Thiazolopyridine Ureas as Novel Antitubercular Agents Acting through Inhibition of DNA Gyrase B

Kale, Manoj; Raichurkar, Anandkumar; P, Shahul Hameed; Waterson, David; McKinney, David C.; Manjunatha, M; Kranthi, Usha; Koushik, Krishna; Jena, Lalit Kumar; Shinde, Vikas; Rudrapatna, Suresh; Barde, Shubhada; Humnabadkar, Vaishali; Madhavapeddi, Prashanti; Basavarajappa, Halesha D.; Ghosh, Anirban; Ramya, V.; Guptha, Supreeth; Sharma, Sreevalli; Vachaspati, Prakash; Kumar, Kunal; Giridhar, Jayashree; Reddy, Jitendar; Panduga, Vijender; Ganguly, Samit; Ahuja, Vijay Kamal; Gaonkar, Sheshagiri; Kumar, C. N. Naveen; Ogg, D.; Tucker, J.A.; Boriack-Sjodin, P.A.; Sousa, Sunita M. de; Sambandamurthy, Vasan K.; Ghorpade, Sandeep R.

doi:10.1021/jm401268f

Cited by 58 publications

(43 citation statements)

References 24 publications

(37 reference statements)

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“…The catalytic subunits (GyrA/ParC) are clinically validated drug targets of the fluoroquinolones, such as moxifloxacin (MXF) (2), while the ATPase subunits (GyrB/ParE) have not been as extensively exploited and may present a new option for treating DR strains of M. tuberculosis (3). Furthermore, several different chemical classes have been described as inhibitors of gyrase B with potent activity against DR bacteria, including M. tuberculosis (4)(5)(6)(7)(8)(9)(10).…”

mentioning

confidence: 99%

A Novel Inhibitor of Gyrase B Is a Potent Drug Candidate for Treatment of Tuberculosis and Nontuberculosis Mycobacterial Infections

Locher

Jones

Hanzelka

et al. 2015

Antimicrob Agents Chemother

101

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dNew drugs to treat drug-resistant tuberculosis are urgently needed. Extensively drug-resistant and probably the totally drugresistant tuberculosis strains are resistant to fluoroquinolones like moxifloxacin, which target gyrase A, and most people infected with these strains die within a year. In this study, we found that a novel aminobenzimidazole, VXc-486, which targets gyrase B, potently inhibits multiple drug-sensitive isolates and drug-resistant isolates of Mycobacterium tuberculosis in vitro (MICs of 0.03 to 0.30 g/ml and 0.08 to 5.48 g/ml, respectively) and reduces mycobacterial burdens in lungs of infected mice in vivo. VXc-486 is active against drug-resistant isolates, has bactericidal activity, and kills intracellular and dormant M. tuberculosis bacteria in a low-oxygen environment. Furthermore, we found that VXc-486 inhibits the growth of multiple strains of Mycobacterium abscessus, Mycobacterium avium complex, and Mycobacterium kansasii (MICs of 0.1 to 2.0 g/ml), as well as that of several strains of Nocardia spp. (MICs of 0.1 to 1.0 g/ml). We made a direct comparison of the parent compound VXc-486 and a phosphate prodrug of VXc-486 and showed that the prodrug of VXc-486 had more potent killing of M. tuberculosis than did VXc-486 in vivo. In combination with other antimycobacterial drugs, the prodrug of VXc-486 sterilized M. tuberculosis infection when combined with rifapentine-pyrazinamide and bedaquiline-pyrazinamide in a relapse infection study in mice. Furthermore, the prodrug of VXc-486 appeared to perform at least as well as the gyrase A inhibitor moxifloxacin. These findings warrant further development of the prodrug of VXc-486 for the treatment of tuberculosis and nontuberculosis mycobacterial infections.

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mentioning

confidence: 99%

A Novel Inhibitor of Gyrase B Is a Potent Drug Candidate for Treatment of Tuberculosis and Nontuberculosis Mycobacterial Infections

Locher

Jones

Hanzelka

et al. 2015

Antimicrob Agents Chemother

101

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“…Além disso, a atividade biológica de diversos heterociclicos já foram descritos como sendo ativos contra a subunidade GyrB, como por exemplo derivados de cumarina, benzimidazol uréia, pirazol, indazol e indolinona. 110,111 Utilizando inibidores de GyrB identificados previamente, foram sintetizados 26 derivados do etil 5-(piperazina-1-il) benzofurano-2--carboxilato, que foram avaliados contra cepas de MTB H 37 Rv. O composto 41 se apresentou como o mais promissor da série, exibindo uma CIM 90 de 9.18 μmol L -1 .…”

Section: Dna Girase E Topoisomerase Iunclassified

“…Estudos in vivo utilizando camundongos com infecção aguda de tuberculose revelaram ação bactericida deste composto em dois diferentes regimes de administração oral (300 mg kg -1 uma vez ao dia ou 150 mg kg -1 duas vezes ao dia) durante 10 dias. 111 Esses resultados sugerem a importância da subunidade GyrB como potencial alvo terapêutico a ser explorado no desenvolvimento de fármacos antituberculose.…”

Section: Dna Girase E Topoisomerase Iunclassified

Potenciais alvos moleculares para o desenvolvimento de novos fármacos antituberculose

2017

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POTENTIAL MOLECULAR TARGETS FOR ANTITUBERCULOSIS DRUG DISCOVERY. Tuberculosis (TB) is an infectious disease caused by mycobacteria from the Mycobacterium genus, mainly by Mycobacterium tuberculosis (MTB). The World HealthOrganization (WHO) aims to reduce the number of TB cases worldwide in the coming years. Nevertheless, the increasing number of multidrug-resistant (MDR-TB) and extensive-drug resistance (XDR-TB) strains, and the ineffectiveness of the current treatment in latent tuberculosis are challenges to be overcome. In this review, we will demonstrate the recent advances in the tuberculosis drug discovery, focusing the research of new molecular targets in the Mycobacterium tuberculosis. Among the promising targets described herein, we highlight those, which act in different pathways in the mycobacteria, such as energy metabolism, cell wall biosynthesis, DNA synthesis, iron metabolism and transport through membranes. Furthermore, bioactive compounds discovered using phenotypic assays screening and validated through genetic approaches are also presented.Keywords: medicinal chemistry; tuberculosis; Mycobacterium tuberculosis; molecular targets; new drugs. INTRODUÇÃOA tuberculose (TB) é uma doença infecciosa causada por micobactérias do complexo Mycobacterium, no entanto, a espécie responsável pelo maior número de casos de morbidade e mortalidade é o Mycobacterium tuberculosis (MTB). 1 Ocupando o ranking mundial como a principal causa de mortes causadas por doenças infecciosas, nos últimos anos a tuberculose ultrapassou, em número de casos, a infecção causada pelo vírus da imunodeficiência humana (HIV). 2,3 O último levantamento realizado em 2015 pela Organização Mundial da Saúde (OMS) apontou 9.6 milhões de novos casos no mundo e 1.5 milhões de mortes causadas pela doença. 3 Somado a esses dados, o surgimento e aumento de cepas de M. tuberculosis multirresistente aos fármacos (MDR-TB) e extensivamente resistente aos fármacos (XDR-TB) vêm alarmando as autoridades de todo o mundo. Essas formas de tuberculose apresentam baixas taxas de cura e maiores taxas de mortalidade devido às dificuldades de tratamento. 4 Além disso, já foram relatados na clínica casos de tuberculose totalmente resistente aos fármacos (TDR-TB). 5,6 Ao longo dos últimos anos, é possível constatar algumas evoluções no desenvolvimento de compostos candidatos a fármacos que possam atuar contra a TB. 7 Após um intervalo de mais de 50 anos sem novos medicamentos para o tratamento da TB, a bedaquilina foi aprovada em 2012 pela agência norte-americana U.S. Food and Drug Administration (FDA) para o tratamento de MDR-TB. Atualmente, diversos candidatos a fármacos estão em estudos clínicos, [8][9][10][11][12] 39 Atualmente, diversos métodos e estratégias são utilizados para o desenvolvimento de novos fármacos contra a TB, como por exemplo: 1) abordagens genéticas para identificação de novos alvos; 2) ensaios de triagem em larga escala utilizando a micobactéria como plataforma; 3) ferramentas de biologia estrutural e triagem virtual e; 4) modificações ...

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“…Inhibitor of gyrB subunit competitively inhibits the ATPase activity conferred by the DNA gyrB subunit and thereby abolishes the energydependent reactions catalyzed by DNA gyrase . [15][16][17][18][19][20] In the present study, we explore a new class of DNA gyrase inhibitor derived from the medium throughput screening (MTS) of BITS-Pilani in house chemical library using the relatively underexploited gyrase ATPase domain as the template. The hit obtained was further customized using medicinal chemistry strategies to obtain a lead molecule displaying considerable in vitro enzyme efficacy and anti-mycobacterial potency against MTB H3Rv strain.…”

Section: Introductionmentioning

confidence: 99%

Exploring the gyrase ATPase domain for tailoring newer anti-tubercular drugs: Hit to lead optimization of a novel class of thiazole inhibitors

Jeankumar

Kotagiri

Renuka

et al. 2015

Bioorganic & Medicinal Chemistry

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Thiazolopyridine Ureas as Novel Antitubercular Agents Acting through Inhibition of DNA Gyrase B

Cited by 58 publications

References 24 publications

A Novel Inhibitor of Gyrase B Is a Potent Drug Candidate for Treatment of Tuberculosis and Nontuberculosis Mycobacterial Infections

A Novel Inhibitor of Gyrase B Is a Potent Drug Candidate for Treatment of Tuberculosis and Nontuberculosis Mycobacterial Infections

Potenciais alvos moleculares para o desenvolvimento de novos fármacos antituberculose

Exploring the gyrase ATPase domain for tailoring newer anti-tubercular drugs: Hit to lead optimization of a novel class of thiazole inhibitors

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