 |
PDBsum entry 4j8e
|
|
|
|
References listed in PDB file
|
 |
|
Key reference
|
|
|
Title
|
|
Structure and function of hip, An attenuator of the hsp70 chaperone cycle.
|
|
|
Authors
|
|
Z.Li,
F.U.Hartl,
A.Bracher.
|
|
|
Ref.
|
|
Nat Struct Biol, 2013,
20,
929-935.
[DOI no: ]
|
|
|
PubMed id
|
|
|
|
|
|
Abstract
|
|
|
The Hsp70-interacting protein, Hip, cooperates with the chaperone Hsp70 in
protein folding and prevention of aggregation. Hsp70 interacts with non-native
protein substrates in an ATP-dependent reaction cycle regulated by J-domain
proteins and nucleotide exchange factors (NEFs). Hip is thought to delay
substrate release by slowing ADP dissociation from Hsp70. Here we present
crystal structures of the dimerization domain and the tetratricopeptide repeat
(TPR) domain of rat Hip. As shown in a cocrystal structure, the TPR core of Hip
interacts with the Hsp70 ATPase domain through an extensive interface, to form a
bracket that locks ADP in the binding cleft. Hip and NEF binding to Hsp70 are
mutually exclusive, and thus Hip attenuates active cycling of Hsp70-substrate
complexes. This mechanism explains how Hip enhances aggregation prevention by
Hsp70 and facilitates transfer of specific proteins to downstream chaperones or
the proteasome.
|
|
|
|
|
|
|
