Your search keyword '"Conformational analysi"' showing total 35 results

1. In-Peptide Synthesis of Imidazolidin-2-one Scaffolds, Equippable with Proteinogenic or Taggable/Linkable Side Chains, General Promoters of Unusual Secondary Structures

Author

Junwei Zhao, Luca Gentilucci, Arianna Greco, Simone Ioannone, Rossella De Marco, De Marco R., Zhao J., Greco A., Ioannone S., and Gentilucci L.

Subjects

Models, Molecular, Stereochemistry, Imidazolidinone, Peptidomimetic, Sequence (biology), Chemistry Techniques, Synthetic, Imidazolidines, 010402 general chemistry, Ring (chemistry), 01 natural sciences, Imidazolidin-2-one, Protein Structure, Secondary, chemistry.chemical_compound, Protein structure, Imidazolidin-2-one, Dap, Scaffolds, peptide, Side chain, Peptide synthesis, Peptide bond, Scaffolds, 010405 organic chemistry, Chemistry, Organic Chemistry, imidazolidinone, Dap, peptide, peptidomimetic, 0104 chemical sciences, conformational analysi, Peptides, unusual turn

Abstract

Peptidomimetics containing ( S)- or ( R)-imidazolidin-2-one-4-carboxylate (Imi) have been obtained by the expedient in-peptide cyclization of ( S)- or ( R)-α,β-diaminopropionic acid (Dap) residues. These Imi scaffolds behave as proline analogues characterized by a flat structure and a trans-restricted geometry of the preceding peptide bond and induce well-defined secondary structures in a biomimetic environment. While ( S)-Imi peptides adopted a γ'-turn conformation, ( R)-Imi induced the contemporary formation of a γ-turn and a rare 11-membered H-bonded structure in the 2→4 opposite direction of the sequence, identified as a e-turn. In order to exploit these Imi scaffolds as general promoters of unusual secondary structures, proteinaceous side chains have been introduced at the N1 position of the five-membered ring, potentially mimicking any residues. Finally, the Imi rings have been equipped with unnatural side chains or with functionalized substituents, which can be utilized as linkers to chemoselectively bind the Imi-peptides onto nanoparticles, biomaterials, or diagnostic probes.

Published

2019

2. A novel β-hairpin peptide derived from the ARC repressor selectively interacts with the major groove of B-DNA

Author

Jussara Amato, José L. Mascareñas, Azzurra Stefanucci, Soraya Learte-Aymamí, Diego Brancaccio, Ettore Novellino, Laura Mayol, Federica Santoro, Alfonso Carotenuto, Adriano Mollica, Bruno Pagano, Antonio Randazzo, Jéssica Rodríguez, Stefanucci, A., Amato, J., Brancaccio, D., Pagano, B., Randazzo, A., Santoro, F., Mayol, L., Learte-Aymami, S., Rodriguez, J., Mascarenas, J. L., Novellino, E., Carotenuto, A., and Mollica, A.

Subjects

Circular dichroism, β-hairpin peptides, Stereochemistry, Repressor, Peptide, Conformational analysi, Antiparallel (biochemistry), 01 natural sciences, Biochemistry, Insert (molecular biology), DNA sequencing, chemistry.chemical_compound, Drug Discovery, Structural motif, Molecular Biology, chemistry.chemical_classification, Molecular Structure, 010405 organic chemistry, Organic Chemistry, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, chemistry, ARC repressor, DNA major groove binder, Transcription factor, DNA, B-Form, Peptides, DNA, Transcription Factors

Abstract

Transcription factors (TFs) have a remarkable role in the homeostasis of the organisms and there is a growing interest in how they recognize and interact with specific DNA sequences. TFs recognize DNA using a variety of structural motifs. Among those, the ribbon-helix-helix (RHH) proteins, exemplified by the MetJ and ARC repressors, form dimers that insert antiparallel β-sheets into the major groove of DNA. A great chemical challenge consists of using the principles of DNA recognition by TFs to design minimized peptides that maintain the DNA affinity and specificity characteristics of the natural counterparts. In this context, a peptide mimic of an antiparallel β-sheet is very attractive since it can be obtained by a single peptide chain folding in a β-hairpin structure and can be as short as 14 amino acids or less. Herein, we designed eight linear and two cyclic dodeca-peptides endowed with β-hairpins. Their DNA binding properties have been investigated using fluorescence spectroscopy together with the conformational analysis through circular dichroism and solution NMR. We found that one of our peptides, peptide 6, is able to bind DNA, albeit without sequence selectivity. Notably, it shows a topological selectivity for the major groove of the DNA which is the interaction site of ARC and many other DNA-binding proteins. Moreover, we found that a type I' β-hairpin folding pattern is a favorite peptide structure for interaction with the B-DNA major groove. Peptide 6 is a valuable lead compound for the development of novel analogs with sequence selectivity.

Published

2021

3. Targeting EphA2-Sam and Its Interactome: Design and Evaluation of Helical Peptides Enriched in Charged Residues

Author

Daniela Marasco, Concetta Di Natale, Luciano Pirone, Susan Costantini, Flavia Anna Mercurio, Marilisa Leone, Emilia Pedone, Mercurio, Flavia A., Marasco, Daniela, Dinatale, Concetta, Pirone, Luciano, Costantini, Susan, Pedone, Emilia M., and Leone, Marilisa

Subjects

0301 basic medicine, Magnetic Resonance Spectroscopy, Peptide, EphA2, Molecular Dynamics Simulation, Conformational analysi, Endocytosis, Biochemistry, Interactome, Protein Structure, Secondary, 03 medical and health sciences, Molecular dynamics, 0302 clinical medicine, Downregulation and upregulation, Sam domain, Amino Acid Sequence, Surface plasmon resonance, Receptor, Molecular Biology, Solid-Phase Synthesis Techniques, Cancer, chemistry.chemical_classification, Chemistry, Microscale thermophoresis, Circular Dichroism, Receptor, EphA2, Organic Chemistry, Surface Plasmon Resonance, Recombinant Proteins, Sterile Alpha Motif, Kinetics, 030104 developmental biology, Drug Design, 030220 oncology & carcinogenesis, Biophysics, Molecular Medicine, Helical peptide, Peptides, Protein Binding

Abstract

The EphA2 receptor controls diverse physiological and pathological conditions and its levels are often upregulated in cancer. Targeting receptor overexpression, through modulation of endocytosis and consequent degradation, appears to be an appealing strategy for attacking tumor malignancy. In this scenario, the Sam domain of EphA2 plays a pivotal role because it is the site where protein regulators of endocytosis and stability are recruited by means of heterotypic Sam-Sam interactions. Because EphA2-Sam heterotypic complexes are largely based on electrostatic contacts, we have investigated the possibility of attacking these interactions with helical peptides enriched in charged residues. Several peptide sequences with high predicted helical propensities were designed, and detailed conformational analyses were conducted by diverse techniques including NMR, CD, and molecular dynamics (MD) simulations. Interaction studies were also performed by NMR, surface plasmon resonance (SPR), and microscale thermophoresis (MST) and led to the identification of two peptides capable of binding to the first Sam domain of Odin. These molecules represent early candidates for the generation of efficient Sam domain binders and antagonists of Sam-Sam interactions involving EphA2.

Published

2016

4. Heterocyclic Scaffolds in the Design of Peptidomimetic Integrin Ligands: Synthetic Strategies, Structural Aspects, and Biological Activity

Author

Arianna Greco, Luca Gentilucci, Rossella De Marco, Giacomo Mazzotti, De Marco, Rossella, Mazzotti, Giacomo, Greco, Arianna, and Gentilucci, Luca

Subjects

Integrins, Integrin receptors, Peptidomimetic, Integrin, Computational biology, Ligands, Structure-Activity Relationship, Heterocyclic Compounds, Drug Discovery, Animals, Humans, Structure–activity relationship, Cancer, Molecular Structure, biology, Chemistry, Heterocycle, Antagonist, Rational design, Biological activity, General Medicine, Combinatorial chemistry, Conformational analysis, Dipeptide scaffold, Molecular docking, Drug Design, conformational analysi, biology.protein, peptidomimetic, Peptidomimetics, ECM Protein

Abstract

The integrin receptors represent valuable targets for therapeutic interventions; being overexpressed in many pathological states, their inhibition can be effective to treat a number of severe diseases. Since integrin functions are mediated by interactions with ECM protein ligands, the inhibition can be achieved by interfering with such interactions using small mimetics of the integrin-ligand recognition motifs (e.g. RGD, LDV, etc.). In this review, we focus on the antagonists with peptideheterocycle hybrid structures. The introduction of well-designed scaffolds has met considerable success in the rational design of highly stable, bioavailable, and conformationally defined antagonists. Two main approaches are discussed herein. The first approach is the use of scaffolds external to the main recognition motifs, aimed at improving conformational definition. In the second approach, heterocyclic cores are introduced within the recognition motifs, giving access to libraries of 3D diverse candidate antagonists.

Published

2015

5. Detection of Significant Aprotic Solvent Effects on the Conformational Distribution of Methyl 4-Nitrophenyl Sulfoxide: From Gas-Phase Rotational to Liquid-Crystal NMR Spectroscopy

Author

Maria Enrica Di Pietro, Giorgio Cinacchi, Sonia Melandri, Giuseppina De Luca, Giorgio Celebre, Barbara M. Giuliano, Celebre, Giorgio, De Luca, Giuseppina, Di Pietro, Maria Enrica, Giuliano, Barbara Michela, Melandri, Sonia, and Cinacchi, Giorgio

Subjects

Quantitative Biology::Biomolecules, solvent effect, LXNMR spectroscopy, Analytical chemistry, microwave technique, QM calculation, Sulfoxide, Nuclear magnetic resonance spectroscopy, Atomic and Molecular Physics, and Optics, Solvent, chemistry.chemical_compound, Electric dipole moment, chemistry, Liquid crystal, conformational analysi, Polar, Physical chemistry, Rotational spectroscopy, Physical and Theoretical Chemistry, Solvent effects

Abstract

The conformational equilibrium of methyl 4-nitrophenyl sulfoxide (MNPSO) was experimentally investigated in the gas phase by using microwave spectroscopy and in isotropic and nematic liquid-crystal solutions, in which the solvents are nonaqueous and aprotic, by using NMR spectroscopy; moreover, it was theoretically studied in vacuo and in solution at different levels of theory. The overall set of results indicates a significant dependence of the solute conformational distribution on the solvent dielectric permittivity constant: when dissolved in low-polarity media, the most stable conformation of MNPSO proved to be strongly twisted with respect to that in more polar solvents, in which the conformational distribution maximum essentially coincides with that obtained in the gas phase. We discuss a possible explanation of this behavior, which rests on electrostatic solute-solvent interactions and is supported by calculations of the solute electric dipole moment as a function of the torsional angle. This function shows that the least polar conformation of MNPSO is located at a twist angle close to that of the conformational distribution maximum found in less-polar solvents. This fact, associated with a relatively flat torsional potential, can justify the stabilization of the twisted conformation by the less-polar solvents.

Published

2015

6. Form Matters: Stable Helical Foldamers Preferentially Target Human Monocytes and Granulocytes

Author

Nicola Zanna, Giulia Malachin, Benedetta Del Secco, Emanuele Papini, Andrea Cornia, Lorenzo Milli, Claudia Tomasini, Regina Tavano, Del Secco, Benedetta, Malachin, Giulia, Milli, Lorenzo, Zanna, Nicola, Papini, Emanuele, Cornia, Andrea, Tavano, Regina, and Tomasini, Claudia

Subjects

Molecular Conformation, Biocompatible Materials, Crystallography, X-Ray, Conformational analysi, 01 natural sciences, Biochemistry, Monocytes, HeLa, Peptoids, chemistry.chemical_compound, Drug Discovery, Rhodamine B, Moiety, foldamers, Amino Acids, General Pharmacology, Toxicology and Pharmaceutics, Cells, Cultured, Microscopy, Confocal, biology, Chemistry, Circular Dichroism, conformational analysis, Biological activity, Cell sorting, bioconjugates, leukocytes, peptides, Peptide, Molecular Medicine, Fluorescent tag, Cell type, Biocompatibility, Cell Survival, Toxicology and Pharmaceutics (all), 010402 general chemistry, Foldamer, Humans, Pharmacology, 010405 organic chemistry, Organic Chemistry, Leukocyte, biology.organism_classification, 0104 chemical sciences, Pharmacology, Toxicology and Pharmaceutics (all), Bioconjugate, Granulocytes, HeLa Cells

Abstract

Some hybrid foldamers of various length, all containing the (4R,5S)-4-carboxy-5-methyloxazolidin-2-one (d-Oxd) moiety alternating with an l-amino acid (l-Val, l-Lys, or l-Ala), were prepared in order to study their preferred conformations and to evaluate their biological activity. Surprisingly, only the longer oligomers containing l-Ala fold into well-established helices, whereas all the other oligomers give partially unfolded turn structures. Nevertheless, they all show good biocompatibility, with no detrimental effects up to 64 μm. After equipping some selected foldamers with the fluorescent tag rhodamine B, a quantitative analysis was performed by dose- and time-response fluorescence-activated cell sorting (FACS) assays with human HeLa cells and primary blood lymphocytes, granulocytes, and monocytes. Among the cell types analyzed, the oligomers associated with monocytes and granulocytes with greatest efficacy, still visible after 24 h incubation. This effect is even more pronounced for foldamers that are able to form stable helices.

Published

2017

7. Receptor-Bound Conformation of Cilengitide Better Represented by Its Solution-State Structure than the Solid-State Structure

Author

Bernhard Wahl, Michael Groll, Valeria La Pietra, Udaya Kiran Marelli, Ettore Novellino, Luciana Marinelli, Horst Kessler, Eberhardt Herdtweck, Andreas O. Frank, Marelli, Udaya Kiran, Frank, Andreas O, Wahl, Bernhard, LA PIETRA, Valeria, Novellino, Ettore, Marinelli, Luciana, Herdtweck, Eberhardt, Groll, Michael, and Kessler, Horst

Subjects

Models, Molecular, Molecular model, Protein Conformation, Stereochemistry, Integrin, Molecular Conformation, Cilengitide, Crystallography, X-Ray, Catalysis, chemistry.chemical_compound, NMR spectroscopy, Protein structure, Nuclear Magnetic Resonance, Biomolecular, X-ray crystallography, Integrin alphaVbeta3, biology, Ligand, Snake Venom, Organic Chemistry, General Chemistry, Nuclear magnetic resonance spectroscopy, peptide, Solutions, Crystallography, chemistry, Drug Design, conformational analysi, biology.protein, Snake Venoms

Abstract

The X-ray crystal and NMR spectroscopic structures of the peptide drug candidate Cilengitide (cyclo(RGDf(NMe)Val)) in various solvents are obtained and compared in addition to the integrin receptor bound conformation. The NMR-based solution structures exhibit conformations closely resembling the X-ray structure of Cilengitide bound to the head group of integrin αvβ3. In contrast, the structure of pure Cilengitide recrystallized from methanol reveals a different conformation controlled by the lattice forces of the crystal packing. Molecular modeling studies of the various ligand structures docked to the αvβ3 integrin revealed that utilization of the solid-state conformation of Cilengitide leads-unlike the solution-based structures-to a mismatch of the ligand-receptor interactions compared with the experimentally determined structure of the protein-ligand complex. Such discrepancies between solution and crystal conformations of ligands can be misleading during the structure-based lead optimization process and should thus be taken carefully into account in ligand orientated drug design.

Published

2014

8. Structural features of the C8 antiviral peptide in a membrane-mimicking environment

Author

Anna Maria D'Ursi, Mario Scrima, Stefano Piotto, Manuela Grimaldi, Giuseppe Vitiello, Sara Di Marino, Federica Campana, Gerardino D'Errico, Scrima, Mario, DI MARINO, Sara, Grimaldi, Manuela, Campana, Federica, Vitiello, Giuseppe, Piotto, Stefano Piotto, D'Errico, Gerardino, and D'Ursi, Anna Maria

Subjects

Circular dichroism, Magnetic Resonance Spectroscopy, Stereochemistry, Protein Conformation, Phospholipid, Biophysics, Peptide, Molecular Dynamics Simulation, Conformational analysi, Micelle, Antiviral Agents, Biochemistry, Fluorescence, Hydrophobic effect, Molecular dynamics, chemistry.chemical_compound, Peptide Fragment, Viral Envelope Proteins, Animals, Humans, Antiviral Agent, chemistry.chemical_classification, Spin Label, Animal, Circular Dichroism, NMR, Conformational analysis, Cell Membrane, Viral fusion, Cat, Viral Envelope Protein, Cell Biology, Peptide Fragments, Membrane, chemistry, Cellular Microenvironment, Cats, Spin Labels, Glycoprotein, Human

Abstract

C8, a short peptide characterized by three regularly spaced Trp residues, belongs to the membrane-proximal external functional domains of the feline immunodeficiency virus coat protein gp36. It elicits antiviral activity as a result of blocking cell entry and exhibits membranotropic and fusogenic activities. Membrane-proximal external functional domains of virus coat proteins are potential targets in the development of new anti-HIV drugs that overcome the limitations of the current anti-retroviral therapy. In the present work, we studied the conformation of C8 and its interaction with micellar surfaces using circular dichroism, nuclear magnetic resonance and fluorescence spectroscopy. The experimental data were integrated by molecular dynamics simulations in a micelle–water system. Our data provide insight into the environmental conditions related to the presence of the fusogenic peptide C8 on zwitterionic or negatively charged membranes. The membrane charge modulates the conformational features of C8. A zwitterionic membrane surface induces C8 to assume canonical secondary structures, with hydrophobic interactions between the Trp residues and the phospholipid chains of the micelles. A negatively charged membrane surface favors disordered C8 conformations and unspecific superficial interactions, resulting in membrane destabilization.

Published

2014

9. Synthesis of mixed MOR/KOR efficacy cyclic opioid peptide analogs with antinociceptive activity after systemic administration

Author

Rossella De Marco, Anna Janecka, Csaba Tömböly, Renata Perlikowska, Justyna Piekielna, Alicja Kluczyk, Roberto Artali, Luca Gentilucci, Maria Camilla Cerlesi, Girolamo Calo, Perlikowska, Renata, Piekielna, Justyna, Gentilucci, Luca, De Marco, Rossella, Cerlesi, Maria Camilla, Calo, Girolamo, Artali, Roberto, Tömböly, Csaba, Kluczyk, Alicja, and Janecka, Anna

Subjects

Male, 0301 basic medicine, Wistar, Receptors, Opioid, mu, Peptide, Phenylalanine, Conformational analysi, Antinociception, Mice, Receptors, Drug Discovery, Binding studies, Calcium mobilization assay, Conformational analysis, Endomorphins, Hot-plate test, Molecular docking, ROESY, Drug Discovery3003 Pharmaceutical Science, Organic Chemistry, Pharmacology, Hot plate test, Receptor, chemistry.chemical_classification, Analgesics, Cyclic, Chemistry, General Medicine, Analgesics, Opioid, Molecular Docking Simulation, Nociception, Systemic administration, Oligopeptide, Cricetulu, Oligopeptides, Endomorphin, Stereochemistry, Guinea Pigs, Socio-culturale, Pain, Opioid, CHO Cells, Peptides, Cyclic, Guinea Pig, Structure-Activity Relationship, 03 medical and health sciences, Residue (chemistry), Cricetulus, Binding studie, Animals, Amino Acid Sequence, Rats, Wistar, Opioid peptide, kappa, Animal, Receptors, Opioid, kappa, Rats, 030104 developmental biology, CHO Cell, mu, Peptides

Abstract

Cyclic pentapeptide Tyr-c[D-Lys-Phe-Phe-Asp]NH2, based on the structure of endomorphin-2 (EM-2), which shows high affinity to the μ-opioid receptor (MOR) and a very strong antinociceptive activity in mice was used as a parent compound for the structure–activity relationship studies. In this report we synthesized analogs of a general sequence Dmt-c[D-Lys-Xaa-Yaa-Asp]NH2, with D-1- or D-2-naphthyl-3-alanine (D-1-Nal or D-2-Nal) in positions 3 or 4. In our earlier papers we have indicated that replacing a phenylalanine residue by the more extended aromatic system of naphthylalanines may result in increased bioactivities of linear analogs. The data obtained here showed that only cyclopeptides modified in position 4 retained the sub-nanomolar MOR and nanomolar κ-opioid receptor (KOR) affinity, similar but not better than that of a parent cyclopeptide. In the in vivo mouse hot-plate test, the most potent analog, Dmt-c[D-Lys-Phe-D-1-Nal-Asp]NH2, exhibited higher than EM-2 but slightly lower than the cyclic parent peptide antinociceptive activity after peripheral (ip) and also central administration (icv). Conformational analyses in a biomimetic environment and molecular docking studies disclosed the structural determinants responsible for the different pharmacological profiles of position 3- versus position 4-modified analogs.

Published

2016

10. C-terminal truncation of Vascular Endothelial Growth Factor mimetic helical peptide preserves structural and receptor binding properties

Author

Roberto Fattorusso, Donatella Diana, Luca Domenico D'Andrea, Barbara Ziaco, Domenica Capasso, Rossella Di Stasi, Veronica Celentano, Rosanna Palumbo, Ziaco, B, Diana, D, Capasso, D, Palumbo, R, Celentano, V, Di Stasi, R, Fattorusso, Roberto, and D'Andrea, L. D.

Subjects

Vascular Endothelial Growth Factor A, Angiogenesis, Peptidomimetic, VEGF receptors, Biophysics, Neovascularization, Physiologic, Sequence (biology), Peptide, Conformational analysi, Biochemistry, Protein Structure, Secondary, chemistry.chemical_compound, Biomimetic Materials, Cell Line, Tumor, Humans, Therapeutic angiogenesis, Nuclear Magnetic Resonance, Biomolecular, Molecular Biology, chemistry.chemical_classification, Helix, Vascular Endothelial Growth Factor Receptor-1, Neovascularization, Pathologic, biology, Circular Dichroism, Cell Biology, VEGF, NMR, Conformational analysis, Vascular endothelial growth factor, chemistry, biology.protein, Peptides, Protein Binding

Abstract

Vascular Endothelial Growth Factor mimetic peptides have interesting applications in therapeutic angiogenesis. Recently, we described the proangiogenic properties of a 15 mer peptide designed on the N-terminal helix 17-25 of VEGF. The peptide was stabilized introducing well known peptide chemical tools among which N- and C-terminal capping sequence. Here, we show that the C-terminal sequence does not affect the structural and biological properties of the full-length peptide. In fact, a C-terminal truncated analog peptide resulted in a well folded and stable helix retaining the ability to bind to VEGF receptors. This study will allow to develop smaller peptidomimetic analogs able to modulate the VEGF-dependent angiogenesis. © 2012 Elsevier Inc.

Published

2012

11. The pseudo-βI-turn

Author

H. Matter, H.-J. Diehl, C. Isernia, Horst Kessler, Gerd Gemmecker, Siggi Mronga, Kessler, H, Matter, H, Gemmecker, G, Diehl, Hj, Isernia, Carla, and Mronga, S.

Subjects

chemistry.chemical_classification, Chemistry, Stereochemistry, Hydrogen bond, cis peptide bond, molecular dynamic, Biochemistry, Cyclic peptide, pseudo‐βI‐turn, Turn (biochemistry), Heteronuclear molecule, conformational analysi, Peptide bond, Molecule, proline, Chirality (chemistry), Isomerization

Abstract

Synthesis and conformational analysis of three cyclic hexapeptides cyclo(-Gly1-Pro2-Phe3-Val4-Xaa5-Phe6), Xaa = Phe (I), D-Phe (II) and D-Pro (III), were carried out to examine the influence of proline on the formation of reverse turns and the dynamics of hydrophobic peptide regions. Assignment of all 1H and 13C resonances was achieved by homo- and heteronuclear 2D-NMR techniques (TOCSY, ROESY, HMQC, HMQC-TOCSY and HMBCS-270). The conformational analysis is based on interproton distances derived from ROESY spectra and homo- and heteronuclear coupling constants (E.COSY, HETLOC and HMBCS-270). For structural refinements restrained molecular dynamics (MD) simulations in vacuo and in DMSO were performed. Each peptide exhibits two conformations in DMSO solution due to cis-trans isomerism about the Gly-Pro peptide bond. Surprisingly the cis-Gly-Pro segment in the minor isomers is not involved in a beta VI-turn, but forms a turn structure with cis-Gly-Pro in the i and i + 1 positions. Although no stabilizing hydrogen bond is found in this turn, the phi- and psi-angles closely correspond to a beta I-turn [Pro2: phi(i + 1) -60 degrees, psi(i + 1) -30 degrees; Phe3: phi(i + 2) -100 degrees, psi(i + 2) -50 degrees]. Hence we call this structural element a pseudo-beta I-turn. As expected, in the dominating all-trans isomers proline occupies the i + 1 position of a standard beta I-turn. Therefore, cis-trans isomerization of the Gly1-Pro2 amide bond only induces a local conformational rearrangement, with minor structural changes in other parts of the molecule. However, the geometry of the other regions is affected by the chirality of the i + 1 amino acid for both isomers (beta I for Phe5, beta II' for D-Phe5 or D-Pro5).

Published

2009

12. Conformational versatility of the Nα-acylated tripeptide amide tail of oxytocin

Author

Carla Isernia, Claudio Toniolo, Vincenzo Pavone, Michele Saviano, Ettore Benedetti, Marco Crisma, G. Valle, Angelina Lombardi, N. Fabiano, Benedetto Di Blasio, Carlo Pedone, Fabiano, N, Valle, G, Crisma, M, Toniolo, C, Saviano, M, Lombardi, A, Isernia, Carla, Pavone, V, DI BLASIO, B, and Pedone, C.

Subjects

integumentary system, Stereochemistry, Hydrogen bond, Chemistry, Sequence (biology), Tripeptide, Crystal structure, crystal state structure, Biochemistry, Peptide Conformation, X‐ray diffraction: β‐turn, Crystallography, chemistry.chemical_compound, Amide, Glycine, conformational analysi, Molecule, peptide conformation, oxytocin tail tripeptide amide, α,α, ‐disubstituted glycine

Abstract

The synthesis, physical and analytical characterization, and crystal‐state structural analysis by X‐ray diffraction of three analogues of the Nα‐acylated tripeptide amide tail of oxytocin, each containing a cyclic Cα, α‐ disubstituted glycine at position 2, have been performed. The peptides arc Boc‐L‐Pro‐Ac3c‐Gly‐NH2, Z‐L‐Pro‐Ac5c‐Gly‐NH2 and Z‐L‐Pro‐Ac5c‐Gly‐NH2. While the former is folded in a type‐II β‐turn conformation at the ‐L‐Pro‐Ac3c‐ sequence, the two latter tripeptides form two consecutive (type‐II, type‐I′) β‐turns. The Ac5c‐ and Ac6c‐tripeptides are the first examples of such a highly folded structural combination in a position‐2 analogue of the Nα‐acylated ‐L‐Pro‐L‐Leu‐GIy‐NH2 sequence. Copyright © 1993, Wiley Blackwell. All rights reserved

Published

2009

13. 5-aminomethyloxazolidine-2,4-dione hybrid α/β-dipeptide scaffolds as inductors of constrained conformations: Applications to the synthesis of integrin antagonists

Author

Rossella, De Marco, Giacomo, Mazzotti, Samantha D, Dattoli, Monica, Baiula, Santi, Spampinato, Arianna, Greco, Luca, Gentilucci, De Marco, Rossella, Mazzotti, Giacomo, Dattoli, Samantha D., Baiula, Monica, Spampinato, Santi, Greco, Arianna, and Gentilucci, Luca

Subjects

Small Molecule Libraries, Integrins, jurkat cell, integrin inhibitor, Molecular Conformation, conformational analysi, conformational analysis, freidinger lactam, jurkat cells, Peptidomimetics, β2-amino acid, Oxazolidinones

Abstract

Peptidomimetics represent an attractive starting point for drug discovery programs; in particular, peptidomimetics that result from the incorporation of a heterocycle may take advantage of increased enzymatic stability and higher ability to reproduce the bioactive conformations of the parent peptides, resulting in enhanced therapeutic potential. Herein, we present mimetics of the α4β1 integrin antagonist BIO1211 (MPUPA-Leu-Asp-Val-Pro-OH), containing a aminomethyloxazolidine-2,4-dione scaffold (Amo). Interestingly, the retro-sequences PhCOAsp(OH)-Amo-APUMP including either (S)- or (R)-configured Amo displayed significant ability to inhibit the adhesion of α4β1 integrin expressing cells, and remarkable stability in mouse serum. Possibly, the conformational bias exerted by the Amo scaffold determined the affinity for the receptors. These peptidomimetics could be of interest for the development of small-molecule agents effective against inflammatory processes and correlated autoimmune diseases. © 2015 Wiley Periodicals, Inc. Biopolymers (Pept Sci) 104: 636-649, 2015.

Published

2015

14. Myelography iodinated contrast media. I. unraveling the atropisomerism properties in solution

Author

Nicola D'Amelio, Marco Paolantoni, Amelia Gamini, Attilio Cesàro, Fulvio Uggeri, Letizia Tavagnacco, John W. Brady, Luca Fontanive, Alessandro Maiocchi, Fontanive, Luca, D'Amelio, Nicola, Cesaro, Attilio, Gamini, Amelia, Tavagnacco, Letizia, Paolantoni, Marco, Brady, John W., Maiocchi, Alessandro, and Uggeri, Fulvio

Subjects

Steric effects, Magnetic Resonance Spectroscopy, Stereochemistry, Iohexol, atropisomerism, Population, Iomeprol, Pharmaceutical Science, Contrast Media, iodinated contrast media, conformational analysis, NMR, IR, MM, Iopamidol, chemistry.chemical_compound, Computational chemistry, Drug Discovery, Spectroscopy, Fourier Transform Infrared, medicine, Molecule, education, Conformational isomerism, Myelography, education.field_of_study, Atropisomer, Iopromide, Solutions, chemistry, conformational analysi, Molecular Medicine, medicine.drug

Abstract

The present work reports a thorough conformational analysis of iodinated contrast media: iomeprol, iopamidol (the world's most utilized contrast agent), and iopromide. Its main aim is the understanding of the complex structural features of these atropisomeric molecules, characterized by the presence of many conformers with hindered rotations, and of the role of atropisomerism in the physicochemical properties of their aqueous solutions. The problem was tackled by using an extensive analysis of (13)C NMR data on the solutions of whole molecules and of simple precursors in addition to FT-IR investigation and molecular simulations. This analysis demonstrated that out of the many possible atropisomers, only a few are significantly populated, and their relative population is provided. The conformational analysis also indicated that the presence of a sterically hindered amidic bond, allowing a significant population of cis forms (E in iopromide and exo in iomeprol), may be the basis for an increased thermodynamic solubility of concentrated solutions of iomeprol.

Published

2015

15. Characterization of the species-dependent ketoprofen/albumin binding modes by induced CD spectroscopy and TD-DFT calculations

Author

Carlo Bertucci, Marco Pistolozzi, Daniele Tedesco, Riccardo Zanasi, Daniele Tedesco, Marco Pistolozzi, Riccardo Zanasi, and Carlo Bertucci

Subjects

Ketoprofen, Circular dichroism, Serum albumins, Magnetic Resonance Spectroscopy, Clinical Biochemistry, Pharmaceutical Science, Drug binding, Conformational analysi, Crystallography, X-Ray, Spectral line, Analytical Chemistry, Stereospecificity, Drug Discovery, medicine, Spectroscopy, Serum Albumin, Chemistry, Circular Dichroism, Albumin, Stereoisomerism, Characterization (materials science), Induced circular dichroism, Crystallography, Conformational analysis, Density functional theory, medicine.drug

Abstract

Accepted Manuscript version. The Published Journal Article is available on the Journal of Pharmaceutical and Biomedical Analysis, Volume 112, pages 176–180 (DOI: https://doi.org/10.1016/j.jpba.2014.11.029). Supplementary Material available free of charge on the article webpage. © 2014. This Manuscript version is made available under the CC-BY-NC-ND 4.0 license. https://creativecommons.org/licenses/by-nc-nd/4.0/ ABSTRACT The stereospecificity of high-affinity biorecognition phenomena at the basis of the activity of drugs is an important topic of active research in medicinal chemistry. The binding of drugs to their targets or to carrier proteins may lead to the onset of an induced circular dichroism (ICD) signal, which can be detected experimentally. Quantum mechanical (QM) calculations based on density functional theory (DFT) and its time-dependent formulation (TD-DFT) can be used to determine the theoretical chiroptical response of all the possible conformations of drugs bound to their hosts; by comparison with the experimental ICD spectra of drug-host complexes, this approach can lead to the identification of possible binding modes in the absence of X-ray crystallography or NMR data. The present article reports the application of experimental electronic circular dichroism (ECD) spectroscopy, DFT conformational analysis and TD-DFT calculations to the investigation of the binding modes of (S)-ketoprofen to serum albumins. The peculiar species-dependent ICD spectra observed for the binding of (S)-ketoprofen to different serum albumins can be explained by the selection of different mutual arrangements of the phenyl moieties inside the binding pocket. Such structural elucidations contribute to a better understanding of the changes in the pharmacokinetic and pharmacodynamic profiles of drugs among different species.

Published

2014

16. Conformational sensitivity of conjugated poly(ethylene oxide)-poly(amidoamine) molecules to cations adducted upon electrospray ionization - A mass spectrometry, ion mobility and molecular modeling study

Author

Qi Wang, Gilles Quéléver, Ling Peng, Sabrina Pricl, Laurence Charles, Stéphane Viel, Christophe Chendo, Aura Tintaru, Paola Posocco, Institut de Chimie Radicalaire (ICR), Aix Marseille Université (AMU)-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS), School of Mathematics and Statistics [Wuhan], Wuhan University [China], Institut de Biologie du Développement de Marseille (IBDM), Aix Marseille Université (AMU)-Centre National de la Recherche Scientifique (CNRS), Centre Interdisciplinaire de Nanoscience de Marseille (CINaM), Tintaru, A, Chendo, C, Wang, Q, Viel, S, Quéléve, G, Peng, L, Posocco, Paola, Pricl, Sabrina, and Charles, L.

Subjects

Models, Molecular, Spectrometry, Mass, Electrospray Ionization, Electrospray ionization, Inorganic chemistry, Molecular Conformation, Protonation, Lithium, Molecular Dynamics Simulation, 010402 general chemistry, Mass spectrometry, 01 natural sciences, Biochemistry, Dissociation (chemistry), Polyethylene Glycols, Analytical Chemistry, Cations, Crown Ethers, Dendrimer, Polyamines, Environmental Chemistry, Molecule, [CHIM]Chemical Sciences, Spectroscopy, mass spectrometry, Biomolecules, Chemistry, Hydrogen bond, dendrimers and dendron, 010401 analytical chemistry, conformational analysis, Poly(amidoamine), 0104 chemical sciences, Crystallography, dendrimers and dendrons, Molecular simulations, Molecular simulation, conformational analysi

Abstract

International audience; Tandem mass spectrometry and ion mobility spectrometry experiments were performed on multiply charged molecules formed upon conjugation of a poly(amidoamine) (PAMAM) dendrimer with a poly(ethylene oxide) (PEO) linear polymer to evidence any conformational modification as a function of their charge state (2+ to 4+) and of the adducted cation (H+ vs Li+). Experimental findings were rationalized by molecular dynamics simulations. The G0 PAMAM head-group could accommodate up to three protons, with protonated terminal amine group enclosed in a pseudo 18-crown-6 ring formed by the PEO segment. This particular conformation enabled a hydrogen bond network which allowed long-range proton transfer to occur during collisionally activated dissociation. In contrast, lithium adduction was found to mainly occur onto oxygen atoms of the polyether, each Li+ cation being coordinated by a 12-crown-4 pseudo structure. As a result, for the studied polymeric segment (M-n = 1500 g mol(-1)), PEO-PAMAM hybrid molecules exhibited a more expanded shape when adducted to lithium as compared to proton. (C) 2013 Elsevier B. V. All rights reserved.

Published

2014

17. Chiroptical properties and conformational flexibility of fenoterol and analogues: a combined experimental and theoretical study

Author

Tedesco, D., Riccardo Zanasi, Wainer, I. W., Bertucci, C., and Daniele Tedesco, Riccardo Zanasi, Irving W. Wainer, Carlo Bertucci

Subjects

Absolute stereochemistry, ECD spectroscopy, TD-DFT calculations, Conformational analysi, Fenoterol

Abstract

Fenoterol is a selective β 2 -adrenergic receptor (AR) agonist used in the treatment of asthma, which is under scrutiny as possible drug against congestive heart failure. Fenoterol is currently used as a racemic mixture of the (R,R′)- and (S,S′)-enantiomers, whose stereochemistry was previously determined by electronic circular dichroism (ECD) analysis through the application of a semi-empirical sector rule. [1] Recently, a series of fenoterol derivatives has been synthesized and tested: [2-3] their absolute configuration was determined by chemical correlation with synthetic precursors, but no further stereochemical characterization has been carried out. In addition, stereoselectivity in the binding to β 2 - AR has been demonstrated, with (R,R′)- and (R,S′)-fenoterol displaying higher affinity compared to (S,R′)- and (S,S′)-fenoterol, and a tridimensional quantitative structure-activity relationship model (3D- QSAR) based on comparative molecular field analysis (CoMFA) has been developed to rationalize the binding of fenoterol derivatives to β 2 -AR. [2-3] The relationship between chiroptical properties and absolute stereochemistry of fenoterol and its derivatives has been investigated [4] by experimental ECD analysis and quantum chemical (QC) calculations using time-dependent density functional theory (TD-DFT). [5-6] The stereoisomers of three compounds have been considered: fenoterol (1), (4′′-methoxy-1′′-naphthyl)fenoterol (2), and (4′′-methoxy- 1′-desmethyl)fenoterol (3). Due to the high conformational flexibility of the investigated structures and the consequent large pool of equilibrium conformers, DFT geometry optimizations were carried out using the resolution of identity (RI) approximation and the B97D functional with empirical dispersion corrections; [7] TD-DFT calculations were then performed using the PBE0 functional. The accuracy of this protocol in reproducing the experimental ECD spectra of fenoterol derivatives will be evaluated. [1] F. Beigi, C. Bertucci, W. Zhu, K. Chakir, I.W. Wainer, R.P. Xiao, D.R. Abernethy, Chirality, 2006, 18, 822-827. [2] K. Jóźwiak, K. Chakir, M.J. Tanga, I. Berzetei-Gurske, L. Jimenez, J.A. Kozocas, A. Woo, W. Zhu, R.P. Xiao, D.R. Abernethy, I.W. Wainer, J. Med. Chem., 2007, 50, 2903-2915. [3] K. Jóźwiak, A.Y.H. Woo, M.J. Tanga, L. Toll, L. Jimenez, J.A. Kozocas, A. Plazinska, R.P. Xiao, I.W. Wainer, Bioorg. Med. Chem., 2010, 18, 728-736. [4] ISCRA project IsC08_SCCFPM (ID: HP10CU0YHL) granted by CINECA, Bologna, Italy. [5] J. Autschbach, Chirality, 2009, 21, E116-E152. [6] L. Goerigk, H. Kruse, S. Grimme, in: N. Berova, P.L. Polavarapu, K. Nakanishi, R.W. Woody (Eds.), Comprehensive chrioptical spectroscopy, vol. 1, 2011, Hoboken: Wiley & Sons, pp. 643-673. [7] S. Grimme, WIREs Comput. Mol. Sci., 2011, 1, 211-228.

Published

2013

18. Conformational changes of small PAMAM dendrimers as a function of their charge state: A combined electrospray mass spectrometry, traveling-wave ion mobility and molecular modeling study

Author

Laetitia Denbigh, Ling Peng, Aura Tintaru, Xiaoxuan Liu, Sabrina Pricl, Laurence Charles, Aura, Tintaru, Pricl, Sabrina, Laetitia, Denbigh, Xiaoxuan, Liu, Ling, Peng, Laurence, Charles, Centre Interdisciplinaire de Nanoscience de Marseille (CINaM), Aix Marseille Université (AMU)-Centre National de la Recherche Scientifique (CNRS), and Cinam, Hal

Subjects

Electrospray, Protonation, 010402 general chemistry, Mass spectrometry, PAMAM dendrimers, 01 natural sciences, Ion, conformational analysis, mass spectrometry, Molecular dynamics simulation, Molecular dynamics, Computational chemistry, Dendrimer, Molecule, Physical and Theoretical Chemistry, Instrumentation, Spectroscopy, Quantitative Biology::Biomolecules, PAMAM dendrimer, 010405 organic chemistry, Chemistry, Condensed Matter Physics, 0104 chemical sciences, Condensed Matter::Soft Condensed Matter, Chemical physics, Mass spectrum, conformational analysi

Abstract

Mass spectrometry was used in conjunction with ion mobility experiments and molecular modeling to study any conformational changes of two PAMAM dendrimers of different structure as a function of their protonation degree. Changes of molecular conformation conjectured from peculiar charge state distribution in the electrospray mass spectra were confirmed by collision cross section values derived from ion mobilograms and supported by theoretical calculations. Shape extension was significant for triply charged molecules of both dendrimers, but the extent of this swelling phenomenon was shown to strongly depend on the PAMAM dendrimers architecture.

Published

2013

19. Structural insights into the interaction between the Cripto CFC domain and the ALK4 receptor

Author

Calvanese, Luisa, Saporito, Angela, Oliva, Romina, D'Auria, Gabriella, Pedone, Carlo, Paolillo, Livio, Ruvo, Menotti, Marasco, Daniela, Falcigno, Lucia, L., Calvanese, A., Saporito, R., Oliva, D'Auria, Gabriella, C., Pedone, L., Paolillo, M., Ruvo, Marasco, Daniela, and Falcigno, Lucia

Subjects

Magnetic Resonance Spectroscopy, Membrane Glycoproteins, EGF-CFC family, Epidermal Growth Factor, homology modeling, Molecular Sequence Data, SPR, GPI-Linked Proteins, Mass Spectrometry, Protein Structure, Secondary, NMR, Neoplasm Proteins, Protein Structure, Tertiary, docking, conformational analysi, Intercellular Signaling Peptides and Proteins, Amino Acid Sequence, Activin Receptors, Type I, Chromatography, High Pressure Liquid, Protein Binding

Abstract

The protein Cripto is the founding member of the extra-cellular EGF-CFC growth factors, which are composed of two adjacent cysteine-rich domains: the EGF-like and the CFC. Members of the EGF-CFC family play key roles in embryonic development and are also implicated in tumourigenesis. Cripto is highly over-expressed in many tumours, while it is poorly detectable in normal tissues. Although both Cripto domains are involved in its tumourigenic activity, the CFC domain appears to play a crucial role. Indeed, through this domain, Cripto interferes with the onco-suppressive activity of Activins, either by blocking the Activin receptor ALK4 or by antagonising proteins of the TGF-beta family. We have undertaken the chemical synthesis and the structural characterisation of human CFC Cripto domain. Using a combined NMR and computational approach, supported by binding studies by SPR, we have investigated the molecular basis of the interaction between h-CFC and ALK4. Binding studies indicate that the synthetic h-CFC interacts with the ALK4 receptor with a K(D) in micro M range, whereas it does not recognise the ActRIIB receptor. The NMR study shows that the h-CFC overall topology is determined by the presence of three disulfide bridges and that residues H120 and W124 are located between the first strand and the first loop with the side chains externally exposed. A model of the CFC-ALK4 complex has also been obtained by molecular docking and shows that all residues indicated by prior mutagenesis studies can contribute to the ALK4-CFC interaction at the protein-protein interface.

Published

2009

20. Asymmetric Biomimetic Oxidations of Phenols: The Mechanism of the Diastereo- and Enantioselective Synthesis of Thomasidioic Acid

Author

Maurizio Bruschi, Luca Zoia, Eeva-Liisa Tolppa, Marco Orlandi, Bruno Rindone, Zoia, L, Bruschi, M, Orlandi, M, Tolppa, E, and Rindone, B

Subjects

lignan, Molecular Conformation, Pharmaceutical Science, enantioselection, Horseradish peroxidase, Benzoates, Diastereoselection, lignans, horseradish peroxidase, oxidative, Article, Analytical Chemistry, Catalysis, lcsh:QD241-441, chemistry.chemical_compound, Hydrolysis, lcsh:Organic chemistry, Phenols, semiempiric calculations, Biomimetics, Drug Discovery, CHIM/06 - CHIMICA ORGANICA, Organic chemistry, Physical and Theoretical Chemistry, Hydrogen peroxide, Furans, biology, Organic Chemistry, Biphenyl Compounds, Enantioselective synthesis, conformational analysis, Stereoisomerism, Enantiopure drug, chemistry, Chemistry (miscellaneous), biology.protein, conformational analysi, Molecular Medicine, Thermodynamics, Oxidative coupling of methane, oxidative phenol coupling, Oxidation-Reduction

Abstract

Enantiopure chiral amidic derivatives of sinapic acid were oxidised with hydrogen peroxide using horseradish peroxidase (HRP) as the catalyst to give the aryltetraline dilignol thomasidioic acid. Trans-diastereoselectivity and enantioselectivity in the formation of thomasidioic acid was observed. Computational methods show that the enantioselectivity is controlled by the beta-beta oxidative coupling step, while the diastereoselectivity is controlled by the stability of the reactive conformation of the intermediate quinomethide.

Published

2008

21. Physicochemical characterization of a peptide deriving from the glycoprotein gp36 of the feline immunodeficiency virus and its lipoylated analogue in micellar systems

Author

Anna Maria D'Ursi, Simone Giannecchini, Paolo Rovero, Mauro Bendinelli, Gerardino D'Errico, Cinzia Esposito, Maria Rosaria Armenante, C., Esposito, D'Errico, Gerardino, M. R., Armenante, S., Giannecchini, M., Bendinelli, P., Rovero, and A. M., D'Ursi

Subjects

Feline immunodeficiency virus, Protein Conformation, Lipoproteins, Phosphorylcholine, Biophysics, Peptide, Immunodeficiency Virus, Feline, Conformational analysi, Antiviral Agents, Biochemistry, Lipopeptide, Diffusion, chemistry.chemical_compound, Viral Envelope Proteins, Nuclear Magnetic Resonance, Biomolecular, Micelles, Glycoproteins, chemistry.chemical_classification, biology, Circular Dichroism, Electron Spin Resonance Spectroscopy, Sodium Dodecyl Sulfate, Cell Biology, biology.organism_classification, In vitro, FIV, Conformational analysis, Spectrometry, Fluorescence, Membrane, chemistry, Viral replication, Cell culture, Micelle interface, Glycoprotein

Abstract

P59 is the Trp-rich 20-mer peptide ( 767 L–G 786 ), partial sequence of the membrane-proximal external region (MPER) of the FIV gp36. It has potent antiviral activity, possibly due to a mechanism that inhibits the fusion of the virus with the cell membranes. In the hypothesis that a lipophilic tail could enhance the adhesion of P59 to the membrane so improving its antiviral activity, we synthesized its lipoylated analogue lipo-P59. Fluorescence, CD and NMR investigations in membrane mimicking environments (such as SDS and DPC micelles) were aimed to assess the potential of the lipo-P59 lipophilic tail to affect the biophysical and conformational behaviour of the peptide. In vitro inhibitory assays using lymphoid cell cultures to check the antiviral activity of peptides were also performed. The data show that the biophysical properties and the conformational preferences of the peptides are not dramatically affected by the hydrophobic tail, suggesting that the lipopeptide is capable of preserving all the biophysical peculiarities. Similarly, antiviral experimental data show that the membrane-anchored lipo-P59 peptide is also effective in inhibiting virus replication. Moreover, the lipophilic tail allows P59 to preserve its antiviral activity even in conditions in which the non lipoylated peptide is devoid of activity. In accordance with the unusual high Trp presence, the peptides confirm the preference to be positioned on the membrane interface. Furthermore, the data point out a peculiarity of interaction of the peptides with SDS as compared with DPC.

Published

2006

22. Assessment of the conformational features of vasoactive intestinal peptide in solution by limited proteolysis experiments

Author

Alessandra Dicitore, Anna Marabotti, Angelo Facchiano, Pasquale Ferranti, Maria Cartenì, Paola Stiuso, Marilena Lepretti, Stiuso, Paola, Marabotti, A., Facchiano, A., Lepretti, M., Dicitore, A., Ferranti, P., Carteni', M., Stiuso, P., Ferranti, Pasquale, and Carten, M.

Subjects

vasoactive intestinal peptide analogue, Protein Conformation, Proteolysis, Molecular Sequence Data, Vasoactive intestinal peptide, Thermolysin, Biophysics, Peptide, Diamines, Biochemistry, Biomaterials, Structure-Activity Relationship, chemistry.chemical_compound, medicine, Trypsin, Amino Acid Sequence, Derivatization, Protein secondary structure, vasoactive intestinal peptide, mass spectrometry, chemistry.chemical_classification, medicine.diagnostic_test, Organic Chemistry, General Medicine, Amino acid, Solutions, limited proteolysi, chemistry, conformational analysi, medicine.drug

Abstract

The structural features of vasoactive intestinal peptide (VIP) and of its Gln16-diaminopropane derivative (VIP-DAP) in solution were investigated by limited proteolysis experiments with trypsin and thermolysin. The proteolysis of the native peptide by both proteinases takes place near the residues in positions 12 and 21/22, suggesting that these amino acids are embedded in segments more flexible than the rest of the molecule. VIP-DAP appears to be more resistant to the proteolytic attack of trypsin, indicating that the derivatization in position 16 is able to stabilize the structure of the peptide. Moreover, the analysis of the mass spectra of the proteolytic mixtures supports the evidence that the derivatization is also able to protect Met17 against oxidation. From these data it can be concluded that VIP in solution under physiological conditions is characterized by the presence of segments with secondary structure, linked together by “hinge” regions that confer flexibility to the peptide, whereas VIP-DAP is embedded in a more rigid conformation, more suitable to receptor interaction. © 2005 Wiley Periodicals, Inc. Biopolymers 81: 110–119, 2006 This article was originally published online as an accepted preprint. The “Published Online” date corresponds to the preprint version. You can request a copy of the preprint by emailing the Biopolymers editorial office at biopolymers@wiley.com

Published

2006

23. Solvent effects on the conformational distribution and optical rotation of g-methyl paraconic acids and esters

Author

Domenico Marchesan, Giuliana Pitacco, Antonio Rizzo, Patrizia Nitti, Cristina Forzato, Lara Ferrighi, Kenneth Ruud, Angelika Baranowska, Sonia Coriani, Coriani, Sonia, A., Baranowska, L., Ferrighi, Forzato, Cristina, Marchesan, Domenico, Nitti, Patrizia, Pitacco, Giuliana, A., Rizzo, and K., Ruud

Subjects

solvent effects, rotatory power, paraconic acids, Computational spectroscopy, conformational analysis, Polarizable continuum model, Catalysis, paraconic acid, Analytical Chemistry, chemistry.chemical_compound, Computational chemistry, Polarizability, Drug Discovery, Molecule, Optical rotation, Conformational isomerism, Spectroscopy, Pharmacology, solvent effect, Organic Chemistry, chemistry, conformational analysi, Methanol, Solvent effects, Cis–trans isomerism

Abstract

A computational investigation of the optical rotatory power of cis and trans 2-methyl-5-oxo-tetrahydro-3-furancarboxylic acids and the corresponding methyl and ethyl esters is presented. Solvent effects on both the conformational space and the rotatory power are analyzed by comparing results obtained in vacuo with those computed—using the Polarizable Continuum Model—in methanol. A comparison with experimental observations for the optical rotatory power of the title compounds in methanol is also carried out, in a few cases also for several wavelengths. Agreement between theory and experiment is in all cases excellent, in particular when solvent effects are included both in the geometry optimization and in the calculation of the OR, thus confirming the validity of the computational procedure adopted, even for this challenging family of floppy molecules. Chirality, 2006. © 2006 Wiley-Liss, Inc.

Published

2006

24. Optical rotation calculation of a highly flexible molecule: the case of paraconic acid

Author

Domenico Marchesan, Sonia Coriani, Patrizia Nitti, Giuliana Pitacco, Kenneth Ruud, Cristina Forzato, Marchesan, Domenico, Coriani, Sonia, Forzato, Cristina, Nitti, Patrizia, Pitacco, Giuliana, and K., Ruud

Subjects

Computational spectroscopy, conformational analysis, absolute configuration, Density functional theory, MP2 theory, Paraconic acid, Chemistry, Absolute configuration, Crystallography, Ab initio quantum chemistry methods, conformational analysi, Molecule, Physical and Theoretical Chemistry, Optical rotation, Line (formation)

Abstract

The absolute configuration of (S)-(-)-paraconic acid is correctly assigned on the basis of ab initio calculations of the specific optical rotation (OR) at the sodium D line, carried out both in vacuum and in methanol. Density functional theory (DFT) and Møller-Plesset second-order perturbation theory (MP2) are used to determine the most stable conformational structures, whose OR values are then calculated using DFT linear response theory and London atomic orbitals. The total OR is obtained by averaging these values using the population fractions determined from Boltzmann's statistics. The total OR of the MP2 structures has the correct sign both in vacuum and in solution, whereas only the solvent-relaxed DFT structures correctly reproduce the experimental sign. The strong solvent effect on the total OR is shown to arise primarily due to the variations in the relative energies of the various conformations.

Published

2005

25. Asymmetric biomimetic oxidations of phenols: The mechanism of the diastereo- and enantioselective synthesis of thomasidioic acid

Author

Zoia, L, Bruschi, M, Orlandi, M, Tolppa, E, Rindone, B, ZOIA, LUCA, BRUSCHI, MAURIZIO, ORLANDI, MARCO EMILIO, TOLPPA, EEVA-LIISA, RINDONE, BRUNO, Zoia, L, Bruschi, M, Orlandi, M, Tolppa, E, Rindone, B, ZOIA, LUCA, BRUSCHI, MAURIZIO, ORLANDI, MARCO EMILIO, TOLPPA, EEVA-LIISA, and RINDONE, BRUNO

Abstract

Enantiopure chiral amidic derivatives of sinapic acid were oxidised with hydrogen peroxide using horseradish peroxidase (HRP) as the catalyst to give the aryltetraline dilignol thomasidioic acid. Trans-diastereoselectivity and enantioselectivity in the formation of thomasidioic acid was observed. Computational methods show that the enantioselectivity is controlled by the beta-beta oxidative coupling step, while the diastereoselectivity is controlled by the stability of the reactive conformation of the intermediate quinomethide.

Published

2008

26. Conformational analysis of HAMLET, the folding variant of human α-lactalbumin associated with apoptosis

Author

Fabrizio Dal Piaz, Piero Pucci, Catharina Svanborg, Leila Birolo, Annarita Casbarra, Giuseppe Infusini, Malin Svensson, Gennaro Marino, A., Casbarra, Birolo, Leila, G., Infusini, F., DAL PIAZ, M., Svensson, Pucci, Pietro, C., Svanborg, and Marino, Gennaro

Subjects

H/D exchange, Proteases, Protein Folding, Proteolysis, Molecular Sequence Data, Apoptosis, Biochemistry, Peptide Mapping, Article, Protein Structure, Secondary, chemistry.chemical_compound, alpha-lactalbumin, medicine, Humans, Amino Acid Sequence, Binding site, Molecular Biology, Lactalbumin, biology, medicine.diagnostic_test, Chemistry, Folding (chemistry), Kinetics, conformational analysi, Biophysics, Alpha-lactalbumin, biology.protein, Protein folding, HAMLET (protein complex), Protons, HAMLET, limited proteolysis

Abstract

A combination of hydrogen/deuterium (H/D) exchange and limited proteolysis experiments coupled to mass spectrometry analysis was used to depict the conformation in solution of HAMLET, the folding variant of human alpha-lactalbumin, complexed to oleic acid, that induces apoptosis in tumor and immature cells. Although near- and far-UV CD and fluorescence spectroscopy were not able to discriminate between HAMLET and apo-alpha-lactalbumin, H/D exchange experiments clearly showed that they correspond to two distinct conformational states, with HAMLET incorporating a greater number of deuterium atoms than the apo and holo forms. Complementary proteolysis experiments revealed that HAMLET and apo are both accessible to proteases in the beta-domain but showed substantial differences in accessibility to proteases at specific sites. The overall results indicated that the conformational changes associated with the release of Ca2+ are not sufficient to induce the HAMLET conformation. Metal depletion might represent the first event to produce a partial unfolding in the beta-domain of alpha-lactalbumin, but some more unfolding is needed to generate the active conformation HAMLET, very likely allowing the protein to bind the C18:1 fatty acid moiety. On the basis of these data, a putative binding site of the oleic acid, which stabilizes the HAMLET conformation, is proposed.

Published

2004

27. Synthesis and conformational analysis of novel N(OCH3)-linked disaccharide analogues

Author

Jesús Jiménez Barbero, Igor Tvaroška, Víctor García–Aparicio, Francesco Peri, Francesco Nicotra, Peri, F, Jiménez Barbero, J, García Aparicio, V, Tvaroska, I, and Nicotra, F

Subjects

Carbohydrate, Glycosylation, Stereochemistry, Molecular Sequence Data, Ab initio, Disaccharide, Conformational analysi, Disaccharides, Catalysis, Coupling reaction, chemistry.chemical_compound, NMR spectroscopy, CHIM/06 - CHIMICA ORGANICA, Carbohydrate Conformation, Monosaccharide, Computer Simulation, Conformational isomerism, chemistry.chemical_classification, Chemistry, Organic Chemistry, Monosaccharides, General Chemistry, Nuclear magnetic resonance spectroscopy, Oligosaccharide, Oxime, Carbohydrate Sequence, Trisaccharides

Abstract

N(OMe)-linked disaccharide analogues, isosteric to the corresponding natural disaccharides, have been synthesized by chemoselective assembly of unprotected natural monosaccharides with methyl 6-deoxy-6-methoxyamino-alpha-D-glucopyranoside in an aqueous environment. The coupling reactions were found to be chemo- and stereoselective affording beta-(1-->6) disaccharide mimics when using Glc and GlcNAc; in the case of Gal, the beta-anomer was prevalent (beta:alpha=7:1). An iterative method for the synthesis of linear N(OMe) oligosaccharide analogues was demonstrated, based on the use of an unprotected monosaccharide building block in which an oxime functionality at C-6 is converted during the synthesis into the corresponding methoxyamino group. The conformational analysis of these compounds was carried out by using NMR spectroscopy, ab initio, molecular mechanics, and molecular dynamics methods. Optimized geometries and energies of fourteen conformers for each compound have been calculated at the B3LYP/6-31G* level. Predicted conformational equilibria were compared with the results based on NMR experiments and good agreement was found. It appears that N(OMe)-linked disaccharide analogues exhibit a slightly different conformational behavior to their parent natural disaccharides.

Published

2004

28. Chain Conformations in the Crystalline Field of Syndiotactic Vinyl Polymers Deriving from 1,3-Diene Monomers. Analysis by Molecular Mechanics

Author

Roberto Napolitano, B. Pirozzi, Simona Esposito, Pirozzi, Beniamino, Napolitano, Roberto, and S., Esposito

Subjects

chemistry.chemical_classification, Quantitative Biology::Biomolecules, Polymers and Plastics, Diene, Organic Chemistry, Torsion (mechanics), Polymer, Condensed Matter Physics, Molecular mechanics, line repetition group, Vinyl polymer, Condensed Matter::Soft Condensed Matter, Inorganic Chemistry, Maxima and minima, chemistry.chemical_compound, Crystallography, Monomer, chemistry, molecular mechanic, Tacticity, Polymer chemistry, Materials Chemistry, conformational analysi, potential functions

Abstract

Conformational energy calculations on the chain conformation in the crystalline field have been performed for various syndiotactic vinyl polymers deriving from 1,3-diene monomers. Energy maps as a function of the independent torsion angles have evidenced for all the polymers minima corresponding to highly extended and to helical chains. Energy minimizations as a function of all the internal parameters for the s(2/1)2 and tcm symmetries have allowed the evaluation of the energy differences between chains having the two symmetries and the prediction of the values of the conformational parameters for each polymer. The results have been compared with the experimental data reported in the literature for some of the studied polymers.

Published

2004

29. Asymmetric biomimetic oxidations of phenols using oxazolidines as chiral auxiliaries: The enantioselective synthesis of (+)- and (-)-dehydrodiconiferyl alcohol

Author

Bruschi, M, Orlandi, M, Rindone, B, Rummakko, P, Zoia, L, BRUSCHI, MAURIZIO, ORLANDI, MARCO EMILIO, RINDONE, BRUNO, ZOIA, LUCA, Bruschi, M, Orlandi, M, Rindone, B, Rummakko, P, Zoia, L, BRUSCHI, MAURIZIO, ORLANDI, MARCO EMILIO, RINDONE, BRUNO, and ZOIA, LUCA

Abstract

Stereoselective bimolecular radical coupling reactions of phenylpropenoid phenols are described. Evans's 2-oxazolidinone 11a-d derivatives of ferulic acid were prepared and oxidized to give dimeric benzofuran neolignan structures 12-13a-d in 40-50% overall yields. The chiral phenols were dimerized either enzymatically with hydrogen peroxide and horseradish peroxidase (HRP) or with silver oxide. The enantioselectivity after reductive cleavage of the chiral auxiliaries to give dehydrodiconiferyl alcohol ranged from 18% to 62% enantiomeric excess. The conformational analysis and the activation energy using semiempirical PM3 calculations on the intermediate quinomethides is used to explain the observed stereoselectivity. Copyright (c) 2006 John Wiley & Sons, Ltd

Published

2006

30. Tetracycline and its analogues as inhibitors of amyloid fibrils: Searching for a geometrical pharmacophore by theoretical investigation of their conformational behavior in aqueous solution

Author

Cosentino, U, Vari', M, Saracino, G, Pitea, D, Moro, G, Salmona, M, COSENTINO, UGO RENATO, Vari', MR, Saracino, GAA, PITEA, DEMETRIO, MORO, GIORGIO, Salmona, M., Cosentino, U, Vari', M, Saracino, G, Pitea, D, Moro, G, Salmona, M, COSENTINO, UGO RENATO, Vari', MR, Saracino, GAA, PITEA, DEMETRIO, MORO, GIORGIO, and Salmona, M.

Abstract

Tetracycline (TC) and its derivatives have recently been proposed as a new class of antagonists in prion diseases as they prevent the aggregation of prion protein peptides and their acquisition of protease resistance in vitro and in vivo. Looking for relationships between conformational flexibility and biological activity, we searched for a geometrical pharmacophore by investigating, in aqueous solution, the conformational behavior of 15 TCs in both the zwitterionic and the anionic forms. For TC similar conformational flexibility was found for the two forms and two main conformational families were detected, an extended and a folded conformation characterized by different intramolecular hydrogen-bond networks. On comparing the Molecular Mechanics results with the ab initio ones and the experimental evidence, it can be seen that the conformational behavior of TC is reasonably well predicted by the MM2 force field, whereas the conformational energies provided by the Amber force field are unreliable. The conformational analysis of the other TC derivatives was then performed by the MM2 force field. As a result, their conformational behavior was similar to that observed for TC itself. Despite the hydronaphthacene moiety's conformational flexibility, no geometrical pharmacophore was found among the TCs, i.e. properties other than geometrical ones should play a crucial role in determining their anti-fibrillogenic ability.

Published

2005

31. X-ray structures of new dipeptide taste ligands

Author

MURRAY GOODMAN, RALPH HEIKO MATTERN, PETER GANTZEL ANTONELLO SANTINI, MICHELE SAVIANO AND ETTORE BENEDETTI, IACOVINO, Rosa, Murray, Goodman, RALPH HEIKO, Mattern, PETER GANTZEL ANTONELLO, Santini, Iacovino, Rosa, and MICHELE SAVIANO AND ETTORE, Benedetti

Subjects

Artificial sweetener, Peptide-based taste ligand, Conformational analysi, X-ray crystal structure

Abstract

The molecular basis of sweet taste was investigated by carrying out the crystal state conformational analysis by X-ray diffraction of the following dipeptide taste ligands: N-3,3-dimethylbutyl-aspartyl-phenylalanine methyl ester, I (N-DMB-Asp-Phe-OMe), its sodium salt (N-DMB-Asp-Phe-ONa). II. aspartyl-D-2-aminobutyric acid-(S)-α-ethylbenzylamide, III (Asp-D-Abu-(S)-α-ethylbenzylamide), aspartyl-N-((2,2,5,5-tetramethylcyclopentanyl)-carbonyl)-(R)-1, 1-diamino-ethane. IV (Asp-(R)-gAla-TMCP), and aspartyl-D-valine-(R)-α-methoxymethylbenzyl amide, V (Asp-D-Val-(R)-α-methoxymethylbenzylamide). With the exception of the sodium salt II, all compounds are sweet-tasting, showing in some cases considerable potency enhancement with respect to sucrose. The results of this study confirm the earlier model that an 'L-shape' molecular array is essential for eliciting sweet taste for dipeptide-like ligands. In addition, it was established that (i) substitution of the N-terminal group does not inhibit sweet taste, if its zwitterionic character is maintained; (ii) a hydrophobic group located between the stem and the base of the L-shape could be responsible for sweetness potency enhancement, as found in I, III and IV; in fact, the extraordinary potency of the N-alkylated analogue I would support a model with an additional hydrophobic binding domain above the base of the 'L'; (iii) removal of the methyl ester at the C-terminus of compound I with the salt formation gives rise to the tasteless compound II; (iv) for the first time all possible side-chain conformers (g-, g+ and t) for the N-substituted aspartyl residue were observed; and (v) a retro-inverso modification, incorporated at position 2 of the dipeptide chain, confers greater flexibility to the molecule, as demonstrated by the contemporary presence of six conformationally distinct independent molecules in the unit cell and yet sweet taste properties are maintained, as found in IV. © 1998 European Peptide Society and John Wiley & Sons, Ltd.

Published

1998

32. Conformational analysis of the dipeptide taste ligand L-aspartyl-D-2-aminobutyric acid-(S)-α-ethylbenzylamide and its analogues by NMR spectroscopy, computer simulations and X-ray diffraction studies

Author

Goodman, M., Zhu, Q., Kent, D. R., Amino, Y., Benedetti, E., Santini, A., IACOVINO, Rosa, Goodman, M., Zhu, Q., Kent, D. R., Amino, Y., Iacovino, Rosa, Benedetti, E., and Santini, A.

Subjects

NMR spectroscopy, Artificial sweetener, Peptide-based taste ligand, Computer simulation, Conformational analysi, X-ray diffraction

Abstract

A dipeptide taste ligand L-aspartyl-D-2-aminobutyric acid-(S)-α-ethylbenzylamide was found to be about 2000 times more potent than sucrose. To Investigate the molecular basis of its potent sweet taste, we carried out conformational analysis of this molecule and several related analogues by NMR spectroscopy, computer simulations and X-ray crystallographic studies. The results of the studies support our earlier model that an L-shape molecular array is essential for eliciting sweet taste. In addition, we have identified an aromatic group located between the stem and the base of the L-shape, which is responsible for enhancement of sweetness potency. In this study, we also assessed the optimal size of the essential hydrophobic group (X) and the effects of the chirality of the second residue toward taste. ©1997 European Peptide Society and John Wiley & Sons, Ltd.

Published

1997

33. Preferred conformation of peptides rich in alicyclic C-alpha,C-alpha-disubstituted glycines

Author

Toniolo, C, Crisma, M, Formaggio, F, Benedetti, E, Santini, A, Saviano, M, DiBlasio, B, Pedone, C, Kamphuis, J., IACOVINO, Rosa, Toniolo, C, Crisma, M, Formaggio, F, Benedetti, E, Santini, A, Iacovino, Rosa, Saviano, M, Diblasio, B, Pedone, C, and Kamphuis, J.

Subjects

Of peptide, disubstituted glycine, helical conformation, Conformational analysi, Ofpeptide, fourier transform ir absorption, Peptides rich in

Abstract

The conformational preferences of the alicyclic Cαα-disubstituted glycines Acnc (1-amino-1-cycloalkane-carboxylic acid; n = 4,7, 9, 12) were assessed in selected model compounds, including homopeptides and Ala (orAib, α-aminoisobutyric acid )/Acnc peptides containing a small total number of residues, by Fourier transform ir absorption,1H-nmr, and x-ray diffraction analyses. The results obtained indicate that β-turn and 310-helical structures are preferentially adopted by short peptides rich in these cycloaliphatic α-amino acids. © 1997 John Wiley & Sons, Inc.

Published

1996

34. Conformational analysis of DNA-basic polypeptide complexes: possible models of nucleoprotamines and nucleohistones

Author

E. Forni, Roberto Rizzo, P. De Santis, De Santis, P., Forni, E., and Rizzo, Roberto

Subjects

peptide-DNA complexes, Molecular model, Chemical Phenomena, Stereochemistry, CONFORMATIONAL ANALYSIS, Biophysics, Molecular Conformation, Biochemistry, Biomaterials, Hydrophobic effect, Histones, symbols.namesake, chemistry.chemical_compound, peptide-DNA complexe, Protamines, biology, Base Sequence, Hydrogen bond, Chemistry, Organic Chemistry, DNA-basic polypeptide complexes, General Medicine, DNA, nucleo-histone models, molecular modelling, Crystallography, conformational analysis, Histone, Nucleoproteins, Models, Chemical, Helix, conformational analysi, biology.protein, symbols, DNA supercoil, van der Waals force, Peptides

Abstract

Conformational analysis of DNA–basic polypeptide complexes, based on stereo-chemical criteria and energy calculations and experimental results, is reported. Three types of polypeptide conformations were selected: the distorted β conformation similar to that proposed by Feughelmann et al.; a structure characterized by a repetition of a right-handed and left-handed α helix-type conformation; and an intermediate structure. A model of the complex between DNA and basic polypeptides was proposed, where the polypeptide chain fits the narrow groove of the B form of DNA. Van der Waals, hydrogen bond, electrostatic, and hydrophobic forces cooperate to stabilize the association complex. This structure also seems to be suitable to represent the molecular model of nucleoprotamines. In the case of nucleohistones, both grooves of DNA are involved in the interaction with the proteins. These have the nonbasic-rich portion in the α-helical conformation, whereas the part where a greater proportion of basic amino acids occurs presents a structure similar to nucleoprotamines and complexes between DNA and basic homopolypeptides. The distribution of basic residues of the F2A1(IV) histone on DNA is markedly disproportionate for the two opposite cylindrical sectors of the double helix. This suggests a new mechanism of supercoiling in nucleo-histones.

Published

1974

35. Conformational analysis of DNA-polypeptide systems

Author

Dentini, M., De Santis, P., Morosetti, S., Rizzo, Roberto, Dentini, M., De Santis, P., Morosetti, S., and Rizzo, Roberto

Subjects

DNA-peptide complexe, molecular modeling, DNA-peptide complexes, conformational analysis, conformational analysi

Published

1972