1. Synthesis, antimycobacterial activity and influence on mycobacterial InhA and PknB of 12-membered cyclodepsipeptides
- Author
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Katja Laqua, Linda Liebe, Melissa Richard-Greenblatt, Esther Pérez-Herrán, Ana Guardia, Tingting Huang, Adrian Richter, Peter Imming, Shuangjun Lin, Marcel Klemm, Yossef Av-Gay, and Lluis Ballell
- Subjects
0301 basic medicine ,Cell Survival ,medicine.drug_class ,Mycobacterium smegmatis ,Clinical Biochemistry ,Antitubercular Agents ,Pharmaceutical Science ,Microbial Sensitivity Tests ,Gram-Positive Bacteria ,Antimycobacterial ,01 natural sciences ,Biochemistry ,Mycobacterium tuberculosis ,03 medical and health sciences ,chemistry.chemical_compound ,Bacterial Proteins ,Cell Line, Tumor ,Depsipeptides ,Gram-Negative Bacteria ,Drug Discovery ,Human Umbilical Vein Endothelial Cells ,medicine ,Humans ,Molecular Biology ,Mycobacterium bovis ,biology ,010405 organic chemistry ,Chemistry ,INHA ,Organic Chemistry ,Isoniazid ,Autophosphorylation ,biology.organism_classification ,0104 chemical sciences ,030104 developmental biology ,Molecular Medicine ,Growth inhibition ,Oxidoreductases ,Proto-Oncogene Proteins c-akt ,medicine.drug - Abstract
In recent years, several small natural cyclopeptides and cyclodepsipeptides were reported to have antimycobacterial activity. Following this lead, a synthetic pathway was developed for a small series of 12-membered ring compounds with one amide and two ester bonds (cyclotridepsipeptides). Within the series, the ring system proved to be necessary for growth inhibition of Mycobacterium smegmatis and Mycobacterium tuberculosis in the low micromolar range. Open-chain precursors and analogues were inactive. The compounds modulated autophosphorylation of the mycobacterial protein kinase B (PknB). PknB inhibitors were active at µM concentration against mycobacteria while inducers were inactive. PknB regulates the activity of the mycobacterial reductase InhA, the target of isoniazid. The activity of the series against Mycobacterium bovis BCG InhA overexpressing strains was indistinguishable from that of the parental strain suggesting that they do not inhibit InhA. All substances were not cytotoxic (HeLa > 5 µg/ml) and did not show any significant antiproliferative effect (HUVEC > 5 µg/ml; K-562 > 5 µg/ml). Within the scope of this study, the molecular target of this new type of small cyclodepsipeptide was not identified, but the data suggest interaction with PknB or other kinases may partly cause the activity.
- Published
- 2018
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