ChemMedChem

Copyright © 2012 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim

Cover image for Vol. 7 Issue 2

Editor-in-Chief: Natalia Ortúzar

Impact Factor: 3.306

ISI Journal Citation Reports © Ranking: 2010: 10/54 (Chemistry Medicinal); 67/249 (Pharmacology & Pharmacy)

Online ISSN: 1860-7187

Associated Title(s): Angewandte Chemie International Edition, Chemistry - A European Journal, Chemistry – An Asian Journal, ChemBioChem, Medicinal Research Reviews, Molecular Informatics

Recently Published Issues

See all

Latest News

Browse more news

February 04, 2012

VIP: Fluorogenic Peptide-Based Substrates for Monitoring Thrombin Activity

VIP: Fluorogenic Peptide-Based Substrates for Monitoring Thrombin Activity

Sander S. van Berkel, Bas van der Lee, Floris L. van Delft, Rob Wagenvoord, H. Coenraad Hemker, Floris P. J. T. Rutjes*

Thrombin plays a pivotal role in various pathological disturbances of the haemostatic system. Overexpression of thrombin can result in thrombosis, whereas its underexpression can lead to haemophilia. Therefore, accurate monitoring of thrombin activity is key to determining the proper course of treatment for a given patient. An accurate assessment of thrombin concentration in a blood sample can be used to estimate the blood's coagulation ability. A tool for monitoring the generation and disappearance of thrombin, and thus its concentration over time, is the so-called thrombin generation test (TGT).

In a collaborative project headed by Prof. Floris Rutjes (Radboud Univeristy Nijmegen (NL)) and Prof. Hemker (Cardiovascular Research Institute Maastricht (NL)), novel thrombin-specific fluorogenic peptides were developed for accurate assessments of thrombin concentrations using the TGT. Adding a thrombin-specific fluorogenic substrate to a clotting plasma sample results in thrombin-mediated hydrolysis of the substrate, releasing the fluorophore from the substrate. The use of a spectrophotometrically measurable fluorophore increases the sensitivity and thus accuracy of the TGT. Monitoring the increase in the induced signal over time gives rise to a thrombin generation curve, providing various essential coagulation parameters. The use of fluorogenic peptides in combination with the TGT is expected to find broad application in the field of haemostasis and thrombosis.

Received November 25, 2011; published online January 31, 2012, DOI: 10.1002/cmdc.201100560.

Your Comment...

[Browse more news]

Recently Published Articles

  1. Investigation of D1 Receptor–Agonist Interactions and D1/D2 Agonist Selectivity Using a Combination of Pharmacophore and Receptor Homology Modeling

    Marcus Malo, Dr. Lars Brive, Prof. Kristina Luthman and Dr. Peder Svensson

    Article first published online: 7 FEB 2012 | DOI: 10.1002/cmdc.201100546

    Thumbnail image of graphical abstract

    The delicate balance between dopamine D1 and D2 agonism was investigated by using our combined receptor and pharmacophore modeling approach described in the preceding paper. Not only can the developed receptor models be used to understand the factors that determine receptor isoform selectivity, but also to design new dopamine receptor-selective agonists for use as potential therapeutic agents.

  2. Investigation of D2 Receptor–Agonist Interactions Using a Combination of Pharmacophore and Receptor Homology Modeling

    Marcus Malo, Dr. Lars Brive, Prof. Kristina Luthman and Dr. Peder Svensson

    Article first published online: 7 FEB 2012 | DOI: 10.1002/cmdc.201100545

    Thumbnail image of graphical abstract

    The magic key for dopamine D2 receptor agonism was studied by using a combined receptor and pharmacophore modeling approach. All available experimental data, including a set of carefully selected active and inactive ligands, were used to identify the reasons behind selectivity and to pinpoint the specific ligand–receptor interactions made by D2 agonists.

  3. Discovery of Novel 2-N-Aryl-Substituted Benzenesulfonamidoacetamides: Orally Bioavailable Tubulin Polymerization Inhibitors with Marked Antitumor Activities

    Dr. Zulong Liu, Dr. Zuyu Zhou, Dr. Wei Tian, Dr. Xing Fan, Ding Xue, Prof. Long Yu, Prof. Qiang Yu and Prof. Ya-Qiu Long

    Article first published online: 6 FEB 2012 | DOI: 10.1002/cmdc.201100529

    Thumbnail image of graphical abstract

    The latest and greatest: Structural optimization of an in-house screening hit afforded a novel class of benzenesulfonamides as orally bioavailable and potent tubulin polymerization inhibitors. These compounds act as antimitotic agents and exhibit a tubulin binding mechanism similar to that of colchicine. The most potent analogues have in vivo antitumor efficacy and are able to circumvent P-glycoprotein-mediated multidrug resistance in tumor cells.

SEARCH

SEARCH BY CITATION