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Development of Inhibitors of SAICAR Synthetase (PurC) from Mycobacterium abscessus Using a Fragment-Based Approach.

Sitthivut CharoensutthivarakulSherine E ThomasAmy CurranKaren P BrownJuan M BelardinelliAndrew J WhitehouseMarta Acebrón-García-de-EulateJaspar SanganSubramanian G GramaniMary JacksonVitor MendesR Andres FlotoTom L BlundellAnthony G CoyneChris Abell
Published in: ACS infectious diseases (2022)
Mycobacterium abscessus (Mab) has emerged as a challenging threat to individuals with cystic fibrosis. Infections caused by this pathogen are often impossible to treat due to the intrinsic antibiotic resistance leading to lung malfunction and eventually death. Therefore, there is an urgent need to develop new drugs against novel targets in Mab to overcome drug resistance and subsequent treatment failure. In this study, SAICAR synthetase (PurC) from Mab was identified as a promising target for novel antibiotics. An in-house fragment library screen and a high-throughput X-ray crystallographic screen of diverse fragment libraries were explored to provide crucial starting points for fragment elaboration. A series of compounds developed from fragment growing and merging strategies, guided by crystallographic information and careful hit-to-lead optimization, have achieved potent nanomolar binding affinity against the enzyme. Some compounds also show a promising inhibitory effect against Mab and Mtb. This work utilizes a fragment-based design and demonstrates for the first time the potential to develop inhibitors against PurC from Mab .
Keyphrases
  • high throughput
  • monoclonal antibody
  • mycobacterium tuberculosis
  • magnetic resonance imaging
  • computed tomography
  • social media
  • anti inflammatory
  • transcription factor
  • binding protein
  • drug induced
  • combination therapy