Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:3.4.21.37 (
neutrophil elastase
)
4,078
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Three insect peptides showing high sequence similarity and belonging to the same structural family incorporating a cysteine knot and a short three-stranded antiparalled beta-sheet were studied. Their inhibitory effect on two serine proteases (bovine alpha-chymotrypsin and human
leukocyte elastase
) is reported. One of them,
PMP
-C, is a strong alpha-chymotrypsin inhibitor (Ki = 0.2 nM) and interacts with
leukocyte elastase
with a Ki of 0.12 microM. The other two peptides,
PMP
-D2 and HI, interact only weakly with alpha-chymotrypsin and do not inhibit
leukocyte elastase
. Synthetic variants of these peptides were prepared by solid-phase synthesis, and their action toward serine proteases was evaluated. This enabled us to locate the P1 residues within the reactive sites (Leu-30 for
PMP
-C and Arg-29 for
PMP
-D2 and HI), and, interestingly, variants of
PMP
-D2 and HI were converted into powerful inhibitors of both alpha-chymotrypsin and
leukocyte elastase
, the most potent elastase inhibitor obtained in this study having a Ki of 3 nM.
...
PMID:Serine protease inhibition by insect peptides containing a cysteine knot and a triple-stranded beta-sheet. 759 20
The solution structure and the disulfide pairings of a 36-residue proteinase inhibitor isolated from the insect Locusta migratoria have been determined using NMR spectroscopy and simulated annealing calculations. The peptide, termed
PMP
-C, was previously shown to inhibit bovine alpha-chymotrypsin as well as human
leukocyte elastase
, and was also found to block high-voltage-activated Ca2+ currents in rat sensory neurones.
PMP
-C has a prolate ellipsoid shape and adopts a tertiary fold hitherto unobserved in the large group of small "canonical" proteinase inhibitors. The over-all fold consists mainly of three strands arranged in a right-handed twisted, antiparallel, beta-sheet that demarcates a cavity, together with a linear amino-terminal segment oriented almost perpendicular to the three strands of the beta-sheet. Inside the cavity a phenyl ring constitutes the centre of a hydrophobic core. The proteinase binding loop is located in the carboxy-terminal part of the molecule, between two cysteine residues involved in disulfide bridges. Its conformation resembles that found in other small canonical proteinase inhibitors. A comparison of
PMP
-C structure with the recently published solution structure of the related peptide
PMP
-D2 shows that the most significant differences are complementary changes involved in the stabilization of similar folds. This comparison led us to review the structure of
PMP
-D2 and to identify two salt bridges in
PMP
-D2.
...
PMID:Solution structure of PMP-C: a new fold in the group of small serine proteinase inhibitors. 861 85
