The truncated cytoplasmic tail of HLA-G serves a quality-control function in post-ER compartments

Boyoun Park; Sungwook Lee; Eunkyung Kim; Sookkyung Chang; Mirim Jin; Kwangseog Ahn

doi:10.1016/S1074-7613(01)00179-0

The truncated cytoplasmic tail of HLA-G serves a quality-control function in post-ER compartments

Boyoun Park, Sungwook Lee, Eunkyung Kim, Sookkyung Chang, Mirim Jin, Kwangseog Ahn

Research output: Contribution to journal › Article › peer-review

19 Citations (Scopus)

Abstract

In contrast to the current model of MHC class I trafficking, which predicts that once a MHC class I molecule leaves the ER, it moves to the cell surface by bulk flow, we show that HLA-G that is loaded with suboptimal peptides is retrieved from post-ER compartments to the ER. Loading of HLA-G with high-affinity peptides abrogates this retrieval due to the lack of binding affinity to coatomer. Moreover, the loss of the endocytosis motif in the truncated cytoplasmic tail results in the prolonged half-life of HLA-G on the cell surface. Our findings reveal that surface expression of HLA-G can be further regulated in post-ER compartments and that the truncated cytoplasmic tail plays a critical role in such quality-control mechanisms.

Original language	English
Pages (from-to)	213-224
Number of pages	12
Journal	Immunity
Volume	15
Issue number	2
DOIs	https://doi.org/10.1016/S1074-7613(01)00179-0
Publication status	Published - 2001

All Science Journal Classification (ASJC) codes

Immunology and Allergy
Immunology
Infectious Diseases

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This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/S1074-7613(01)00179-0

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abstract = "In contrast to the current model of MHC class I trafficking, which predicts that once a MHC class I molecule leaves the ER, it moves to the cell surface by bulk flow, we show that HLA-G that is loaded with suboptimal peptides is retrieved from post-ER compartments to the ER. Loading of HLA-G with high-affinity peptides abrogates this retrieval due to the lack of binding affinity to coatomer. Moreover, the loss of the endocytosis motif in the truncated cytoplasmic tail results in the prolonged half-life of HLA-G on the cell surface. Our findings reveal that surface expression of HLA-G can be further regulated in post-ER compartments and that the truncated cytoplasmic tail plays a critical role in such quality-control mechanisms.",

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T1 - The truncated cytoplasmic tail of HLA-G serves a quality-control function in post-ER compartments

AU - Park, Boyoun

AU - Lee, Sungwook

AU - Kim, Eunkyung

AU - Chang, Sookkyung

AU - Jin, Mirim

AU - Ahn, Kwangseog

PY - 2001

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N2 - In contrast to the current model of MHC class I trafficking, which predicts that once a MHC class I molecule leaves the ER, it moves to the cell surface by bulk flow, we show that HLA-G that is loaded with suboptimal peptides is retrieved from post-ER compartments to the ER. Loading of HLA-G with high-affinity peptides abrogates this retrieval due to the lack of binding affinity to coatomer. Moreover, the loss of the endocytosis motif in the truncated cytoplasmic tail results in the prolonged half-life of HLA-G on the cell surface. Our findings reveal that surface expression of HLA-G can be further regulated in post-ER compartments and that the truncated cytoplasmic tail plays a critical role in such quality-control mechanisms.

AB - In contrast to the current model of MHC class I trafficking, which predicts that once a MHC class I molecule leaves the ER, it moves to the cell surface by bulk flow, we show that HLA-G that is loaded with suboptimal peptides is retrieved from post-ER compartments to the ER. Loading of HLA-G with high-affinity peptides abrogates this retrieval due to the lack of binding affinity to coatomer. Moreover, the loss of the endocytosis motif in the truncated cytoplasmic tail results in the prolonged half-life of HLA-G on the cell surface. Our findings reveal that surface expression of HLA-G can be further regulated in post-ER compartments and that the truncated cytoplasmic tail plays a critical role in such quality-control mechanisms.

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The truncated cytoplasmic tail of HLA-G serves a quality-control function in post-ER compartments

Abstract

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