Novel isoniazid derivative as promising antituberculosis agent

Author:

Volynets Galyna P1ORCID,Tukalo Michail A2ORCID,Bdzhola Volodymyr G1ORCID,Derkach Nataliia M3,Gumeniuk Mykola I3ORCID,Tarnavskiy Sergiy S1,Yarmoluk Sergiy M1

Affiliation:

1. Department of Medicinal Chemistry, Institute of Molecular Biology & Genetics, NAS of Ukraine, 150 Zabolotnogo St., Kyiv 03143, Ukraine

2. Department of Protein Synthesis Enzymology, Institute of Molecular Biology & Genetics, NAS of Ukraine, 150 Zabolotnogo St., Kyiv 03143, Ukraine

3. Department of Nonspecific Lung Diseases Treatment Technologies, National Institute of Phthisiology & Pulmonology named after F.G. Yanovsky NAMS of Ukraine, 10, M. Amosova Str., Kyiv 03038, Ukraine

Abstract

Background: A major focus of tuberculosis drug discovery is aimed at the development of novel antibiotics with activity against drug-resistant strains of Mycobacterium tuberculosis. Results: We have synthesized ten isoniazid derivatives and investigated for antibacterial activity toward M. tuberculosis H37Rv and isoniazid-resistant strain SRI 1369. It was revealed that only one compound, isonicotinic acid (1-methyl-1H-pyrrol-2-ylmethylene)-hydrazide (1), is active toward isoniazid-resistant strain with minimum inhibitory concentration value of 0.14 μM. This compound is not cytotoxic toward human liver cells (HepG2; IC50 >100 μM), demonstrates good permeability in Caco-2 cells. Accordingly to the results of plasma protein binding assay, unbound fraction of compound 1, which potentially exhibits pharmacologic effects, is 57.9%. Conclusion: Therefore, isonicotinic acid (1-methyl-1H-pyrrol-2-ylmethylene)-hydrazide is a promising compound for further preclinical studies.

Publisher

Future Medicine Ltd

Subject

Microbiology (medical),Microbiology

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