Proteomics

Dataset Information

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HDX-MS analysis of IRGQ in the presence of GABARAP-L2 and LC3B


ABSTRACT: The autophagy-lysosome system directs the degradation of a wide variety of cargo and is also involved in tumor progression. Here we show that immunity-related GTPase family Q protein (IRGQ) acts in the quality control of MHC-I molecules and directs misfolded MHC-I for lysosomal degradation through its binding to GABARAPL2 and LC3B. IRGQ specifically targets the non-conformational heavy chains of MHC-I, sorting them for degradation through the autophagy-lysosome system. In the absence of IRGQ, free MHC-I heavy chains accumulate in the cell and additionally get localized to the cell surface, thereby increasing interactions with mature MHC-I molecules and promoting immune response. Accordingly, mice suffering from hepatocellular carcinoma with reduced IRGQ levels display higher survival rates and bear more activated CD8+ T cells. Similarly, low IRGQ expression in human liver cancer correlates with higher levels of MHC-I molecules in the tumors, and patient survival is directly affected by IRGQ expression levels in CD8+ enriched tumors. Moreover, human T cells are more reactive toward tumorigenic IRGQ knock-out cells. Thus, we reveal IRGQ as a regulator of MHC-I quality control, mediating tumor immune evasion.

INSTRUMENT(S): Synapt MS

ORGANISM(S): Homo Sapiens (human) Escherichia Coli

SUBMITTER: Julian Langer  

LAB HEAD: Julian D. Langer

PROVIDER: PXD045212 | Pride | 2024-11-26

REPOSITORIES: pride

Dataset's files

Source:
Action DRS
20211202_IRGQ_GL2_1to4.7z Other
20211207_IRGQ_LC3B_1to4.7z Other
Data_table_IRGQ_GL2_LC3B_HDX-MS.txt Txt
IRGQ_GL2_Rel_Uptake.7z Other
IRGQ_LC3B_Rel_Uptake.7z Other
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Publications


The autophagy-lysosome system directs the degradation of a wide variety of cargo and is also involved in tumor progression. Here, we show that the immunity-related GTPase family Q protein (IRGQ), an uncharacterized protein to date, acts in the quality control of major histocompatibility complex class I (MHC class I) molecules. IRGQ directs misfolded MHC class I toward lysosomal degradation through its binding mode to GABARAPL2 and LC3B. In the absence of IRGQ, free MHC class I heavy chains do no  ...[more]

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