Detailed molecular comparison between the inhibition mode of A/B-type carboxypeptidases in the zymogen state and by the endogenous inhibitor latexin

Treatment of advanced stages of prostate carcinoma with histone-deacetylase inhibitors entails expression of human procarboxypeptidase-A4 (hPCPA4). The three-dimensional structure of hPCPA4 has been solved and shows the features of related metallocarboxypeptidase zymogens, with a preformed alpha/bet...

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Published inCellular and molecular life sciences : CMLS Vol. 62; no. 17; pp. 1996 - 2014
Main Authors García-Castellanos, R, Bonet-Figueredo, R, Pallarés, I, Ventura, S, Avilés, F X, Vendrell, J, Gomis-Rütha, F X
Format Journal Article
LanguageEnglish
Published Switzerland Springer Nature B.V 01.09.2005
Birkhäuser-Verlag
Subjects
Amino Acid Sequence
Animals
Antigens - chemistry
Antigens - pharmacology
Carboxypeptidase B - antagonists & inhibitors
Carboxypeptidase B - chemistry
Carboxypeptidases A - antagonists & inhibitors
Carboxypeptidases A - chemistry
Crystal structure
Crystallography, X-Ray
Enzyme Precursors - antagonists & inhibitors
Enzyme Precursors - chemistry
Enzymes
Humans
Male
Mice
Molecular Sequence Data
Peptides
Prostate cancer
Prostatic Neoplasms - enzymology
Protein Conformation
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Summary:Treatment of advanced stages of prostate carcinoma with histone-deacetylase inhibitors entails expression of human procarboxypeptidase-A4 (hPCPA4). The three-dimensional structure of hPCPA4 has been solved and shows the features of related metallocarboxypeptidase zymogens, with a preformed alpha/beta/-hydrolase active-enzyme moiety (hCPA4) and an inhibiting pro-domain (PD). The protease moiety recalls a sphere, out of which a spherical cone has been cut. This results in a funnel-like structure, at the bottom of which the active-site cleft resides. The border of this funnel is shaped by loops, which are responsible for the interaction with the PD, characterised by a large interface area and relatively few contacts. Such an inhibitory mode is evocative of the recently reported structure of the human inhibitor latexin in its complex with hCPA4. The main contacting structure of latexin is similar to the one employed for PD inhibition. In both cases, active-site blocking relies mainly on a loop provided by the central part of a beta sheet.
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ISSN:1420-682X
1420-9071
DOI:10.1007/s00018-005-5174-4