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Literature DB >> 21989937

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.

Phanourios Tamamis¹, Panayiota Pierou, Chrystalla Mytidou, Christodoulos A Floudas, Dimitrios Morikis, Georgios Archontis.

Abstract

The peptide compstatin and its derivatives inhibit the complement-component protein C3 in primate mammals and are potential therapeutic agents against the unregulated activation of complement in humans, but are inactive against C3 from lower mammals. Recent molecular dynamics (MD) simulations showed that the most potent compstatin analog comprised entirely of natural amino acids (W4A9) had a smaller affinity for rat C3, due to reproducible changes in the rat protein structure with respect to the human protein, which eliminated or weakened specific protein-ligand interactions seen in the human C3:W4A9 complex. Here, we study by MD simulations three W4A9 complexes with the mouse C3 protein, and two "transgenic" mouse derivatives, containing a small number (6-9) of human C3 substitutions. The mouse complex experiences the conformational changes and affinity reduction of the rat complex. In the "transgenic" complexes, the conformation remains closer to that of the human complex, the protein-ligand interactions are improved, and the affinity for compstatin becomes "human-like." The present work creates new avenues for a compstatin-sensitive animal model. A similar strategy, involving the comparison of a series of complexes by MD simulations, could be used to design "transgenic" sequences in other systems.

Entities: CellLine Chemical Disease Gene Mutation Species

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Year: 2011 PMID： 21989937 PMCID： PMC3193182 DOI： 10.1002/prot.23149

Source DB: PubMed Journal: Proteins ISSN： 0887-3585

36 in total

1. Studies of structure-activity relations of complement inhibitor compstatin.

Authors: Athena M Soulika; Dimitrios Morikis; Maria-Rosa Sarrias; Melinda Roy; Lynn A Spruce; Arvind Sahu; John D Lambris
Journal: J Immunol Date: 2003-08-15 Impact factor: 5.422

2. CH/pi interactions involving aromatic amino acids: refinement of the CHARMM tryptophan force field.

Authors: Alba T Macias; Alexander D Mackerell
Journal: J Comput Chem Date: 2005-11-15 Impact factor: 3.376

Review 3. Calculation of protein-ligand binding affinities.

Authors: Michael K Gilson; Huan-Xiang Zhou
Journal: Annu Rev Biophys Biomol Struct Date: 2007

4. Conformational analysis of compstatin analogues with molecular dynamics simulations in explicit water.

Authors: Phanourios Tamamis; Spiros S Skourtis; Dimitrios Morikis; John D Lambris; Georgios Archontis
Journal: J Mol Graph Model Date: 2007-04-04 Impact factor: 2.518

Review 5. CHARMM: the biomolecular simulation program.

Authors: B R Brooks; C L Brooks; A D Mackerell; L Nilsson; R J Petrella; B Roux; Y Won; G Archontis; C Bartels; S Boresch; A Caflisch; L Caves; Q Cui; A R Dinner; M Feig; S Fischer; J Gao; M Hodoscek; W Im; K Kuczera; T Lazaridis; J Ma; V Ovchinnikov; E Paci; R W Pastor; C B Post; J Z Pu; M Schaefer; B Tidor; R M Venable; H L Woodcock; X Wu; W Yang; D M York; M Karplus
Journal: J Comput Chem Date: 2009-07-30 Impact factor: 3.376

Review 6. 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

7. Conformational interconversion in compstatin probed with molecular dynamics simulations.

Authors: Buddhadeb Mallik; John D Lambris; Dimitrios Morikis
Journal: Proteins Date: 2003-10-01

8. 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

9. Generalized born model with a simple smoothing function.

Authors: Wonpil Im; Michael S Lee; Charles L Brooks
Journal: J Comput Chem Date: 2003-11-15 Impact factor: 3.376

10. Improvement of the anti-C3 activity of compstatin using rational and combinatorial approaches.

Authors: D Morikis; A M Soulika; B Mallik; J L Klepeis; C A Floudas; J D Lambris
Journal: Biochem Soc Trans Date: 2004-02 Impact factor: 5.407

16 in total

1. Molecular recognition of CXCR4 by a dual tropic HIV-1 gp120 V3 loop.

Authors: Phanourios Tamamis; Christodoulos A Floudas
Journal: Biophys J Date: 2013-09-17 Impact factor: 4.033

2. 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

3. Editor's Highlight: Microbial-Derived 1,4-Dihydroxy-2-naphthoic Acid and Related Compounds as Aryl Hydrocarbon Receptor Agonists/Antagonists: Structure-Activity Relationships and Receptor Modeling.

Authors: Yating Cheng; Un-Ho Jin; Laurie A Davidson; Robert S Chapkin; Arul Jayaraman; Phanourios Tamamis; Asuka Orr; Clint Allred; Michael S Denison; Anatoly Soshilov; Evelyn Weaver; Stephen Safe
Journal: Toxicol Sci Date: 2016-11-11 Impact factor: 4.849

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.

1. Studies of structure-activity relations of complement inhibitor compstatin.

2. CH/pi interactions involving aromatic amino acids: refinement of the CHARMM tryptophan force field.

Review 3. Calculation of protein-ligand binding affinities.

4. Conformational analysis of compstatin analogues with molecular dynamics simulations in explicit water.

Review 5. CHARMM: the biomolecular simulation program.

Review 6. Compstatin: a complement inhibitor on its way to clinical application.

7. Conformational interconversion in compstatin probed with molecular dynamics simulations.

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

9. Generalized born model with a simple smoothing function.

10. Improvement of the anti-C3 activity of compstatin using rational and combinatorial approaches.

1. Molecular recognition of CXCR4 by a dual tropic HIV-1 gp120 V3 loop.

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

3. Editor's Highlight: Microbial-Derived 1,4-Dihydroxy-2-naphthoic Acid and Related Compounds as Aryl Hydrocarbon Receptor Agonists/Antagonists: Structure-Activity Relationships and Receptor Modeling.

4. Molecular dynamics in drug design: new generations of compstatin analogs.

5. Insights from molecular dynamics simulations for computational protein design.

6. Molecular Mechanism for Attractant Signaling to DHMA by E. coli Tsr.

7. N-Formyl-Perosamine Surface Homopolysaccharides Hinder the Recognition of Brucella abortus by Mouse Neutrophils.

8. Molecular recognition of CCR5 by an HIV-1 gp120 V3 loop.

9. Insights into the structure, correlated motions, and electrostatic properties of two HIV-1 gp120 V3 loops.

10. Elucidating a key component of cancer metastasis: CXCL12 (SDF-1α) binding to CXCR4.