AI Article Synopsis

  • Development of new anti-infectives is essential due to rising antibiotic resistance, focusing on the Mip protein as a target for inhibition in Gram-negative bacteria.
  • Inhibiting Mip has shown to reduce the virulence of various pathogens, prompting the creation of a library of Mip inhibitors.
  • The study details the metabolic transformation of these inhibitors using human liver microsomes, identifying active metabolites that could enhance future drug development.

Article Abstract

Due to increasing antibiotic resistance, the development of anti-infectives with new mechanisms of action is crucial. Virulence factors such as the "macrophage infectivity potentiator" (Mip) protein, which catalyzes the folding of proline-containing proteins by means of their cis-trans isomerase (PPIase) activity, have come into focus as a potential new target. Since the inhibition of Mip by small molecules has been shown to lead to reduced virulence and survival in vitro, especially of Gram-negative bacteria such as Burkholderia pseudomallei (Bp), Neisseria meningitidis (Nm), and Neisseria gonorrhoeae (Ng), or Coxiella burnetii (Cb), among many others, a library of Mip inhibitors was developed. As drug metabolism has a significant impact on the overall therapeutic outcome, this report describes the biotransformation of the most potent Mip inhibitors. Therefore, the anti-infectives were treated using human liver microsomes in vitro. Liquid chromatography with tandem mass spectrometry (LC/MS-MS) methods were applied to identify the metabolites and quantify the metabolic degradation of the hit compounds. Active metabolites, N-oxides, were found, leading to new opportunities for further drug development.

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http://dx.doi.org/10.1002/ardp.202400032DOI Listing

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