ALBERT — All Library Books, journals and Electronic Records Telegrafenberg

1

Electronic Resource

BUNDLE: A program for building the transmembrane domains of G-protein-coupled receptors (1998)

Filizola, Marta ; Perez, Juan J. ; Cartenì-Farina, Maria

Springer

Journal of computer aided molecular design 12 (1998), S. 111-118

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ISSN: 1573-4951

Keywords: GPCR ; novo modeling ; rhodopsin ; transmembrane domains ; receptors

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract The only information available at present about the structural features of G-protein-coupled receptors (GPCRs) comes from low resolution electron density maps of rhodopsin obtained from electron microscopy studies on 2D crystals. Despite their low resolution, maps can be used to extract information about transmembrane helix relative positions and their tilt. This information, together with a reliable algorithm to assess the residues involved in each of the membrane spanning regions, can be used to construct a 3D model of the transmembrane domains of rhodopsin at atomic resolution. In the present work, we describe an automated procedure applicable to generate such a model and, in general, to construct a 3D model of any given GPCR with the only assumption that it adopts the same helix arrangement as in rhodopsin. The present approach avoids uncertainties associated with other procedures available for constructing models of GPCRs based on a template, since sequence identity among GPCRs of different families in most of the cases is not significant. The steps involved in the construction of the model are: (i) locate the centers of the helices according to the low-resolution electron density map; (ii) compute the tilt of each helix based on the elliptical shape observed by each helix in the map; (iii) define a local coordinate system for each of the helices; (iv) bring them together in an antiparallel orientation; (v) rotate each helix through the helical axis in such a way that its hydrophobic moment points in the same direction of the bisector formed between three consecutive helices in the bundle; (vi) rotate each helix through an axis perpendicular to the helical one to assign a proper tilt; and (vii) translate each helix to its center deduced from the projection map.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1007969112988

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2

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A proposed bioactive conformation of Peptide T (1998)

Centeno, Nuria B. ; Perez, Juan J.

Springer

Journal of computer aided molecular design 12 (1998), S. 7-14

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ISSN: 1573-4951

Keywords: bioactive conformation ; conformational analysis ; Peptide T ; Peptide T analogs

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract The conformational profiles of Peptide T, (5–8)Peptide T, [Abu5](4–8)Peptide T and (4–8)Peptide T were computed independently to assess the geometrical characteristics of the bioactive conformation of Peptide T. The conformational profiles of the peptides were computed within the molecular mechanics framework using an effective dielectric constant of 80. The conformational space was thoroughly sampled using an iterative simulated annealing protocol. The bioactive conformation was assessed by pairwise cross comparisons of each of the unique low energy conformations found for each of the different analogs studied. After a putative bioactive conformation was selected, in order to further validate our hypothesis the conformational profile of the potent compound cyclo(Thr-Thr-Asn-Tyr-Thr-Asp) was computed and the putative bioactive conformation was found. The conformation exhibits a pseudo β-turn involving the side chain of Thr5 and the carbonyl oxygen of Tyr7 forming a C12 ring.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1007994502997

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3

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Molecular modeling study of the differential ligand–receptor interaction at the μ, δ and κ opioid receptors (1999)

Filizola, Marta ; Carteni-Farina, Maria ; Perez, Juan J.

Springer

Journal of computer aided molecular design 13 (1999), S. 397-407

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ISSN: 1573-4951

Keywords: GPCR modeling ; ligand docking ; ligand–receptor interactions ; opioid antagonists ; opioid receptors

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract 3D models of the opioid receptors μ, δ and κ were constructed using BUNDLE, an in-house program to build de novo models of G-protein coupled receptors at the atomic level. Once the three opioid receptors were constructed and before any energy refinement, models were assessed for their compatibility with the results available from point-site mutations carried out on these receptors. In a subsequent step, three selective antagonists to each of three receptors (naltrindole, naltrexone and nor-binaltorphamine) were docked onto each of the three receptors and subsequently energy minimized. The nine resulting complexes were checked for their ability to explain known results of structure-activity studies. Once the models were validated, analysis of the distances between different residues of the receptors and the ligands were computed. This analysis permitted us to identify key residues tentatively involved in direct interaction with the ligand.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008079823736

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4

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A general procedure for building the transmembrane domains of G‐protein coupled receptors (1998)

Perez, Juan J. ; Filizola, Marta ; Caritenì‐Farina, Maria

Springer

Journal of mathematical chemistry 23 (1998), S. 229-238

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ISSN: 1572-8897

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology , Mathematics

Notes: Abstract The only results available at present about the structural features of G‐protein coupled receptors are the low resolution electron projection maps obtained from microscopy studies carried out on two‐dimensional crystals of rhodopsin. These studies support previous suggestions that these integral proteins are constituted by seven transmembrane domains. The low resolution electron density map of rhodopsin can be used to extract information about helix relative positions and tilt. This information, together with a reliable procedure to assess the residues involved in each of the transmembrane regions, can be used to construct a model of rhodopsin at atomic resolution. We have developed an algorithm that can be used to generate such a model in a completely automated fashion. The steps involved are: (i) locate the centers of the helices according to the low resolution electron density map; (ii) compute the tilt of each helix based on the elliptical shape observed by each helix in the map; (iii) define a local coordinate system for each of the helices; (iv) bring them together in an antiparallel orientation; (v) rotate each helix through the helical axis in such a way that its hydrophobic moment points in the same direction as the bisector formed between three consecutive helices in the bundle; (vi) rotate each helix through an axis perpendicular to the helical one to assign a proper tilt; (vii) translate each of the helix to its center deduced from the projection map. A major advantage of the procedure presented is its generality and consequently can be used to obtain a model of any G‐protein coupled receptor with the only assumption that the shape of the bundle is the same as found in rhodopsin. This avoids uncertainties found in other procedures that construct models of G‐protein coupled receptors based on sequence homology using rhodopsin as template.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1019169124352

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5

Electronic Resource

Characterization of the bioactive form of linear peptide antagonists at the δ-opioid receptor (1996)

Chao, Tain-Ming ; Perez, Juan J. ; Loew, Gilda H.

New York : Wiley-Blackwell

Biopolymers 38 (1996), S. 759-768

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ISSN: 0006-3525

Keywords: Chemistry ; Polymer and Materials Science

Source: Wiley InterScience Backfile Collection 1832-2000

Topics: Chemistry and Pharmacology

Notes: The stereochemical requirements for δ-opioid receptor binding of a series of linear peptide antagonists with a novel conformationally restricted Phe analogue (Tic) as a second residue were examined by using a variety of computational chemistry methods. The δ-opioid receptor analogues with significant affinity, Tyr-Tic-NH2 (TI-NH2), Tyr-Tic-Phe-OH (TIP), Tyr-Tic-Phe-NH2(TIP-NH2), Tyr-Tic-Phe-Phe-OH (TIPP), Tyr-Tic-Phe-Phe-NH2) (TIPP-NH2), and the low affinity δ-opioid peptides Tyr-Pro-Phe-Pro-NH2 (morphiceptin) and Tyr-Phe-Phe-Phe-NH2 (TPPP-NH2), were included in this study. The conformational profiles of these peptides were obtained by consecutive cycles of high and low temperature molecular dynamic simulations, coupled to molecular mechanical energy minimization carried out until no new conformational minima were obtained. Comparing the results for TPPP-NH2 and TIPP-NH2, the presence of the conformationally restricted Tic residue did not greatly reduce the number of unique low energy conformations, but did allow low energy conformers involving cis bonds between the first two residues. The conformational libraries of these peptides were examined for their ability to satisfy the three key ligand components for receptor recognition already identified by previous studies of high affinity cyclic (Tyr1-D-Pen2-Gly3-Phe4-D -Pen5) enkephalin (DPDPE) type agonists: a protonated amine group, an aromatic ring, and a lipophilic moiety in a specific geometric arrangement. Two types of conformations common to the five high δ-opioid affinity L-Tic analogues were found that satisfied these requirements, one with a cis and the other with a trans peptide bond between the Tyr1 and Tic2 residues. Moreover, both the Tic2 and Phe3 residues could mimic the hydrophobic interactions with the receptor of the Phe4 moiety in the cyclic DPDPE type agonists, consistent with the appreciable affinity of both di-and tripeptides. The low δ-opioid receptor affinity of morphiceptin can be understood as the result of conformational preferences that prevent the fulfillment of this pharmacophore for recognition. © 1996 John Wiley & Sons, Inc.

Additional Material: 5 Ill.

Type of Medium: Electronic Resource

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6

Electronic Resource

Conformational behavior of the HAV-VP3(110-121) peptidic sequence and synthetic analogs in membrane environments studied by CD and computational methods (1998)

Pérez, José A. ; Cantó, Josep ; Reig, Francisca ; [et al.]

New York : Wiley-Blackwell

Biopolymers 45 (1998), S. 479-492

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ISSN: 0006-3525

Keywords: hepatitis A ; synthetic peptides ; CD ; liposomes ; computational study ; Chemistry ; Polymer and Materials Science

Source: Wiley InterScience Backfile Collection 1832-2000

Topics: Chemistry and Pharmacology

Notes: The present study was undertaken to examine the structural features that may be important to explain the immunogenicity of the (110-121) peptide sequence (FWRGDLVFDFQV) of VP3 capsid protein of hepatitis A virus. A conformational analysis of the preferred conformations by CD and molecular mechanics was carried out. Present results suggest that the interaction with liposomes as biomembrane model induces and stabilizes the amphipathic β-structure of the peptide.To study the contribution of amino acid replacements at the RGD tripeptide as well as the influence of the peptide chain length on peptide conformation, solid-phase peptide synthesis of several peptide analogs was carried out and the peptide conformation was studied using CD spectroscopy. The results show that the RGD sequence is necessary to induce the β-structure in the presence of liposomes. © 1998 John Wiley & Sons, Inc. Biopoly 45: 479-492, 1998

Additional Material: 9 Ill.

Type of Medium: Electronic Resource

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7

Electronic Resource

An easy NMR method to study the formation of parallel β-sheets in peptide aggregates (1999)

Millet, Oscar ; Pérez, Juan J. ; Pons, Miquel

Springer

International journal of peptide research and therapeutics 6 (1999), S. 247-253

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ISSN: 1573-3904

Keywords: aggregation ; assignment ; peptide T ; β-sheet ; symmetry ; transferred NOE

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract There is currently great interest in the study of peptide aggregation by β-sheet formation because of its relevance in pathological states or in the design of self-assembling systems of technological interest. NMR studies of β-sheet aggregates are difficult because of their long correlation times and spectral degeneracy. In this communication we demonstrate the combination of a semiselective TOCSY-NOESY experiment with partial deuterium exchange of labile protons to assign inter-molecular NOE cross peaks and prove the presence of a soluble parallel β-sheet in fast exchange with monomeric Ac-ASTTTNYT-NH2 (Ac-T-NH2) in solution.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008968104503

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8

Electronic Resource

An easy NMR method to study the formation of parallel β-sheets in peptide aggregates (1999)

Millet, Oscar ; Pérez, Juan J. ; Pons, Miquel

Springer

International journal of peptide research and therapeutics 6 (1999), S. 247-253

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ISSN: 1573-3904

Keywords: aggregation ; assignment ; peptide T ; β-sheet ; symmetry ; transferred NOE

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Summary There is currently great interest in the study of peptide aggregation by β-sheet formation because of its relevance in pathological states or in the design of self-assembling systems of technological interest. NMR studies of β-sheet aggregates are difficult because of their long correlation times and spectral degeneracy. In this communication we demonstrate the combination of a semiselective TOCSY-NOESY experiment with partial deuterium exchange of labile protons to assign inter-molecular NOE cross peaks and prove the presence of a soluble parallel β-sheet in fast exchange with monomeric Ac-ASTTNYT-NH2 (Ac-T-NH2) in solution.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF02443513

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9

Electronic Resource

Conformational study of the preferred conformations of the peptide sequence VP3(110–121) of HAV by circular dichroism and molecular mechanics (1997)

Canto, Josep ; Perez, Jose A. ; Centeno, Nuria B. ; [et al.]

Springer

International journal of peptide research and therapeutics 4 (1997), S. 13-19

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ISSN: 1573-3904

Keywords: Hepatitis A ; Circular dichroism ; Conformational analysis ; Molecular mechanics ; Liposomes

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Summary A conformational analysis of the fragment 110–121 of VP3 coating protein of the hepatitis A virus was carried out using circular dichroism spectroscopy and computational studies. The latter studies indicate the tendency of the peptide to adopt hairpin-type structures. Circular dichroism experiments indicate that, in spite of the fact that the isolated peptide exhibits no structure under different experimental conditions, negatively charged liposomes induce a secondary structure that agrees with the results of the computational study.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF02443550

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10

Electronic Resource

A proposed bioactive form of peptide T and the design of peptidomimetics (1998)

Llorens, Oriol ; Centeno, Nuria B. ; Filizola, Marta ; [et al.]

Springer

International journal of peptide research and therapeutics 5 (1998), S. 179-182

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ISSN: 1573-3904

Keywords: data base search ; drug discovery ; peptide T ; peptidomimetics

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract Peptide T is a non-natural octapeptide of sequence Ala-Ser-Thr-Thr-Thr-Asn-Tyr-Thr, taken from the sequence of the protein gp120 of HIV. The peptide has been shown to bind competitively to the CD4 receptors of the helper/inducer lymphocytes T. The peptide is presently used for the treatment of AIDS-associated dementia and has been proven useful for the treatment of psoriasis. Using molecular modeling procedures, we studied the conformational profile of this peptide as well as those of several active and inactive analogs. The analysis of these results gave rise to the proposal of a bioactive conformation of the peptide, which can be described as a pseudo β-turn structure, involving the last four residues at the C-terminus of the peptide. The secondary structure is stabilized by a hydrogen bond between the hydroxyl hydrogen of the side chain of Thr5 and the carbonyl oxygen of Tyr7. From the bioactive form and different structure–activity relationship studies, a pharmacophore was proposed. This hypothesis was used to search on several 3D data bases. One of the hits obtained was the natural compound amigdalin, which was tested and exhibited moderate activity.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1008843818049

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