Literature DB >> 12161451

Crystal structure of human group X secreted phospholipase A2. Electrostatically neutral interfacial surface targets zwitterionic membranes.

Ying H Pan1, Bao-Zhu Yu, Alan G Singer, Farideh Ghomashchi, Gerard Lambeau, Michael H Gelb, Mahendra K Jain, Brian J Bahnson.   

Abstract

The crystal structure of human group X (hGX) secreted phospholipase A2 (sPLA2) has been solved to a resolution of 1.97 A. As expected the protein fold is similar to previously reported sPLA2 structures. The active site architecture, including the positions of the catalytic residues and the first and second shell water around the Ca2+ cofactor, are highly conserved and remarkably similar to the group IB and group IIA enzymes. Differences are seen in the structures following the (1-12)-N-terminal helix and at the C terminus. These regions are proposed to interact with the substrate membrane surface. The opening to the active site slot is considerably larger in hGX than in human group IIA sPLA2. Furthermore, the electrostatic surface potential of the hGX interfacial-binding surface does not resemble that of the human group IIA sPLA2; the former is highly neutral, whereas the latter is highly cationic. The cationic residues on this face of group IB and IIA enzymes have been implicated in membrane binding and in k(cat*) allostery. In contrast, hGX does not show activation by the anionic charge at the lipid interface when acting on phospholipid vesicles or short-chain phospholipid micelles. Together, the crystal structure and kinetic results of hGX supports the conclusion that it is as active on zwitterionic as on anionic interfaces, and thus it is predicted to target the zwitterionic membrane surfaces of mammalian cells.

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Year:  2002        PMID: 12161451     DOI: 10.1074/jbc.M202531200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  23 in total

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2.  Structural and phylogenetic basis for the classification of group III phospholipase A2.

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4.  In vitro effects of recombinant otoconin 90 upon calcite crystal growth. Significance of tertiary structure.

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Review 5.  Secretory phospholipase A2 enzymes as pharmacological targets for treatment of disease.

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Journal:  Biochem Pharmacol       Date:  2014-06-04       Impact factor: 5.858

6.  Discovery of a Series of Indole-2 Carboxamides as Selective Secreted Phospholipase A2 Type X (sPLA2-X) Inhibitors.

Authors:  Laurent Knerr; Fabrizio Giordanetto; Peter Nordberg; Daniel Pettersen; Nidhal Selmi; Hans-Georg Beisel; Hannah de la Motte; Thomas Olsson; Tim D J Perkins; Margareta Herslöf; Åsa Månsson; Mikael Dahlström; Ingemar Starke; Johan Broddefalk; Gabrielle Saarinen; Fredrik Klingegård; Eva Hurt-Camejo; Birgitta Rosengren; Johan Brengdahl; Frank Jansen; Mattias Rohman; Jenny Sandmark; Kenth Hallberg; Tomas Åkerud; Robert G Roth; Marie Ahlqvist
Journal:  ACS Med Chem Lett       Date:  2018-06-23       Impact factor: 4.345

7.  Molecular basis of phospholipase A2 activity toward phospholipids with sn-1 substitutions.

Authors:  Lars Linderoth; Thomas L Andresen; Kent Jørgensen; Robert Madsen; Günther H Peters
Journal:  Biophys J       Date:  2007-09-07       Impact factor: 4.033

8.  Effect of bilayer phospholipid composition and curvature on ligand transfer by the alpha-tocopherol transfer protein.

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Journal:  Lipids       Date:  2009-05-21       Impact factor: 1.880

9.  Crystal structure of a class XIB phospholipase A2 (PLA2): rice (oryza sativa) isoform-2 pla2 and an octanoate complex.

Authors:  Jodie E Guy; Ulf Ståhl; Ylva Lindqvist
Journal:  J Biol Chem       Date:  2009-05-20       Impact factor: 5.157

Review 10.  Secretory phospholipase A2: a multifaceted family of proatherogenic enzymes.

Authors:  Robert S Rosenson; Michael H Gelb
Journal:  Curr Cardiol Rep       Date:  2009-11       Impact factor: 2.931

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