Allosteric modulation of peroxisomal membrane protein recognition by farnesylation of the peroxisomal import receptor PEX19

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作者
Leonidas Emmanouilidis
Ulrike Schütz
Konstantinos Tripsianes
Tobias Madl
Juliane Radke
Robert Rucktäschel
Matthias Wilmanns
Wolfgang Schliebs
Ralf Erdmann
Michael Sattler
机构
[1] Institute of Structural Biology,Department Chemie
[2] Helmholtz Zentrum München,Department of Systems Biology
[3] Munich Center for Integrated Protein Science at Chair of Biomolecular NMR,undefined
[4] Technische Universität München,undefined
[5] CEITEC—Central European Institute of Technology,undefined
[6] Masaryk University,undefined
[7] Institute of Molecular Biology and Biochemisty,undefined
[8] Medical University of Graz,undefined
[9] Institute of Biochemistry and Pathobiochemistry,undefined
[10] Faculty of Medicine,undefined
[11] Ruhr University Bochum,undefined
[12] EMBL Hamburg,undefined
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摘要
The transport of peroxisomal membrane proteins (PMPs) requires the soluble PEX19 protein as chaperone and import receptor. Recognition of cargo PMPs by the C-terminal domain (CTD) of PEX19 is required for peroxisome biogenesis in vivo. Farnesylation at a C-terminal CaaX motif in PEX19 enhances the PMP interaction, but the underlying molecular mechanisms are unknown. Here, we report the NMR-derived structure of the farnesylated human PEX19 CTD, which reveals that the farnesyl moiety is buried in an internal hydrophobic cavity. This induces substantial conformational changes that allosterically reshape the PEX19 surface to form two hydrophobic pockets for the recognition of conserved aromatic/aliphatic side chains in PMPs. Mutations of PEX19 residues that either mediate farnesyl contacts or are directly involved in PMP recognition abolish cargo binding and cannot complement a ΔPEX19 phenotype in human Zellweger patient fibroblasts. Our results demonstrate an allosteric mechanism for the modulation of protein function by farnesylation.
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