EXPLORE PUBLICATIONS BY COUNTRIES


	EUROPE

	MIDDLE EAST

	ASIA

	AFRICA
.............................

	United States of America

	United Kingdom

	Canada

	Australia

	Italy

	France

	Brazil

	Germany

	Malaysia

	Turkey

	China

	Taiwan

	Japan

	Saudi Arabia

	Jordan

	Egypt

	United Arab Emirates

	India

	Nigeria

Comparative Structural Analysis of Phospholipase A2 and Combinatorial Screening of PLA2 Inhibitors

Sanjay Sharma Timilsina, Sarnim Gurung, Roshan Adhikari, Jignesh Savani, Mayank Agrawal, Vedamurthy A.B., Joy Harris Hoskeri

Pages - 14 - 26 | Revised - 05-04-2013 | Published - 30-04-2013

Published in International Journal of Biometrics and Bioinformatics (IJBB)

Volume - 7 Issue - 1 | Publication Date - June 2013 Table of Contents

MORE INFORMATION

References | Abstracting & Indexing

KEYWORDS

Phospholipase A2, Antivenom Drugs, Superimposition Studies, Sequence Alignment, Combinatorial Screening, Molecular Docking.

ABSTRACT

Phospholipases A2 (PLA2) enzyme release fatty acids from the second carbon group of glycerol. This particular phospholipase specifically recognizes the Sn-2 acyl bond of phospholipids and catalytically hydrolyzes the bond releasing arachidonic acid and lysophospholipids. PLA2 are commonly found in mammalian tissues as well as in insects and snakes venom. Venoms constitute a rich source of phospholipase A2 (PLA2) enzymes, which show remarkable diversity in their structure and function. In this investigation, we have made an attempt in analyzing the identical active domain in different PLA2 protein structure isolated from different venoms by studying the conserved active pocket residues. The 21 crystal structures of different PLA2 enzymes isolated from venoms of different species were studied and collected from PDB database. Comparative studies to analyse the conserved active site in this protein was carried out by superimposition studies using TOPMATCH server. To validate the superimposition results sequence alignment studies was carried out using T-COFFEE by multiple sequence alignment analysis. This revealed that 9 PLA2 enzymes from different venoms viz., Daboia russellii, Cerrophidion godmani, Dienagkistrodon acutus, Bothrops Neuwied, Agkistrodon contortrix, Naja sagittifera, Bos Taurus, Notechis sentatusscutatus, Apis mellifera showed similarity in their active pocket residues, indicating a single drug can effectively occupy their pocket and inhibit the functions of these nine proteins. Hence, in-silico drug designing studies for antivenom drugs against PLA2 was carried out by combinatorial screening of 18 antivenom compounds by docking with PLA2 molecule using Autodock 3.0 tool. In-silico drug designing studies revealed that among 18 antivenom compounds, Indole was most potent in its action in inhibiting the PLA2 function with inhibition constant of 0.04.

ABSTRACTING & INDEXING

1	Google Scholar

2	CiteSeerX

3	refSeek

4	Scribd

5	SlideShare

6	PdfSR

REFERENCES

A. Argiolas and J.J. Pisano. "Facilitation of phospholipase A2 activity by mastoparans, a new class of mast cell degranulating peptides from wasp venom". Journal of Biological Chemistry. Vol 258(22), pp. 13697-13702, Nov. 1983.

A.K. Ghose and G.M. Crippen. “Atomic physicochemical parameters for three-dimensionalstructure-directed quantitative structure–activity relationships 2. Modeling dispersive and hydrophobic interactions”. Journal of Chemical Information Computer Sciences. Vol 27(1), pp.21-35, Feb. 1987.

A.W. Schüttelkopf and D.M.Van Aalten. “PRODRG: a tool for high-throughput crystallography of protein-ligand complexes”. Acta Crystallographica Section D Biological Crystallography. Vol 60(8), pp. 1355-1363, Aug. 2004.

C. Notredame, D.G. Higgins and J. Heringa. “T-Coffee: A novel method for fast and accurate multiple sequence alignment”. Journal of Molecular Biology. Vol 302(1), pp. 205-217, Sep.2000.

D. De Luca, A. Minucci, P. Cogo, E.D. Capoluongo, G. Conti, D. Pietrini, V.P. Carnielli, and M.Piastra. "Secretory phospholipase A pathway during pediatric acute respiratory distress syndrome: a preliminary study". Pediatric Critical CareMediciine. Vol 12(1), 20-24, Jan. 2011.

E.A. Dennis. “Diversity of group types, regulation, and function of phospholipaseA2." Journal of Biological Chemistry. Vol 269(18), pp. 13057-13060, May. 1994.

J. Gasteiger and M. Marsili. “Iterative partial equalization of orbital electronegativity - a rapid access to atomic charges”. Tetrahedron. Vol 36(22), pp. 3219-3288, Mar. 1980.

J. P. Chippaux. Snake bites- appraisal of the global situation. Bulletin of World Health Organization, Vol 76(5), 515-524, May. 1998.

J.P. Nicolas, Y. Lin, G. Lambeau, F. Ghomashchi, M. Lazdunski and M.H. Gelb. "Localization of structural elements of bee venom phospholipase A2 involved in N-type receptor binding and neurotoxicity". Journal Biological Chemistry. Vol 272(11), pp. 7173-7181, Mar. 1997.

L.A. Ferreira., O.B. Henriques, A.A. Andreoni, G.R. Vital, M.M. Campos, G.G. Habermehl, and V.L. de Moraes. “Antivenom and biological effects of ar-turmerone isolated from Curcuma longa (Zingiberaceae)”. Toxicon. 30, pp. 1211–1218, Oct. 1992.

M.J. Sippl and M. Wiederstein. “A note on difficult structure alignment problems”.Bioinformatics. Vol 24(3), pp. 426-427, Jan. 2008.

R. Bhat, Y. Xue and S. Berg. “Structural insights and biological effects of glycogen synthase kinase 3-specific inhibitor AR-A014418”. Journal of Biological Chemistry. Vol 278(46), pp.45937–45945, Aug 2003.

R.M. Kini. Venom Phospholipase A2 Enzymes: Structure, Function and Mechanism. England,John Wiley & Sons, Chichester, 1997, pp. 1-511.

T. Reya and H. Clevers. ” Wnt signalling in stem cells and cancer”. Nature. Vol 434(7035), pp.843-850, Apr. 2005.

T.A. Binkowski, S. Naghibzadeg and J. Liang. “ CASTp computed atlas of surface topography of proteins”. Nucleic Acid Research. Vol 31(13), pp. 3352–3355, Jul. 2003.

W.R. Henderson, R.C. Oslund, J.G. Bollinger, X. Ye, Y.T. Tien, J. Xue, and M.H. Gelb. "Blockade of Human Group X Secreted Phospholipase A2 (GX-sPLA2)-induced Airway Inflammation and Hyperresponsiveness in a Mouse Asthma Model by a Selective GX-sPLA2 Inhibitor". Journal of Biological Chemistry, Vol 286(32), 28049–28055, Aug. 2011.

Y. Wei, S.P. Epstein, S. Fukuoka, N.P. Birmingham, X.M. Li, and P.A. Asbell. "sPLA2-IIa Amplifies Ocular Surface Inflammation in the Experimental Dry Eye (DE) BALB/c Mouse Model". Investigative Opthalmology and Visual Science. Vol 52(7), pp. 4780–4788, Jul. 2011.

Y.H. Pan, T.M. Epstein, M.K. Jain and B.J. Bahnson. "Five coplanar anion binding sites on one face of phospholipase A2: relationship to interface binding". Biochemistry. Vol 40(3), pp. 609–617, Jan. 2001.

Z. Mallat, G. Lambeau, A. Tedgui. "Lipoprotein-Associated and Secreted Phospholipases A2 in Cardiovascular Disease: Roles as Biological Effectors and Biomarkers". Circulation. Vol 122(21), pp. 2183-2200. Nov. 2010.