From Peptide to Non-Peptide. 2. The de Novo Design of Potent, Non-peptidal Inhibitors of Platelet Aggregation Based on a Benzodiazepinedione Scaffold

McDowell, Robert S.; Blackburn, Brent; Gadek, Thomas R.; McGee, Lawrence R.; Rawson, Thomas E.; Reynolds, Mark; Robarge, Kirk; Somers, T. C.; Thorsett, Eugene D.

doi:10.1021/ja00091a008

Cited by 106 publications

(61 citation statements)

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“…Secondly, techniques for evaluating the binding characteristics of peptides are well established and easily performed in the laboratory. Finally, proteaseresistant peptide analogs, or nonpeptidic small molecules, can be designed based on the side-chain chemistries of the original peptide (13).…”

Section: Discussionmentioning

confidence: 99%

Design of a Novel Small Peptide Targeted against a Tumor-Specific Receptor

Campa

Kuan

O’Connor-McCourt

et al. 2000

Biochemical and Biophysical Research Communications

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Section: Discussionmentioning

confidence: 99%

Design of a Novel Small Peptide Targeted against a Tumor-Specific Receptor

Campa

Kuan

O’Connor-McCourt

et al. 2000

Biochemical and Biophysical Research Communications

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“…Similar de novo smallmolecule design efforts had been successful in the past from a similarly sized peptide (19)(20)(21). While these design studies were under way, ortho-bromobenzoyl tryptophan (designated compound 1 in Table 1 Table 1)…”

mentioning

confidence: 94%

Generation of an LFA-1 Antagonist by the Transfer of the ICAM-1 Immunoregulatory Epitope to a Small Molecule

Gadek

Burdick

McDowell

et al. 2002

Science

169

123

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The protein-protein interaction between leukocyte functional antigen-1 (LFA-1) and intercellular adhesion molecule-1 (ICAM-1) is critical to lymphocyte and immune system function. Here, we report on the transfer of the contiguous, nonlinear epitope of ICAM-1, responsible for its association with LFA-1, to a small-molecule framework. These LFA-1 antagonists bound LFA-1, blocked binding of ICAM-1, and inhibited a mixed lymphocyte reaction (MLR) with potency significantly greater than that of cyclosporine A. Furthermore, in comparison to an antibody to LFA-1, they exhibited significant anti-inflammatory effects in vivo. These results demonstrate the utility of small-molecule mimics of nonlinear protein epitopes and the protein epitopes themselves as leads in the identification of novel pharmaceutical agents.

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“…Where will isocyanide based multi-component reactions go in the next decade? With the advent of functional proteomics [72] delivering hundreds of new targets to drug discovery, ultra-high-throughput screening and a premium on novel biologically active entities, it seems reasonable to speculate that the discovery of new IMCRs will continue, spawning multiple post-condensation possibilities via secondary reactions. In addition to rational chemical design, Weber's pioneering 'combinatorial reaction finding' is one way to accelerate this [119].…”

Section: Resultsmentioning

confidence: 99%

“…Reports of the biological utility of 1,4-benzodiazepine-2,5-diones (BDP's), in particular, have appeared in many areas, including applications as antagonists of the platelet glycoprotein IIb-IIIa [72] and anti-convulsant agents to name but a few [73]. Many routes to libraries of this class of molecule have been developed, including one of the early pioneering solid phase methods reported by Bunin and Ellman [74].…”

Section: Udc (Ugi/de-boc/cyclize) Methodologymentioning

confidence: 99%

“Multi-component Reactions : Emerging Chemistry in Drug Discovery” ‘From Xylocain to Crixivan’

Hulme

Gore

2003

CMC

995

276

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With the recent emergence of combinatorial chemistry and high-speed parallel synthesis for drug discovery applications, the multi-component reaction (MCR) has seen a resurgence of interest. Easily automated one-pot reactions, such as the Ugi and Passerini reactions, are powerful tools for producing diverse arrays of compounds, often in one step and high yield. Despite this synthetic potential, the Ugi reaction is limited by producing products that are flexible and peptide-like, often being classified as 'non drug-like'. This review details developments of new, highly atom-economic MCR derived chemical methods, which enable the fast and efficient production of chemical libraries comprised of a variety of biologically relevant templates. Representative examples will also be given demonstrating the successful impact of MCR combinatorial methods at different stages of the lead discovery, lead optimization and pre-clinical process development arenas. This will include applications spanning biological tools, natural products and natural product-like diversity, traditional small molecule and 'biotech' therapeutics respectively. In particular, this review will focus on applications of isocyanide based MCR (IMCR) reactions.

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From Peptide to Non-Peptide. 2. The de Novo Design of Potent, Non-peptidal Inhibitors of Platelet Aggregation Based on a Benzodiazepinedione Scaffold

Cited by 106 publications

References 0 publications

Design of a Novel Small Peptide Targeted against a Tumor-Specific Receptor

Design of a Novel Small Peptide Targeted against a Tumor-Specific Receptor

Generation of an LFA-1 Antagonist by the Transfer of the ICAM-1 Immunoregulatory Epitope to a Small Molecule

“Multi-component Reactions : Emerging Chemistry in Drug Discovery” ‘From Xylocain to Crixivan’

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From Peptide to Non-Peptide. 2. The de Novo Design of Potent, Non-peptidal Inhibitors of Platelet Aggregation Based on a Benzodiazepinedione Scaffold

Cited by 106 publications

References 0 publications

Design of a Novel Small Peptide Targeted against a Tumor-Specific Receptor

Design of a Novel Small Peptide Targeted against a Tumor-Specific Receptor

Generation of an LFA-1 Antagonist by the Transfer of the ICAM-1 Immunoregulatory Epitope to a Small Molecule

&#x201C;Multi-component Reactions : Emerging Chemistry in Drug Discovery&#x201D; &#x2018;From Xylocain to Crixivan&#x2019;

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“Multi-component Reactions : Emerging Chemistry in Drug Discovery” ‘From Xylocain to Crixivan’