Combating highly resistant emerging pathogen Mycobacterium abscessus and Mycobacterium tuberculosis with novel salicylanilide esters and carbamates

Zsuzsa Baranyai; Martin Krátký; Jarmila Vinšová; Nóra Szabó; Zsuzsanna Senoner; Kata Horváti; Jiřina Stolaříková; Sándor Dávid; Szilvia Bősze

doi:10.1016/j.ejmech.2015.07.001

Combating highly resistant emerging pathogen Mycobacterium abscessus and Mycobacterium tuberculosis with novel salicylanilide esters and carbamates

Eur J Med Chem. 2015 Aug 28:101:692-704. doi: 10.1016/j.ejmech.2015.07.001. Epub 2015 Jul 7.

Authors

Zsuzsa Baranyai¹, Martin Krátký², Jarmila Vinšová³, Nóra Szabó⁴, Zsuzsanna Senoner⁵, Kata Horváti⁶, Jiřina Stolaříková⁷, Sándor Dávid⁸, Szilvia Bősze⁹

Affiliations

¹ MTA-ELTE Research Group of Peptide Chemistry, Pázmány Péter Sétány 1/A, Budapest, H-1117, Hungary, P.O. Box 32, 1518 Budapest 112, Hungary. Electronic address: baranyaizsuzs@gmail.com.
² Department of Inorganic and Organic Chemistry, Faculty of Pharmacy, Charles University, Heyrovského 1203, 500 05 Hradec Králové, Czech Republic. Electronic address: martin.kratky@faf.cuni.cz.
³ Department of Inorganic and Organic Chemistry, Faculty of Pharmacy, Charles University, Heyrovského 1203, 500 05 Hradec Králové, Czech Republic. Electronic address: jarmila.vinsova@faf.cuni.cz.
⁴ Laboratory of Bacteriology, Korányi National Institute for Tuberculosis and Respiratory Medicine, Pihenő út 1, Budapest H-1122, Hungary. Electronic address: nora.szabo@koranyi.hu.
⁵ Laboratory of Bacteriology, Korányi National Institute for Tuberculosis and Respiratory Medicine, Pihenő út 1, Budapest H-1122, Hungary.
⁶ MTA-ELTE Research Group of Peptide Chemistry, Pázmány Péter Sétány 1/A, Budapest, H-1117, Hungary, P.O. Box 32, 1518 Budapest 112, Hungary. Electronic address: khorvati@gmail.com.
⁷ Laboratory for Mycobacterial Diagnostics and Tuberculosis, Regional Institute of Public Health in Ostrava, Partyzánské Náměstí 7, 702 00 Ostrava, Czech Republic. Electronic address: jirina.stolarikova@zu.cz.
⁸ MTA-ELTE Research Group of Peptide Chemistry, Pázmány Péter Sétány 1/A, Budapest, H-1117, Hungary, P.O. Box 32, 1518 Budapest 112, Hungary; Laboratory of Bacteriology, Korányi National Institute for Tuberculosis and Respiratory Medicine, Pihenő út 1, Budapest H-1122, Hungary.
⁹ MTA-ELTE Research Group of Peptide Chemistry, Pázmány Péter Sétány 1/A, Budapest, H-1117, Hungary, P.O. Box 32, 1518 Budapest 112, Hungary. Electronic address: bosze@elte.hu.

PMID: 26210507
DOI: 10.1016/j.ejmech.2015.07.001

Abstract

In the Mycobacterium genus over one hundred species are already described and new ones are periodically reported. Species that form colonies in a week are classified as rapid growers, those requiring longer periods (up to three months) are the mostly pathogenic slow growers. More recently, new emerging species have been identified to lengthen the list, all rapid growers. Of these, Mycobacterium abscessus is also an intracellular pathogen and it is the most chemotherapy-resistant rapid-growing mycobacterium. In addition, the cases of multidrug-resistant Mycobacterium tuberculosis infection are also increasing. Therefore there is an urgent need to find new active molecules against these threatening strains. Based on previous results, a series of salicylanilides, salicylanilide 5-chloropyrazinoates and carbamates was designed, synthesized and characterised. The compounds were evaluated for their in vitro activity on M. abscessus, susceptible M. tuberculosis H37Rv, multidrug-resistant (MDR) M. tuberculosis MDR A8, M. tuberculosis MDR 9449/2006 and on the extremely-resistant Praha 131 (XDR) strains. All derivatives exhibited a significant activity with minimum inhibitory concentrations (MICs) in the low micromolar range. Eight salicylanilide carbamates and two salicylanilide esters exhibited an excellent in vitro activity on M. abscessus with MICs from 0.2 to 2.1 μM, thus being more effective than ciprofloxacin and gentamicin. This finding is potentially promising, particularly, as M. abscessus is a threateningly chemotherapy-resistant species. M. tuberculosis H37Rv was inhibited with MICs from 0.2 μM, and eleven compounds have lower MICs than isoniazid. Salicylanilide esters and carbamates were found that they were effective also on MDR and XDR M. tuberculosis strains with MICs ≥1.0 μM. The in vitro cytotoxicity (IC50) was also determined on human MonoMac-6 cells, and selectivity index (SI) of the compounds was established. In general, salicylanilide derivatives substituted by halogens on both salicyl and aniline rings showed better activity, than 4-benzoylaniline derivatives. The ester or carbamate bond formation of parent salicylanilides mostly retained or improved antimycobacterial potency with moderate selectivity.

Keywords: Antimycobacterial activity; Multidrug-resistant Mycobacterium tuberculosis; Mycobacterium abscessus; Salicylanilide; Salicylanilide 5-chloropyrazinoate; Salicylanilide carbamate.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Anti-Bacterial Agents / chemical synthesis
Anti-Bacterial Agents / chemistry
Anti-Bacterial Agents / pharmacology*
Carbamates / chemical synthesis
Carbamates / chemistry
Carbamates / pharmacology*
Cell Line
Dose-Response Relationship, Drug
Esters / chemical synthesis
Esters / chemistry
Esters / pharmacology*
Humans
Microbial Sensitivity Tests
Molecular Structure
Mycobacterium / classification
Mycobacterium / drug effects*
Salicylanilides / chemical synthesis
Salicylanilides / chemistry
Salicylanilides / pharmacology*
Structure-Activity Relationship
Tuberculosis, Multidrug-Resistant / microbiology*

Substances

Anti-Bacterial Agents
Carbamates
Esters
Salicylanilides
salicylanilide