Conformations of Arg-Gly-Asp containing heterodetic cyclic peptides: solution and crystal studies

Kopple, Kenneth D.; Baures, Paul W.; Bean, James C.; D'Ambrosio, Cynthia A.; Hughes, John L.; Peishoff, Catherine E.; Eggleston, Drake S.

doi:10.1021/ja00050a049

Cited by 88 publications

(53 citation statements)

References 6 publications

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“…This finding is not in agreement with a recently published comparative study of a series of homo-and heterodetic cyclic Arg-Gly-Asp peptides, refined by means of NMR spectroscopy and X-ray crystallography [63,67,68]. In this investigation the authors defined four structurally distinct categories, according to the conformational preference of the recognition tripeptide backbone.…”

Section: Significance Of the Residue Following The Rgd Tripeptidecontrasting

confidence: 61%

Pharmacophore refinement of gpIIb/IIIa antagonists based on comparative studies of antiadhesive cyclic and acyclic RGD peptides

Müller

Gurrath

Kessler

1994

J Computer-Aided Mol Des

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Structurally guided design approaches to low-molecular-weight platelet aggregation antagonists addressing the platelet-associated heterodimeric cell surface receptor gpIIb/IIIa rely on comparative studies of an ensemble of conformationally and biologically characterized compounds, since no high-resolution structure of the receptor system is available. We report a classical indirect and comparative pharmacophore refinement approach based on a series of small cyclic Arg-Gly-Asp (RGD) peptides as gpIIb/IIIa-fibrinogen interaction antagonists. These peptides have previously been investigated as potent and selective tumor cell adhesion inhibitors. The definition of geometrical descriptors classifying the RGD peptide conformations and their subsequent analysis over selected RGD- and RXD-containing protein structures allows for a correlation of distinct structural features for platelet aggregation inhibition. An almost parallel alignment of the Arg and Asp side chains was identified by a vector analysis as being present in all active cyclic hexa- and pentapeptides. This orientation is induced mainly by the constraint of backbone cyclization and is not of any covalent tripeptide-inherent origin, which was rationalized by a 500 ps high-energy MD simulation of a sequentially related linear model peptide. The incorporation of the recognition tripeptide Arg-Gly-Asp into the cyclic peptide templates acted as a filter mechanism, restricting the otherwise free torsional relation of both side chains to a parallel orientation. Based on the derived results, several detailed features of the receptor binding site could be deduced in terms of receptor complementarity. These findings should govern the design of next-generation compounds with enhanced activities. Furthermore, the complementary stereochemical characteristics of the substrate can be used as boundary conditions for pseudoreceptor modelling studies that are capable of reconstructing a hypothetical binding pocket, qualitatively resembling the steric and electronic demands of gpIIb/IIIa. It is interesting to note that these features provide clear differentiation to requirements for inhibition of alpha v beta 3 substrate binding. This can account for the extremely high selectivity and activity of some of our constrained peptides for either the alpha IIb beta 3 or the alpha v beta 3 receptor.

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Section: Significance Of the Residue Following The Rgd Tripeptidecontrasting

confidence: 61%

Pharmacophore refinement of gpIIb/IIIa antagonists based on comparative studies of antiadhesive cyclic and acyclic RGD peptides

Müller

Gurrath

Kessler

1994

J Computer-Aided Mol Des

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“…The RGD region was found to be highly flexible, and the side chains of Arg and Asp with positive and negative charges, respectively, are separated by glycine and turned in opposite directions. Based on this information on their steric structure, a series of RGD-and KGD-containing peptides, including cyclic peptides, were designed by computer modelling; some derivatives were found to be as potent as intact kistrin in a platelet aggregation assay [64][65][66][67]. To date, a variety of RGD-and KGD derivatives have been under clinical trials and have been demonstrated to be effective agents in reducing complications of ischemia, especially restenosis after percutaneous transluminal coronary angioplasty (PTCA) [68,69].…”

Section: Design Of Antithrombotic Agentsmentioning

confidence: 99%

What have snakes taught us about integrins?

Huang¹

1998

Cellular and Molecular Life Sciences (CMLS)

101

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Snake venoms contain unique components that affect cell-matrix interactions. Disintegrins represent a class of low molecular weight, Arg-Gly-Asp (RGD)-containing, cysteine-rich peptides purified from the venom of various snakes among the Viperidae and Crotalidae. They bind with various degrees of specificity to integrins alpha IIb beta 3, alpha 5 beta 1 and alpha V beta 3 expressed on cells. Snake venom metalloproteases (high molecular mass haemorrhagins) also contain disintegrin-like domains, in addition to zinc-chelating sequences. Membrane-anchored ADAMs (A Disintegrin And Metalloprotease domain), multidomain molecules consisting of metalloprotease, disintegrin-like, cysteine-rich, and epidermal growth factor domains, a transmembrane domain and a cytoplasmic tail, are a new family of proteins. In the light of the large number and wide distribution of ADAMs, they may participate in cell-cell fusion events, including sperm-egg binding and fusion, myoblast fusion and other cell-cell and cell-matrix interactions. The structure-function relationship of these molecules is discussed.

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“…Scientists at SmithKline Beecham reported on the cyclic RGD-containing disulfide derivative 12, a highly active antagonist of the α IIb β 3 , with crystal and solution structures characterized by an extended conformation at the Gly residue, and C 7 -like conformations in the regions around Arg and Asp residues [69]. To test this conformational features, γ-turn mimetics were incorporated at the Asp level in nonpeptide analogues.…”

Section: β-Turn-based Peptidomimetics As Antagonists Of Integrinsmentioning

confidence: 99%

Modulation of Protein-Protein Interactions by Stabilizing/Mimicking Protein Secondary Structure Elements

Vega

Martı́n-Martı́nez²,

González‐Muñiz

2007

CTMC

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In view of the crucial role of protein-protein intercommunication both in biological and pathological processes, the search of modulators of protein-protein interactions (PPIs) is currently a challenging issue. The development of rational strategies to imitate key secondary structure elements of protein interfaces is complementary to other approaches based on the screening of synthetic or virtual libraries. In this sense, the present review provides representative examples of compounds that are able to disturb PPIs of therapeutic relevance, through the stabilization or the imitation of peptide hot-spots detected in contact areas of the interacting proteins. The review is divided into three sections, covering mimetics of the three main secondary structural elements found in proteins, in general, and in protein-protein interfaces, in particular (alpha-helices, beta-sheets, and reverse turns). Once the secondary element has been identified, the first approach typically involves the translation of the primary peptide structure into different cyclic analogues. This is normally followed by gradual decrease of the peptide nature through combination of peptide and non-peptide fragments in the same molecule. The final step usually consists in the development of pertinent organic scaffolds for appending key functional groups in the right spatial disposition, as a means towards totally non-peptide small molecule PPI modulators.

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Conformations of Arg-Gly-Asp containing heterodetic cyclic peptides: solution and crystal studies

Cited by 88 publications

References 6 publications

Pharmacophore refinement of gpIIb/IIIa antagonists based on comparative studies of antiadhesive cyclic and acyclic RGD peptides

Pharmacophore refinement of gpIIb/IIIa antagonists based on comparative studies of antiadhesive cyclic and acyclic RGD peptides

What have snakes taught us about integrins?

Modulation of Protein-Protein Interactions by Stabilizing/Mimicking Protein Secondary Structure Elements

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