Structure-Based Library Design and Fragment Screening for the Identification of Reversible Complement Factor D Protease Inhibitors.
Anna VulpettiStefan RandlSimon RüdisserNils OstermannPaul ErbelAengus Mac SweeneyThomas ZollerBahaa SalemBernd GerhartzFrederic CuminUlrich HommelClaudio DalvitEdwige LorthioisJürgen MaibaumPublished in: Journal of medicinal chemistry (2017)
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.
Keyphrases
- age related macular degeneration
- high resolution
- bioinformatics analysis
- blood pressure
- obstructive sleep apnea
- nitric oxide
- high throughput
- molecular docking
- molecular dynamics simulations
- transcription factor
- anti inflammatory
- single cell
- health information
- sleep apnea
- mass spectrometry
- protein kinase
- crystal structure
- amino acid
- structural basis
- binding protein
- label free