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  4. Full Profiling of GE81112A, an Underexplored Tetrapeptide Antibiotic with Activity against Gram-Negative Pathogens
 
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2023
Journal Article
Title

Full Profiling of GE81112A, an Underexplored Tetrapeptide Antibiotic with Activity against Gram-Negative Pathogens

Abstract
After the first total synthesis combined with structure revision, we performed thorough in vitro and in vivo profiling of the underexplored tetrapeptide GE81112A. From the determination of the biological activity spectrum and physicochemical and early absorption-distribution-metabolism-excretion-toxicity (eADMET) properties, as well as in vivo data regarding tolerability and pharmacokinetics (PK) in mice and efficacy in an Escherichia coli-induced septicemia model, we were able to identify the critical and limiting parameters of the original hit compound. Thus, the generated data will serve as the basis for further compound optimization programs and developability assessments to identify candidates for preclinical/clinical development derived from GE81112A as the lead structure. IMPORTANCE The spread of antimicrobial resistance (AMR) is becoming a more and more important global threat to human health. With regard to current medical needs, penetration into the site of infection represents the major challenge in the treatment of infections caused by Gram-positive bacteria. Considering infections associated with Gram-negative bacteria, resistance is a major issue. Obviously, novel scaffolds for the design of new antibacterials in this arena are urgently needed to overcome this crisis. Such a novel potential lead structure is represented by the GE81112 compounds, which inhibit protein synthesis by interacting with the small 30S ribosomal subunit using a binding site distinct from that of other known ribosome-targeting antibiotics. Therefore, the tetrapeptide antibiotic GE81112A was chosen for further exploration as a potential lead for the development of antibiotics with a new mode of action against Gram-negative bacteria.
Author(s)
Schuler, Sören M.M.
Fraunhofer-Institut für Molekularbiologie und Angewandte Oekologie IME  
Jürjens, Gerrit
Fraunhofer-Institut für Molekularbiologie und Angewandte Oekologie IME  
Marker, Alexander
Hemmann, Ulrike
Rey, Astrid
Yvon, Stéphane
Lagrevol, Marjorie
Hamiti, Mohamed
Nguyen, Fabian
Hirsch, Rolf
Fraunhofer-Institut für Molekularbiologie und Angewandte Oekologie IME  
Pöverlein, Christoph
Vilcinskas, Andreas  
Fraunhofer-Institut für Molekularbiologie und Angewandte Oekologie IME  
Hammann, Peter Eugen
Wilson, Daniel N.
Mourez, Michäel
Coyne, Sébastien
Bauer, Armin
Journal
Microbiology spectrum  
Open Access
DOI
10.1128/spectrum.02247-22
Additional link
Full text
Language
English
Fraunhofer-Institut für Molekularbiologie und Angewandte Oekologie IME  
Keyword(s)
  • antibiotic

  • GE81112A

  • profiling

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