1 and MHC-I expression, impair T-cell immunity, and diminish immunotherapy efficacy in murine cancer models and patients with cancer. Mechanistically, we observed that IFNGR1 was -palmitoylated on Cys122, and AP3D1 bound with and sorted palmitoylated IFNGR1 to lysosome for degradation. Unexpectedly, optineurin interacted with AP3D1 to prevent palmitoylated IFNGR1 lysosomal sorting and degradation, thereby maintaining IFNγ and MHC-I signaling integrity. Furthermore, pharmacologically targeting IFNGR1 palmitoylation stabilized IFNGR1, augmented tumor immunity, and sensitized checkpoint therapy. Thus, loss of optineurin drives immune evasion and intrinsic immunotherapy resistance in colorectal cancer. SIGNIFICANCE: Loss of optineurin impairs the integrity of both IFNγ and MHC-I signaling pathways via palmitoylation-dependent IFNGR1 lysosomal sorting and degradation, thereby driving immune evasion and intrinsic immunotherapy resistance in colorectal cancer. Our work suggests that pharmacologically targeting IFNGR1 palmitoylation can stabilize IFNGR1, enhance T-cell immunity, and sensitize checkpoint therapy in colorectal cancer. . .
ISSN:2159-8274
2159-8290
DOI:10.1158/2159-8290.CD-20-1571