Literature DB >> 32393499

Insights into the l,d-Transpeptidases and d,d-Carboxypeptidase of Mycobacterium abscessus: Ceftaroline, Imipenem, and Novel Diazabicyclooctane Inhibitors.

Khalid M Dousa1, Sebastian G Kurz2, Magdalena A Taracila3,4, Tracey Bonfield4,5, Christopher R Bethel3, Melissa D Barnes3,4, Suresh Selvaraju6, Ayman M Abdelhamed7, Barry N Kreiswirth8, W Henry Boom1, Shannon H Kasperbauer9, Charles L Daley9, Robert A Bonomo10,4,11,12,13,14,15,16.   

Abstract

Mycobacterium abscessus is a highly drug-resistant nontuberculous mycobacterium (NTM). Efforts to discover new treatments for M. abscessus infections are accelerating, with a focus on cell wall synthesis proteins (M. abscessus l,d-transpeptidases 1 to 5 [LdtMab1 to LdtMab5] and d,d-carboxypeptidase) that are targeted by β-lactam antibiotics. A challenge to this approach is the presence of chromosomally encoded β-lactamase (BlaMab). Using a mechanism-based approach, we found that a novel ceftaroline-imipenem combination effectively lowered the MICs of M. abscessus isolates (MIC50 ≤ 0.25 μg/ml; MIC90 ≤ 0.5 μg/ml). Combining ceftaroline and imipenem with a β-lactamase inhibitor, i.e., relebactam or avibactam, demonstrated only a modest effect on susceptibility compared to each of the β-lactams alone. In steady-state kinetic assays, BlaMab exhibited a lower Ki  app (0.30 ± 0.03 μM for avibactam and 136 ± 14 μM for relebactam) and a higher acylation rate for avibactam (k 2/K = 3.4 × 105 ± 0.4 × 105 M-1 s-1 for avibactam and 6 × 102 ± 0.6 × 102 M-1 s-1 for relebactam). The k cat/Km was nearly 10-fold lower for ceftaroline fosamil (0.007 ± 0.001 μM-1 s-1) than for imipenem (0.056 ± 0.006 μM-1 s-1). Timed mass spectrometry captured complexes of avibactam and BlaMab, LdtMab1, LdtMab2, LdtMab4, and d,d-carboxypeptidase, whereas relebactam bound only BlaMab, LdtMab1, and LdtMab2 Interestingly, LdtMab1, LdtMab2, LdtMab4, LdtMab5, and d,d-carboxypeptidase bound only to imipenem when incubated with imipenem and ceftaroline fosamil. We next determined the binding constants of imipenem and ceftaroline fosamil for LdtMab1, LdtMab2, LdtMab4, and LdtMab5 and showed that imipenem bound >100-fold more avidly than ceftaroline fosamil to LdtMab1 and LdtMab2 (e.g., Ki  app or Km of LdtMab1 = 0.01 ± 0.01 μM for imipenem versus 0.73 ± 0.08 μM for ceftaroline fosamil). Molecular modeling indicates that LdtMab2 readily accommodates imipenem, but the active site must widen to ≥8 Å for ceftaroline to enter. Our analysis demonstrates that ceftaroline and imipenem binding to multiple targets (l,d-transpeptidases and d,d-carboxypeptidase) and provides a mechanistic rationale for the effectiveness of this dual β-lactam combination in M. abscessus infections. This is a work of the U.S. Government and is not subject to copyright protection in the United States. Foreign copyrights may apply.

Entities:  

Keywords:  Mycobacterium abscessus; antibiotic resistance; antibiotics; bacteria; ceftaroline; diazabicyclooctane; imipenem; inhibitor; mycobacteria

Mesh:

Substances:

Year:  2020        PMID: 32393499      PMCID: PMC7526840          DOI: 10.1128/AAC.00098-20

Source DB:  PubMed          Journal:  Antimicrob Agents Chemother        ISSN: 0066-4804            Impact factor:   5.191


  18 in total

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Journal:  J Comput Chem       Date:  2005-12       Impact factor: 3.376

2.  Strategic Approaches to Overcome Resistance against Gram-Negative Pathogens Using β-Lactamase Inhibitors and β-Lactam Enhancers: Activity of Three Novel Diazabicyclooctanes WCK 5153, Zidebactam (WCK 5107), and WCK 4234.

Authors:  Krisztina M Papp-Wallace; Nhu Q Nguyen; Michael R Jacobs; Christopher R Bethel; Melissa D Barnes; Vijay Kumar; Saralee Bajaksouzian; Susan D Rudin; Philip N Rather; Satish Bhavsar; Tadiparthi Ravikumar; Prasad K Deshpande; Vijay Patil; Ravindra Yeole; Sachin S Bhagwat; Mahesh V Patel; Focco van den Akker; Robert A Bonomo
Journal:  J Med Chem       Date:  2018-04-20       Impact factor: 7.446

3.  Automated comparative protein structure modeling with SWISS-MODEL and Swiss-PdbViewer: a historical perspective.

Authors:  Nicolas Guex; Manuel C Peitsch; Torsten Schwede
Journal:  Electrophoresis       Date:  2009-06       Impact factor: 3.535

4.  β-Lactamase inhibition by avibactam in Mycobacterium abscessus.

Authors:  Vincent Dubée; Audrey Bernut; Mélanie Cortes; Tiffany Lesne; Delphine Dorchene; Anne-Laure Lefebvre; Jean-Emmanuel Hugonnet; Laurent Gutmann; Jean-Luc Mainardi; Jean-Louis Herrmann; Jean-Louis Gaillard; Laurent Kremer; Michel Arthur
Journal:  J Antimicrob Chemother       Date:  2014-12-18       Impact factor: 5.790

5.  Impact of β-lactamase inhibition on the activity of ceftaroline against Mycobacterium tuberculosis and Mycobacterium abscessus.

Authors:  Vincent Dubée; Daria Soroka; Mélanie Cortes; Anne-Laure Lefebvre; Laurent Gutmann; Jean-Emmanuel Hugonnet; Michel Arthur; Jean-Luc Mainardi
Journal:  Antimicrob Agents Chemother       Date:  2015-03-02       Impact factor: 5.191

6.  Mycobacterium abscessus l,d-Transpeptidases Are Susceptible to Inactivation by Carbapenems and Cephalosporins but Not Penicillins.

Authors:  Pankaj Kumar; Varsha Chauhan; José Rogério A Silva; Jerônimo Lameira; Felipe B d'Andrea; Shao-Gang Li; Stephan L Ginell; Joel S Freundlich; Cláudio Nahum Alves; Scott Bailey; Keira A Cohen; Gyanu Lamichhane
Journal:  Antimicrob Agents Chemother       Date:  2017-09-22       Impact factor: 5.191

7.  Characterization of broad-spectrum Mycobacterium abscessus class A β-lactamase.

Authors:  Daria Soroka; Vincent Dubée; Olivia Soulier-Escrihuela; Guillaume Cuinet; Jean-Emmanuel Hugonnet; Laurent Gutmann; Jean-Luc Mainardi; Michel Arthur
Journal:  J Antimicrob Chemother       Date:  2013-10-16       Impact factor: 5.790

Review 8.  Nontuberculous mycobacteria in respiratory tract infections, eastern Asia.

Authors:  Sami Simons; Jakko van Ingen; Po-Ren Hsueh; Nguyen Van Hung; P N Richard Dekhuijzen; Martin J Boeree; Dick van Soolingen
Journal:  Emerg Infect Dis       Date:  2011-03       Impact factor: 6.883

9.  The addition of avibactam renders piperacillin an effective treatment for Mycobacterium abscessus infection in an in vivo model.

Authors:  Michal Meir; Pablo Bifani; Daniel Barkan
Journal:  Antimicrob Resist Infect Control       Date:  2018-12-13       Impact factor: 4.887

10.  Dual β-Lactam Combinations Highly Active against Mycobacterium abscessus Complex In Vitro.

Authors:  R Pandey; L Chen; C Manca; S Jenkins; L Glaser; C Vinnard; G Stone; J Lee; B Mathema; E L Nuermberger; R A Bonomo; B N Kreiswirth
Journal:  mBio       Date:  2019-02-12       Impact factor: 7.786

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2.  Inhibiting Mycobacterium abscessus Cell Wall Synthesis: Using a Novel Diazabicyclooctane β-Lactamase Inhibitor To Augment β-Lactam Action.

Authors:  Khalid M Dousa; David C Nguyen; Sebastian G Kurz; Magdalena A Taracila; Christopher R Bethel; William Schinabeck; Barry N Kreiswirth; Sheldon T Brown; W Henry Boom; Richard S Hotchkiss; Kenneth E Remy; Frank J Jacono; Charles L Daley; Steven M Holland; Alita A Miller; Robert A Bonomo
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3.  Strongly Bactericidal All-Oral β-Lactam Combinations for the Treatment of Mycobacterium abscessus Lung Disease.

Authors:  Dereje A Negatu; Matthew D Zimmerman; Véronique Dartois; Thomas Dick
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4.  "One-Two Punch": Synergistic ß-Lactam Combinations for Mycobacterium abscessus and Target Redundancy in the Inhibition of Peptidoglycan Synthesis Enzymes.

Authors:  David C Nguyen; Khalid M Dousa; Sebastian G Kurz; Sheldon T Brown; George Drusano; Steven M Holland; Barry N Kreiswirth; W Henry Boom; Charles L Daley; Robert A Bonomo
Journal:  Clin Infect Dis       Date:  2021-10-20       Impact factor: 20.999

5.  First Penicillin-Binding Protein Occupancy Patterns for 15 β-Lactams and β-Lactamase Inhibitors in Mycobacterium abscessus.

Authors:  Alaa R M Sayed; Nirav R Shah; Kari B Basso; Manasi Kamat; Yuanyuan Jiao; Bartolome Moya; Dhruvitkumar S Sutaria; Yinzhi Lang; Xun Tao; Weiguo Liu; Eunjeong Shin; Jieqiang Zhou; Carolin Werkman; Arnold Louie; George L Drusano; Jürgen B Bulitta
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