Stefan Andreas Randl
Novartis
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Publication
Featured researches published by Stefan Andreas Randl.
Nature Chemical Biology | 2016
Jürgen Maibaum; Sha-Mei Liao; Anna Vulpetti; Nils Ostermann; Stefan Andreas Randl; Simon Rüdisser; Edwige Liliane Jeanne Lorthiois; Paul Erbel; Bernd Kinzel; Fabrice Kolb; Samuel Barbieri; Julia Wagner; Corinne Durand; Kamal Fettis; Solene Dussauge; Nicola Hughes; Omar Delgado; Ulrich Hommel; Ty Gould; Aengus Mac Sweeney; Bernd Gerhartz; Frederic Cumin; Stefanie Flohr; Anna Schubart; Bruce Jaffee; Richard Harrison; Antonio M. Risitano; Jörg Eder; Karen Anderson
Complement is a key component of the innate immune system, recognizing pathogens and promoting their elimination. Complement component 3 (C3) is the central component of the system. Activation of C3 can be initiated by three distinct routes-the classical, the lectin and the alternative pathways-with the alternative pathway also acting as an amplification loop for the other two pathways. The protease factor D (FD) is essential for this amplification process, which, when dysregulated, predisposes individuals to diverse disorders including age-related macular degeneration and paroxysmal nocturnal hemoglobinuria (PNH). Here we describe the identification of potent and selective small-molecule inhibitors of FD. These inhibitors efficiently block alternative pathway (AP) activation and prevent both C3 deposition onto, and lysis of, PNH erythrocytes. Their oral administration inhibited lipopolysaccharide-induced AP activation in FD-humanized mice. These data demonstrate the feasibility of inhibiting the AP with small-molecule antagonists and support the development of FD inhibitors for the treatment of complement-mediated diseases.
Journal of Medicinal Chemistry | 2017
Anna Vulpetti; Stefan Andreas Randl; Simon Rüdisser; Nils Ostermann; Paul Erbel; Aengus Mac Sweeney; Thomas Zoller; Bahaa Salem; Bernd Gerhartz; Frederic Cumin; Ulrich Hommel; Claudio Dalvit; Edwige Liliane Jeanne Lorthiois; Jürgen Maibaum
Chronic dysregulation of alternative complement pathway activation has been associated with diverse clinical disorders including age-related macular degeneration and paroxysmal nocturnal hemoglobinurea. Factor D is a trypsin-like serine protease with a narrow specificity for arginine in the P1 position, which catalyzes the first enzymatic reaction of the amplification loop of the alternative pathway. In this article, we describe two hit finding approaches leading to the discovery of new chemical matter for this pivotal protease of the complement system: in silico active site mapping for hot spot identification to guide rational structure-based design and NMR screening of focused and diverse fragment libraries. The wealth of information gathered by these complementary approaches enabled the identification of ligands binding to different subpockets of the latent Factor D conformation and was instrumental for understanding the binding requirements for the generation of the first known potent noncovalent reversible Factor D inhibitors.
Journal of Medicinal Chemistry | 2017
Edwige Liliane Jeanne Lorthiois; Karen S. Anderson; Anna Vulpetti; Olivier Rogel; Frederic Cumin; Nils Ostermann; Stefan Steinbacher; Aengus Mac Sweeney; Omar Delgado; Sha-Mei Liao; Stefan Andreas Randl; Simon Rüdisser; Solene Dussauge; Kamal Fettis; Laurence Kieffer; Andrea De Erkenez; Louis Yang; Constanze Hartwieg; Upendra A. Argikar; Laura R. La Bonte; Ronald Newton; Viral Kansara; Stefanie Flohr; Ulrich Hommel; Bruce Jaffee; Jürgen Maibaum
The highly specific S1 serine protease factor D (FD) plays a central role in the amplification of the complement alternative pathway (AP) of the innate immune system. Genetic associations in humans have implicated AP activation in age-related macular degeneration (AMD), and AP dysfunction predisposes individuals to disorders such as paroxysmal nocturnal hemoglobinuria (PNH) and atypical hemolytic uremic syndrome (aHUS). The combination of structure-based hit identification and subsequent optimization of the center (S)-proline-based lead 7 has led to the discovery of noncovalent reversible and selective human factor D (FD) inhibitors with drug-like properties. The orally bioavailable compound 2 exerted excellent potency in 50% human whole blood in vitro and blocked AP activity ex vivo after oral administration to monkeys as demonstrated by inhibition of membrane attack complex (MAC) formation. Inhibitor 2 demonstrated sustained oral and ocular efficacy in a model of lipopolysaccharide (LPS)-induced systemic AP activation in mice expressing human FD.
Archive | 2013
Eva Altmann; Ulrich Hommel; Edwige Liliane Jeanne Lorthiois; Juergen Klaus Maibaum; Nils Ostermann; Jean Quancard; Stefan Andreas Randl; Olivier Rogel; Oliver Simic; Anna Vulpetti
Archive | 2008
Shawn D. Britt; Jiping Fu; David Thomas Parker; Michael A. Patane; Prakash Raman; Branko Radetich; Mohindra Seepersaud; Aregahegn Yifru; Rui Zheng; Trixi Brandl; Sylvain Cottens; Claus Ehrhardt; Stefan Andreas Randl; Pascal Rigollier; Nikolaus Schiering; Oliver Simic
Archive | 2012
Eva Altmann; Ulrich Hommel; Edwige Liliane Jeanne Lorthiois; Juergen Klaus Maibaum; Nils Ostermann; Jean Quancard; Stefan Andreas Randl; Olivier Rogel; Oliver Simic; Anna Vulpetti
Archive | 2008
Stefanie Flohr; Stefan Andreas Randl; Nils Ostermann; Ulrich Hassiepen; Frederic Berst; Ursula Bodendorf; Bernd Gerhartz; Andreas Marzinzik; Claus Ehrhardt; Josef G. Meingassner
Archive | 2013
Eva Altmann; Ulrich Hommel; Edwige Liliane Jeanne Lorthiois; Jeurgen Klaus Maibaum; Nils Ostermann; Jean Quancard; Stefan Andreas Randl; Olivier Rogel; Anna Vulpetti
Archive | 2014
Christopher Towler; Eva Altmann; Ulrich Hommel; Edwige Liliane Jeanne Lorthiois; Juergen Klaus Maibaum; Nils Ostermann; Jean Quancard; Stefan Andreas Randl; Oliver Simic; Anna Vulpetti; Olivier Rogel
Archive | 2013
Christopher Towler; Eva Altmann; Ulrich Hommel; Edwige Liliane Jeanne Lorthiois; Juergen Klaus Maibaum; Nils Ostermann; Jean Quancard; Stefan Andreas Randl; Oliver Simic; Anna Vulpetti; Olivier Rogel