Alexander Lederer
University of Zurich
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Featured researches published by Alexander Lederer.
Science | 2010
Nityakalyani Srinivas; Peter Jetter; Bernhard J. Ueberbacher; Martina Werneburg; Katja Zerbe; Jessica Steinmann; Benjamin Van der Meijden; Francesca Bernardini; Alexander Lederer; Ricardo L. A. Dias; Pauline Misson; Heiko Henze; Jürg Zumbrunn; Frank Gombert; Daniel Obrecht; Peter Hunziker; Stefan Schauer; Urs Ziegler; Andres Käch; Leo Eberl; Kathrin Riedel; Steven J. Demarco; John A. Robinson
Killing Pseudomonas Gram-negative Pseudomonas bacteria are opportunistic pathogens, and drug-resistant strains present a serious health problem. Srinivas et al. (p. 1010) synthesized a family of peptidomimetic antibiotics that is active only against Pseudomonas. These antibiotics do not lyse the cell membrane, but instead target an essential outer membrane protein, LptD, which plays a role in the assembly of lipopolysaccharide in the outer cell membrane. Activity in a mouse infection model suggests that the antibiotics might have therapeutic potential. In addition, LptD is widely distributed in gram-negative bacteria and so its validation as a target has the potential to drive development of antibiotics with a broader spectrum of activity against gram-negative pathogens. A synthesized antibiotic targets a protein involved in outer-membrane biogenesis to selectively kill Pseudomonas pathogens. Antibiotics with new mechanisms of action are urgently required to combat the growing health threat posed by resistant pathogenic microorganisms. We synthesized a family of peptidomimetic antibiotics based on the antimicrobial peptide protegrin I. Several rounds of optimization gave a lead compound that was active in the nanomolar range against Gram-negative Pseudomonas spp., but was largely inactive against other Gram-negative and Gram-positive bacteria. Biochemical and genetic studies showed that the peptidomimetics had a non–membrane-lytic mechanism of action and identified a homolog of the β-barrel protein LptD (Imp/OstA), which functions in outer-membrane biogenesis, as a cellular target. The peptidomimetic showed potent antimicrobial activity in a mouse septicemia infection model. Drug-resistant strains of Pseudomonas are a serious health problem, so this family of antibiotics may have important therapeutic applications.
Bioorganic & Medicinal Chemistry | 2006
Steven J. Demarco; Heiko Henze; Alexander Lederer; Kerstin Moehle; Reshmi Mukherjee; Barbara Romagnoli; John A. Robinson; Federico Brianza; Frank Gombert; Sergio Lociuro; Christian Ludin; Jan W. Vrijbloed; Jürg Zumbrunn; Jean-Pierre Obrecht; Daniel Obrecht; Vincent Brondani; François Hamy; Thomas Klimkait
Archive | 2016
Frank Gombert; Daniel Obrecht; Alexander Lederer; Johann Zimmermann; Christian Oefner
Archive | 2014
Sophie Barthélémy; Christian Bisang; Frank Gombert; Alexander Lederer; Daniel Obrecht; Barbara Romagnoli; Jürg Zumbrunn; Tobias Remus; Guillaume Lemercier
Archive | 2014
Daniel Obrecht; Frank Gombert; Alexander Lederer; Barbara Romagnoli; Christian Bisang
Archive | 2010
Frank Gombert; Alexander Lederer; Daniel Obrecht; Barbara Romagnoli; Christian Bisang; Christian Ludin
Chimia | 2007
Alexander Lederer; Steven J. Demarco; Heiko Henze; Barbara Romagnoli; Reshmi Mukherjee; Jürg Zumbrunn; Federico Brianza; Frank Gombert; Christian Ludin; Jan W. Vrijbloed; Jean-Pierre Obrecht; Sergio Lociuro; Vincent Brondani; François Hamy; Thomas Klimkait; Kerstin Moehle; John A. Robinson; Daniel Obrecht
Archive | 2010
Françoise Jung; Frank Gombert; Daniel Obrecht; Christian Bisang; Sophie Barthélémy; Alexander Lederer; Eric Chevalier
Archive | 2017
John Anthony Robinson; Kerstin Möhle; Markus Seitz; Ludovic T. Maillard; Roba Mounme; Frank Gombert; Odile Sellier-Kessler; Heiko Henze; Daniel Obrecht; Christian Bisang; Alexander Lederer
Archive | 2015
Daniel Obrecht; Anatol Luther; Francesca Bernardini; Gildas Deniau; Alexander Lederer