 |
PDBsum entry 3gjs
|
|
|
|
References listed in PDB file
|
 |
|
Key reference
|
|
|
Title
|
|
Caspase-3 binds diverse p4 residues in peptides as revealed by crystallography and structural modeling.
|
|
|
Authors
|
|
B.Fang,
G.Fu,
J.Agniswamy,
R.W.Harrison,
I.T.Weber.
|
|
|
Ref.
|
|
Apoptosis, 2009,
14,
741-752.
|
|
|
PubMed id
|
|
|
|
|
|
Abstract
|
|
|
Caspase-3 recognition of various P4 residues in its numerous protein substrates
was investigated by crystallography, kinetics, and calculations on model
complexes. Asp is the most frequent P4 residue in peptide substrates, although a
wide variety of P4 residues are found in the cellular proteins cleaved by
caspase-3. The binding of peptidic inhibitors with hydrophobic P4 residues, or
no P4 residue, is illustrated by crystal structures of caspase-3 complexes with
Ac-IEPD-Cho, Ac-WEHD-Cho, Ac-YVAD-Cho, and Boc-D(OMe)-Fmk at resolutions of
1.9-2.6 A. The P4 residues formed favorable hydrophobic interactions in two
separate hydrophobic regions of the binding site. The side chains of P4 Ile and
Tyr form hydrophobic interactions with caspase-3 residues Trp206 and Trp214
within a non-polar pocket of the S4 subsite, while P4 Trp interacts with Phe250
and Phe252 that can also form the S5 subsite. These interactions of hydrophobic
P4 residues are distinct from those for polar P4 Asp, which indicates the
adaptability of caspase-3 for binding diverse P4 residues. The predicted trends
in peptide binding from molecular models had high correlation with experimental
values for peptide inhibitors. Analysis of structural models for the binding of
20 different amino acids at P4 in the aldehyde peptide Ac-XEVD-Cho suggested
that the majority of hydrophilic P4 residues interact with Phe250, while
hydrophobic residues interact with Trp206, Phe250, and Trp214. Overall, the S4
pocket of caspase-3 exhibits flexible adaptation for different residues and the
new structures and models, especially for hydrophobic P4 residues, will be
helpful for the design of caspase-3 based drugs.
|
|
|
|
|
|
|
