Literature DB >> 22215060

Structural analysis of secretory phospholipase A2 from Clonorchis sinensis: therapeutic implications for hepatic fibrosis.

Gururao Hariprasad1, Punit Kaur, Alagiri Srinivasan, Tej Pal Singh, Manoj Kumar.   

Abstract

Hepatic fibrosis is a common complication of the infection by the parasite, Clonorchis sinensis. There is a high incidence of this disease in the Asian countries with an increased risk of conversion to cancer. A secretory phospholipase A(2) (PLA(2)) enzyme from the parasite is implicated in the pathology. This is an attractive drug target in the light of extensive structural characterization of this class of enzyme. In this study, the structure of the enzyme was modeled based on its sequence homology to the group III bee venom PLA(2). On analysis, the overall structure essentially is comprised of three helices, two sets of β-wings and an elongated C-terminal extension. The structure is stabilized by four disulfide bonds. The structure is comprised of a calcium binding loop, active site and a substrate binding hydrophobic channel. The active site of the enzyme shows the classical features of PLA(2) with the participation of the three residues: histidine-aspartic acid-tyrosine in hydrogen bond formation. This is an interesting variation from the house keeping group III PLA(2) enzyme of human which has a histidine-aspartic acid and phenylalanine arrangement at the active site. This difference is therefore an important structural parameter that can be exploited to design specific inhibitor molecules against the pathogen PLA(2). Likewise, there are certain unique structural features in the hydrophobic channel and the putative membrane binding surface of the PLA(2) from Clonorchis sinensis that not only help understand the mechanism of action but also provide knowledge for a targeted therapy of liver fibrosis caused by the parasite.

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Year:  2012        PMID: 22215060     DOI: 10.1007/s00894-011-1333-8

Source DB:  PubMed          Journal:  J Mol Model        ISSN: 0948-5023            Impact factor:   1.810


  30 in total

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2.  The SWISS-MODEL workspace: a web-based environment for protein structure homology modelling.

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Authors:  Julie D Thompson; Toby J Gibson; Des G Higgins
Journal:  Curr Protoc Bioinformatics       Date:  2002-08

5.  Structural analysis of a group III Glu62-phospholipase A2 from the scorpion, Mesobuthus tamulus: Targeting and reversible inhibition by native peptides.

Authors:  Gururao Hariprasad; Manoj Kumar; Alagiri Srinivasan; Punit Kaur; Tej Pal Singh; Othayoth Jithesh
Journal:  Int J Biol Macromol       Date:  2011-01-14       Impact factor: 6.953

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Authors:  D L Scott; P B Sigler
Journal:  Adv Protein Chem       Date:  1994

7.  Novel human secreted phospholipase A(2) with homology to the group III bee venom enzyme.

Authors:  E Valentin; F Ghomashchi; M H Gelb; M Lazdunski; G Lambeau
Journal:  J Biol Chem       Date:  2000-03-17       Impact factor: 5.157

8.  Cloning, sequence analysis and homology modeling of a novel phospholipase A2 from Heterometrus fulvipes (Indian black scorpion).

Authors:  Gururao Hariprasad; Baskar Singh; Utpal Das; Abdul S Ethayathulla; Punit Kaur; Tej P Singh; Alagiri Srinivasan
Journal:  DNA Seq       Date:  2007-06

9.  Human group III secreted phospholipase A2 promotes neuronal outgrowth and survival.

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10.  [Excretory/secretory antigens from Clonorchis sinensis induces hepatic fibrosis in rats].

Authors:  Feng-Yu Hu; Xu-Chu Hu; Chang-Ling Ma; Jin Xu; Xin-Bing Yu
Journal:  Nan Fang Yi Ke Da Xue Xue Bao       Date:  2009-03
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4.  Structural Modeling of Wild and Mutant Forms of Human Plasma Platelet Activating Factor-Acetyl Hydrolase Enzyme.

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Journal:  J Inflamm Res       Date:  2020-12-16

5.  Molecular Characterization and In Silico Analyses of Maurolipin Structure as a Secretory Phospholipase A 2 (sPLA2) from Venom Glands of Iranian Scorpio maurus (Arachnida: Scorpionida).

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  5 in total

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