Structural basis for antigenic peptide precursor processing by the endoplasmic reticulum aminopeptidase ERAP1

被引:0
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作者
Tina T Nguyen
Shih-Chung Chang
Irini Evnouchidou
Ian A York
Christos Zikos
Kenneth L Rock
Alfred L Goldberg
Efstratios Stratikos
Lawrence J Stern
机构
[1] University of Massachusetts Medical School,Department of Biochemistry and Molecular Pharmacology
[2] Harvard Medical School,Department of Cell Biology
[3] National Centre for Scientific Research 'Demokritos',Department of Microbiology and Molecular Genetics
[4] Michigan State University,Department of Pathology
[5] University of Massachusetts Medical School,undefined
[6] Present addresses: Institute of Microbiology and Biochemistry,undefined
[7] Department of Biochemical Science and Technology,undefined
[8] National Taiwan University,undefined
[9] Taipei,undefined
[10] Taiwan. (S.C.C.); Influenza Division,undefined
[11] Centers for Disease Control and Prevention,undefined
[12] Atlanta,undefined
[13] Georgia,undefined
[14] USA. (I.A.Y.).,undefined
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摘要
Endoplasmic reticulum aminopeptidase 1 (ERAP1) has a crucial role in antigen presentation because it trims peptide ligands to 8–10 residues so that they fit into the peptide-binding groove of MHC class I molecules. The structure of the ERAP1 in complex with bestatin, an aminopeptidase inhibitor, reveals how the enzyme´s catalytic center how the enzyme can preferentially process peptides 10–15 residues long while sparing shorter ones and provides the first evidence that substrate binding induces conformational changes.
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页码:604 / 613
页数:9
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