Exquisite selectivity of griselimycin extends to beta subunit of DNA polymerases from Gram-negative bacterial pathogens.

Publication date: Dec 05, 2024

Griselimycin, a cyclic depsidecapeptide produced by Streptomyces griseus, is a promising lead inhibitor of the sliding clamp component of bacterial DNA polymerases (β-subunit of Escherichia coli DNA pol III). It was previously shown to inhibit the Mycobacterium tuberculosis β-clamp with remarkably high affinity and selectivity – the peptide lacks any interaction with the human sliding clamp. Here, we used a structural genomics approach to address the prospect of broader-spectrum inhibition, in particular of β-clamps from Gram-negative bacterial targets. Fifteen crystal structures of β-clamp orthologs were solved, most from Gram-negative bacteria, including eight cocrystal structures with griselimycin. The ensemble of structures samples widely diverse β-clamp architectures and reveals unique protein-ligand interactions with varying degrees of complementarity. Although griselimycin clearly co-evolved with Gram-positive β-clamps, binding affinity measurements demonstrate that the high selectivity observed previously extends to the Gram-negative orthologs, with K values ranging from 7 to 496 nM for the wild-type orthologs considered. The collective results should aid future structure-guided development of peptide antibiotics against β-clamp proteins of a wide variety of bacterial targets.

Open Access PDF

Concepts Keywords
Ligand Anti-Bacterial Agents
Mycobacterium Anti-Bacterial Agents
Polymerases Bacterial Proteins
Promising Bacterial Proteins
Tuberculosis Crystallography, X-Ray
DNA Polymerase III
DNA Polymerase III
Gram-Negative Bacteria
Models, Molecular

Semantics

Type Source Name
disease IDO bacteria
disease IDO protein
drug DRUGBANK Methionine
disease IDO replication
drug DRUGBANK Coenzyme M
drug DRUGBANK Pentaerythritol tetranitrate
disease MESH tuberculosis
pathway KEGG Tuberculosis
disease IDO site
disease IDO bactericidal
drug DRUGBANK L-Leucine
drug DRUGBANK L-Arginine
drug DRUGBANK Pirenzepine
drug DRUGBANK Oxygen
drug DRUGBANK Nitrogen
disease IDO disposition
drug DRUGBANK Water
disease IDO organism
drug DRUGBANK L-Alanine
drug DRUGBANK Glycerin
drug DRUGBANK Aspartame
drug DRUGBANK Dimethyl sulfoxide
drug DRUGBANK Iodide
drug DRUGBANK Formic Acid
drug DRUGBANK Imidazole
drug DRUGBANK Potassium
drug DRUGBANK Sodium acetate
drug DRUGBANK Sodium Chloride
drug DRUGBANK Sodium Citrate
drug DRUGBANK Sodium phosphate dibasic
drug DRUGBANK Bicine
drug DRUGBANK Tromethamine
drug DRUGBANK Polyethylene glycol

Original Article

Leave a Comment

Your email address will not be published. Required fields are marked *