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Structural basis for dimerization quality control
by
Gee, Christine L.
, Mena, Elijah L.
, Lew, Brandon G.
, Akopian, David
, Rape, Michael
, Greber, Basil J.
, Kuriyan, John
, Nogales, Eva
, Jevtić, Predrag
in
101/28
/ 631/1647/2258
/ 631/337/458/582
/ 631/45/173
/ 631/45/474/1768
/ 82
/ 82/29
/ 82/58
/ 82/80
/ 82/83
/ BASIC BIOLOGICAL SCIENCES
/ BTB-POZ Domain - genetics
/ Cell division
/ Chemical properties
/ Chemical reactions
/ Complementarity
/ Crystal structure
/ Dimerization
/ Dimers
/ Dissociation
/ Divergence
/ Domains
/ Enzyme mechanisms
/ F-Box Proteins - metabolism
/ Humanities and Social Sciences
/ Humans
/ Kelch-Like ECH-Associated Protein 1 - chemistry
/ Kelch-Like ECH-Associated Protein 1 - genetics
/ Kelch-Like ECH-Associated Protein 1 - metabolism
/ Kinases
/ Models, Biological
/ Models, Molecular
/ multidisciplinary
/ Mutation
/ Oligomers
/ Protein Binding
/ Protein Folding
/ Protein Multimerization
/ Protein quality control
/ Protein research
/ Protein Stability
/ Protein-protein interactions
/ Proteins
/ Quality control
/ Science
/ Science (multidisciplinary)
/ Stem Cell Factor - metabolism
/ Structure
/ Structure determination
/ Ubiquitin
/ Ubiquitin-protein ligase
/ Ubiquitination
/ Ubiquitylation
2020
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Structural basis for dimerization quality control
by
Gee, Christine L.
, Mena, Elijah L.
, Lew, Brandon G.
, Akopian, David
, Rape, Michael
, Greber, Basil J.
, Kuriyan, John
, Nogales, Eva
, Jevtić, Predrag
in
101/28
/ 631/1647/2258
/ 631/337/458/582
/ 631/45/173
/ 631/45/474/1768
/ 82
/ 82/29
/ 82/58
/ 82/80
/ 82/83
/ BASIC BIOLOGICAL SCIENCES
/ BTB-POZ Domain - genetics
/ Cell division
/ Chemical properties
/ Chemical reactions
/ Complementarity
/ Crystal structure
/ Dimerization
/ Dimers
/ Dissociation
/ Divergence
/ Domains
/ Enzyme mechanisms
/ F-Box Proteins - metabolism
/ Humanities and Social Sciences
/ Humans
/ Kelch-Like ECH-Associated Protein 1 - chemistry
/ Kelch-Like ECH-Associated Protein 1 - genetics
/ Kelch-Like ECH-Associated Protein 1 - metabolism
/ Kinases
/ Models, Biological
/ Models, Molecular
/ multidisciplinary
/ Mutation
/ Oligomers
/ Protein Binding
/ Protein Folding
/ Protein Multimerization
/ Protein quality control
/ Protein research
/ Protein Stability
/ Protein-protein interactions
/ Proteins
/ Quality control
/ Science
/ Science (multidisciplinary)
/ Stem Cell Factor - metabolism
/ Structure
/ Structure determination
/ Ubiquitin
/ Ubiquitin-protein ligase
/ Ubiquitination
/ Ubiquitylation
2020
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Structural basis for dimerization quality control
by
Gee, Christine L.
, Mena, Elijah L.
, Lew, Brandon G.
, Akopian, David
, Rape, Michael
, Greber, Basil J.
, Kuriyan, John
, Nogales, Eva
, Jevtić, Predrag
in
101/28
/ 631/1647/2258
/ 631/337/458/582
/ 631/45/173
/ 631/45/474/1768
/ 82
/ 82/29
/ 82/58
/ 82/80
/ 82/83
/ BASIC BIOLOGICAL SCIENCES
/ BTB-POZ Domain - genetics
/ Cell division
/ Chemical properties
/ Chemical reactions
/ Complementarity
/ Crystal structure
/ Dimerization
/ Dimers
/ Dissociation
/ Divergence
/ Domains
/ Enzyme mechanisms
/ F-Box Proteins - metabolism
/ Humanities and Social Sciences
/ Humans
/ Kelch-Like ECH-Associated Protein 1 - chemistry
/ Kelch-Like ECH-Associated Protein 1 - genetics
/ Kelch-Like ECH-Associated Protein 1 - metabolism
/ Kinases
/ Models, Biological
/ Models, Molecular
/ multidisciplinary
/ Mutation
/ Oligomers
/ Protein Binding
/ Protein Folding
/ Protein Multimerization
/ Protein quality control
/ Protein research
/ Protein Stability
/ Protein-protein interactions
/ Proteins
/ Quality control
/ Science
/ Science (multidisciplinary)
/ Stem Cell Factor - metabolism
/ Structure
/ Structure determination
/ Ubiquitin
/ Ubiquitin-protein ligase
/ Ubiquitination
/ Ubiquitylation
2020
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Journal Article
Structural basis for dimerization quality control
2020
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Overview
Most quality control pathways target misfolded proteins to prevent toxic aggregation and neurodegeneration
1
. Dimerization quality control further improves proteostasis by eliminating complexes of aberrant composition
2
, but how it detects incorrect subunits remains unknown. Here we provide structural insight into target selection by SCF–FBXL17, a dimerization-quality-control E3 ligase that ubiquitylates and helps to degrade inactive heterodimers of BTB proteins while sparing functional homodimers. We find that SCF–FBXL17 disrupts aberrant BTB dimers that fail to stabilize an intermolecular β-sheet around a highly divergent β-strand of the BTB domain. Complex dissociation allows SCF–FBXL17 to wrap around a single BTB domain, resulting in robust ubiquitylation. SCF–FBXL17 therefore probes both shape and complementarity of BTB domains, a mechanism that is well suited to establish quality control of complex composition for recurrent interaction modules.
Structural studies of the dimerization quality control E3 ubiquitin ligase SCF–FBXL17 indicate that its selectivity for aberrant complex formation is based on recognizing both shape and complementarity of interacting domains.
Publisher
Nature Publishing Group UK,Nature Publishing Group
Subject
/ 82
/ 82/29
/ 82/58
/ 82/80
/ 82/83
/ Dimers
/ Domains
/ Humanities and Social Sciences
/ Humans
/ Kelch-Like ECH-Associated Protein 1 - chemistry
/ Kelch-Like ECH-Associated Protein 1 - genetics
/ Kelch-Like ECH-Associated Protein 1 - metabolism
/ Kinases
/ Mutation
/ Protein-protein interactions
/ Proteins
/ Science
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