Literature DB >> 11847226

The structural basis of compstatin activity examined by structure-function-based design of peptide analogs and NMR.

Dimitrios Morikis1, Melinda Roy, Arvind Sahu, Anastasios Troganis, Patricia A Jennings, George C Tsokos, John D Lambris.   

Abstract

We have previously identified compstatin, a 13-residue cyclic peptide, that inhibits complement activation by binding to C3 and preventing C3 cleavage to C3a and C3b. The structure of compstatin consists of a disulfide bridge and a type I beta-turn located at opposite sides to each other. The disulfide bridge is part of a hydrophobic cluster, and the beta-turn is part of a polar surface. We present the design of compstatin analogs in which we have introduced a series of perturbations in key structural elements of their parent peptide, compstatin. We have examined the consistency of the structures of the designed analogs compared with compstatin using NMR, and we have used the resulting structural information to make structure-complement inhibitory activity correlations. We propose the following. 1) Even in the absence of the disulfide bridge, a linear analog has a propensity for structure formation consistent with a turn of a 3(10)-helix or a beta-turn. 2) The type I beta-turn is a necessary but not a sufficient condition for activity. 3) Our substitutions outside the type I beta-turn of compstatin have altered the turn population but not the turn structure. 4) Flexibility of the beta-turn is essential for activity. 5) The type I beta-turn introduces reversibility and sufficiently separates the two sides of the peptide, whereas the disulfide bridge prevents the termini from drifting apart, thus aiding in the formation of the hydrophobic cluster. 6) The hydrophobic cluster at the linked termini is involved in binding to C3 and activity but alone is not sufficient for activity. 7) beta-Turn residues Gln(5) (Asn(5))-Asp(6)-Trp(7)(Phe(7))-Gly(8) are specific for the turn formation, but only Gln(5)(Asn(5))-Asp(6)-Trp(7)-Gly(8) residues are specific for activity. 8) Trp(7) is likely to be involved in direct interaction with C3, possibly through the formation of a hydrogen bond. Finally we propose a binding model for the C3-compstatin complex.

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Year:  2002        PMID: 11847226     DOI: 10.1074/jbc.M200021200

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


  20 in total

1.  Conformational studies of immunodominant myelin basic protein 1-11 analogues using NMR and molecular modeling.

Authors:  Despina Laimou; Eliada Lazoura; Anastassios N Troganis; Minos-Timotheos Matsoukas; Spyros N Deraos; Maria Katsara; John Matsoukas; Vasso Apostolopoulos; Theodore V Tselios
Journal:  J Comput Aided Mol Des       Date:  2011-11-01       Impact factor: 3.686

2.  New compstatin variants through two de novo protein design frameworks.

Authors:  M L Bellows; H K Fung; M S Taylor; C A Floudas; A López de Victoria; D Morikis
Journal:  Biophys J       Date:  2010-05-19       Impact factor: 4.033

3.  A simple, yet highly accurate, QSAR model captures the complement inhibitory activity of compstatin.

Authors:  Chandrika Mulakala; John D Lambris; Yiannis Kaznessis
Journal:  Bioorg Med Chem       Date:  2006-12-13       Impact factor: 3.641

4.  Kinetics and thermodynamics of type VIII beta-turn formation: a CD, NMR, and microsecond explicit molecular dynamics study of the GDNP tetrapeptide.

Authors:  Patrick F J Fuchs; Alexandre M J J Bonvin; Brigida Bochicchio; Antonietta Pepe; Alain J P Alix; Antonio M Tamburro
Journal:  Biophys J       Date:  2006-01-27       Impact factor: 4.033

Review 5.  Compstatin: a complement inhibitor on its way to clinical application.

Authors:  Daniel Ricklin; John D Lambris
Journal:  Adv Exp Med Biol       Date:  2008       Impact factor: 2.622

6.  A new generation of potent complement inhibitors of the Compstatin family.

Authors:  Aliana López de Victoria; Ronald D Gorham; Meghan L Bellows-Peterson; Jun Ling; David D Lo; Christodoulos A Floudas; Dimitrios Morikis
Journal:  Chem Biol Drug Des       Date:  2011-04-26       Impact factor: 2.817

7.  Design of a modified mouse protein with ligand binding properties of its human analog by molecular dynamics simulations: the case of C3 inhibition by compstatin.

Authors:  Phanourios Tamamis; Panayiota Pierou; Chrystalla Mytidou; Christodoulos A Floudas; Dimitrios Morikis; Georgios Archontis
Journal:  Proteins       Date:  2011-08-30

8.  Novel compstatin family peptides inhibit complement activation by drusen-like deposits in human retinal pigmented epithelial cell cultures.

Authors:  Ronald D Gorham; David L Forest; Phanourios Tamamis; Aliana López de Victoria; Márta Kraszni; Chris A Kieslich; Christopher D Banna; Meghan L Bellows-Peterson; Cynthia K Larive; Christodoulos A Floudas; Georgios Archontis; Lincoln V Johnson; Dimitrios Morikis
Journal:  Exp Eye Res       Date:  2013-08-15       Impact factor: 3.467

9.  Species specificity of the complement inhibitor compstatin investigated by all-atom molecular dynamics simulations.

Authors:  Phanourios Tamamis; Dimitrios Morikis; Christodoulos A Floudas; Georgios Archontis
Journal:  Proteins       Date:  2010-09

10.  Cell membrane modification for rapid display of bi-functional peptides: a novel approach to reduce complement activation.

Authors:  Ledia Goga; Gustavo Perez-Abadia; Sathnur B Pushpakumar; Daniel Cramer; Jun Yan; Nathan Todnem; Gary Anderson; Chirag Soni; John Barker; Claudio Maldonado
Journal:  Open Cardiovasc Med J       Date:  2010-07-20
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