From peptide libraries to optimized nonpeptide ligands in the search for S‐farnesyltransferase inhibitors

Henlin, Jean‐Michel; Kucharczyk, Nathalie; Desmet-Beaufort, C.; Loynel, Armelle; Genton, Annie; Tucker, Gordon C.; Atassi, Ghanem; Fauchère, Jean‐Luc; Boutin, Jean A.; Bertrand, Marc

doi:10.1034/j.1399-3011.2001.00787.x

The Journal of Peptide Research

2001

DOI: 10.1034/j.1399-3011.2001.00787.x

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From peptide libraries to optimized nonpeptide ligands in the search for S‐farnesyltransferase inhibitors

Jean‐Michel Henlin

Nathalie Kucharczyk

C. Desmet-Beaufort

et al.

Abstract: A complete 331,776-member library of tetrapeptides made of 24 amino acid building blocks was synthesized robotically on solid phase and subjected to a deconvolution based on the inhibitory potency of the sublibraries in a HPLC assay of the S-farnesyltransferase activity in vitro. One of the non-natural peptide and noncysteine-containing leads Nip-Trp-Phe-His (Nip=p-nitrophenyl-L-alanine) was optimized chemically to give a proteolytically stable pseudopeptide with a 200-fold potency compared with the original l… Show more

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Cited by 3 publications

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“…Synthetic methods have been described for many peptide structural motifs, allowing the replacement of such motifs by nonpeptide moieties (30,31,38–40). In this way, the properties of high affinity and specificity can be transferred to a peptide mimetic, whose pharmacokinetic properties are more suitable for clinical use (31,41–43).…”

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NMR‐derived model of interconverting conformations of an ICAM‐1 inhibitory cyclic nonapeptide

Sillerud

Burks

Wester

et al. 2003

The Journal of Peptide Research

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We have produced by phage-display a disulfide-linked cyclic nonapeptide (inhibitory peptide-01, IP01), CLLRMRSIC, that binds to intracellular adhesion molecule-1 (ICAM-1) and blocks binding to its counter-structure, leukocyte functional antigen-1 (LFA-1). As a first step towards improving its pharmacologic properties, we have performed a structural and functional analysis of this peptide inhibitor to determine the features relevant to ICAM-1 binding. We report here the solution model of our initial product, IP01, as derived from two-dimensional nuclear magnetic resonance (NMR) restraints and molecular modeling. Distance and dihedral angle restraints, generated from nuclear Overhauser effect spectroscopy (NOESY) and one-dimensional-NMR experiments respectively, were used to generate an ensemble of structures using distance geometry and simulated annealing. Molecular dynamic simulations produced three interconverting conformational families consistent with the NMR-derived constraints. We describe these conformations and their mechanism of interconversion. Furthermore, we have measured the IC50 s of a series of inhibitors generated from IP01 through alanine substitution of each residue. These results show that the L2-L3-R4-M5-R6 segment is functionally active, conformationally flexible, and contains a beta-turn involving residues R4-S7, while the C1-C9-I8-S7 segment is less functionally-active but adopts a more defined solution conformation, consistent with a scaffolding function. This model will be useful for designing nonpeptide-based organic inhibitors with improved pharmacologic properties.

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mentioning

confidence: 99%

NMR‐derived model of interconverting conformations of an ICAM‐1 inhibitory cyclic nonapeptide

Sillerud

Burks

Wester

et al. 2003

The Journal of Peptide Research

View full text Add to dashboard Cite

show abstract

“…Synthetic methods have been described for many peptide structural motifs, allowing the replacement of such motifs by nonpeptide moieties (28,37–39). In this way, the properties of high affinity and specificity can be transferred to a peptidomimetic or nonpeptide organic, increasing potency and allowing for oral administration (28,40,41). The identification and structural elucidation of more potent peptide derivatives is a necessary first step in this process.…”

mentioning

confidence: 99%

NMR solution structure of a potent cyclic nonapeptide inhibitor of ICAM‐1‐mediated leukocyte adhesion produced by homologous amino acid substitution

Sillerud

Burks

Brown

et al. 2004

The Journal of Peptide Research

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We have previously described a disulfide-linked cyclic nonapeptide (inhibitory peptide-01, IP01), with the sequence CLLRMRSIC, which binds to intercellular adhesion molecule-1 (ICAM-1), and blocks binding to its counter-structure, the integrin alphaLbeta2 (leukocyte functional antigen-1, LFA-1) (Sillerud et al., J. Peptide Res. 62, 2003: 97). We now report the optimization of this peptide by means of single homologous amino acid substitutions to yield a new peptide (IP02-K6; CLLRMKSAC) which shows an approximately sixfold improvement in inhibitory activity of multivalent leukocyte binding (inhibition constant for 50% inhibition, IC50 = 90 microm) compared with IP01 (IC50 = 580 microm). This improvement in activity gives IP02-K6 potent in vivo activity in a murine model of ischemia reperfusion injury (Merchant et al., Am. J. Physiol. Heart Circ. 284, 2003: H1260). In order to determine the structural features relevant to ICAM-1-binding, we have determined the structure of IP02-K6 using proton nuclear magnetic resonance (NMR) spectroscopy and restrained molecular modeling. In our previously reported study of solution models of IP01, we observed three interconverting conformations during low-temperature molecular dynamics simulation. In the present study, we find a single conformation of IP02-K6 similar to one of the previously found conformations of IP01 (family C). In particular, an R4-S7 beta-turn is present in similar proportions in both conformation C of IP01 and in IP02-K6; this motif is important in binding to ICAM-1 because this turn enables the IP02-K6 backbone to drape over proline-36 on ICAM-1. The NMR-derived solution model of IP02-K6 was found to dock at the alphaLbeta2-binding site on ICAM-1 with no changes in peptide backbone conformation. This docking model displaced five of the 15 alphaLbeta2 residues at the ICAM-1-binding site and provided a rationale for understanding the quantitative relationship between IP02-K6 structure and biologic activity.

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Papers on combinatorial chemistry or solid-phase synthesis from other journals - April 2001

2001

Combinatorial Chemistry - an Online Journal

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From peptide libraries to optimized nonpeptide ligands in the search for S‐farnesyltransferase inhibitors

Cited by 3 publications

References 32 publications

NMR‐derived model of interconverting conformations of an ICAM‐1 inhibitory cyclic nonapeptide

NMR‐derived model of interconverting conformations of an ICAM‐1 inhibitory cyclic nonapeptide

NMR solution structure of a potent cyclic nonapeptide inhibitor of ICAM‐1‐mediated leukocyte adhesion produced by homologous amino acid substitution

Papers on combinatorial chemistry or solid-phase synthesis from other journals - April 2001

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