Elsa Locardi
Jerini
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Publication
Featured researches published by Elsa Locardi.
Journal of Medicinal Chemistry | 2009
Christoph Gibson; Karsten Schnatbaum; Jochen Pfeifer; Elsa Locardi; Matthias Paschke; Ulf Reimer; Uwe Richter; Dirk Scharn; Alexander Faussner; Thomas Tradler
Blockade of the bradykinin B(2) receptor provides therapeutic benefit in hereditary angioedema (HAE) and potentially in many other diseases. Herein, we describe the development of highly potent B(2) receptor antagonists with a molecular weight of approximately 500 g/mol. First, known quinoline-based B(2) receptor antagonists were stripped down to their shared core motif 53, which turned out to be the minimum pharmacophore. Targeted modifications of 53 resulted in the highly water-soluble lead compound 8a. Extensive exploration of its structure-activity relationship resulted in a series of highly potent B(2) receptor antagonists, featuring a hydrogen bond accepting functionality, which presumably interacts with the side chain of Asn-107 of the B(2) receptor. Optimization of the microsomal stability and cytochrome P450 inhibition eventually led to the discovery of the highly potent and orally available B(2) receptor antagonist 52e (JSM10292), which showed the best overall properties.
Bioorganic & Medicinal Chemistry Letters | 2010
Gunther Zischinsky; Roland Stragies; Marco Schaudt; Jochen Pfeifer; Christoph Gibson; Elsa Locardi; Dirk Scharn; Uwe Richter; Holger Kalkhof; Klaus Dinkel; Karsten Schnatbaum
Efforts to find new bradykinin B(1) receptor antagonists identified 2-aminobenzimidazole as a novel core. Subsequent transformation into five-membered diaminoheterocycle derivatives and their synthesis and SAR is described. This resulted in compounds with low nanomolar activity.
Bioorganic & Medicinal Chemistry Letters | 2010
Marco Schaudt; Elsa Locardi; Gunther Zischinsky; Roland Stragies; Jochen Pfeifer; Christoph Gibson; Dirk Scharn; Uwe Richter; Holger Kalkhof; Klaus Dinkel; Karsten Schnatbaum
The synthesis and SAR of two series of bradykinin B(1) receptor antagonists is described. The benzamide moiety proved to be a suitable replacement for the aryl ester functionality of biaryl based antagonists. In addition, it was found that semicarbazides can effectively replace cyclopropyl amino acids. The compounds with the best overall profile were biaryl semicarbazides which display high antagonistic activity, low Caco-2 efflux and high oral bioavailability in the rat.
Bioorganic & Medicinal Chemistry Letters | 2010
Karsten Schnatbaum; Marco Schaudt; Roland Stragies; Jochen Pfeifer; Christoph Gibson; Elsa Locardi; Dirk Scharn; Uwe Richter; Holger Kalkhof; Klaus Dinkel; Gunther Zischinsky
Hydroxy urea moieties are introduced as a new class of bradykinin B(1) receptor antagonists. First, the SAR of the lead compound was systematically explored. Subsequent optimization resulted in the identification of several biaryl-based hydroxyurea bradykinin B(1) receptor antagonists with low-nanomolar activity and very high oral bioavailability in the rat.
Bioorganic & Medicinal Chemistry Letters | 2006
Karsten Schnatbaum; Elsa Locardi; Dirk Scharn; Uwe Richter; Heiko Hawlisch; Jochen Knolle; Thomas Polakowski
Archive | 2006
Karsten Schnatbaum; Dirk Scharn; Elsa Locardi; Thomas Polakowski; Uwe Richter; Ulrich Reineke; Gerd Hummel
Archive | 2008
Christoph Gibson; Thomas Tradler; Karsten Schnatbaum; Jochen Pfeifer; Elsa Locardi; Dirk Scharn; Matthias Paschke; Ulf Reimer; Uwe Richter; Gerd Hummel; Ulrich Reineke
Archive | 2008
Elsa Locardi; Klaus Dinkel; Marco Schaudt; Uwe Richter; Dirk Scharn; Gerd Hummel; Ulrich Reineke; Ulf Reimer
Archive | 2008
Christoph Gibson; Karsten Schnatbaum; Thomas Tradler; Jochen Pfeifer; Dirk Scharn; Ulf Reimer; Uwe Richter; Gerd Hummel; Ulrich Reineke; Elsa Locardi; Matthias Paschke
Archive | 2005
Karsten Schnatbaum; Dirk Scharn; Elsa Locardi; Thomas Polakowski; Uwe Richter; Gerd Hummel; Ulrich Reineke
