Asha B. Thomas, Manjiri D. Bhosale, K. Lokhande, Kakumani VenkateswaraSwamy, Soumya Basu, S. Chitlange
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The molecular docking performed using FlexX indicated compounds IIb5 (1-(R)-(4-hydroxyphenyl)(4-methylpiperazin-1-yl)methyl)-3-((S)-(4-hydroxyphenyl)(4-methylpiperazin-1-yl)methyl)urea and IIc5 ((1-(R)-(4-hydroxyphenyl)(4-methylpiperazin-1-yl)methyl)-3-((S)-(4-hydroxyphenyl)(4-methylpiperazin-1-yl)methyl) thiourea to exhibit promising binding affinity (dock score of -15.01 and -13.77) when compared to the reference MFX moxifloxacin (dock score -4.40) with the target 5BS8 (DNA gyrase). Further, the best 10 compounds were synthesized by one-pot synthesis employing the reaction of indole/N-methyl piperazine/piperidine/pyrrolidine with N-substituted benzaldehydes in the presence of acetamide/urea/thiourea to afford the compounds in 54.60% to 85.47% yield. The synthesized compounds were suitably characterized using chromatographic and spectroscopic tools.\n\n\n\nIn the microplate Alamar Blue assay (MABA), compounds IIb1, IIIc2, IIIb1, and IIb5 exhibited good minimum inhibitory concentrations of 1.6µg/mL, 3.12µg/mL, and 12.5µg/mL, respectively, when compared to the standard rifampicin with 0.8µg/mL inhibitory concentration. The MTB gyrase supercoiling assay performed using Mycobacterium tuberculosis gyrase supercoiling assay kit demonstrated compound IIb5 at a concentration of 300µg/mL to show gyrase inhibition in comparison to MFX at 60 µg/mL. In the MTT assay performed using the human breast cancer cell line MCF-7, compounds IIc2, IIb5, and IIb1 showed IC50 values of 2.57µM, 12.54µM, and 12.75µM, respectively, compared to doxorubicin (1.10µM) at 7-48hrs and 72hrs of the study.\n\n\n\nBased on these observations, N-methyl piperazine class of compounds can serve as a lead/pharmacophore for the rational design of potent molecules against MTB gyrase to combat the growing issue of MDR-TB.\n","PeriodicalId":18063,"journal":{"name":"Letters in Drug Design & Discovery","volume":null,"pages":null},"PeriodicalIF":0.0000,"publicationDate":"2023-05-23","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Design, docking, synthesis, and in vitro evaluation of potent anti-tubercular agents targeting DNA Gyrase\",\"authors\":\"Asha B. Thomas, Manjiri D. Bhosale, K. Lokhande, Kakumani VenkateswaraSwamy, Soumya Basu, S. 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引用次数: 0
摘要
据报道,由结核分枝杆菌引起的结核病感染了全球约三分之二的人口,并不断产生多药耐药性。DNA回转酶是一种II型拓扑异构酶,是喹诺酮类药物治疗结核病的一个有希望的靶点。目前的研究重点是设计和合成新的含吲哚、n-甲基哌嗪、哌啶和吡咯烷环结构的氮杂环化合物,初步设计的化合物对DNA旋切酶靶点的亲和力进行了评估。使用FlexX进行的分子对接表明,化合物IIb5 (1-(R)-(4-羟基苯基)(4-甲基哌嗪-1-基)甲基尿素和IIc5 ((1-(R)-(4-羟基苯基)(4-甲基哌嗪-1-基)甲基)-3-((S)-(4-羟基苯基)(4-甲基哌嗪-1-基)甲基)硫脲与靶标5BS8 (DNA旋切酶)的结合亲和力较参比MFX莫西沙星(对接评分-4.40)为-15.01和-13.77。以吲哚/ n -甲基哌嗪/哌啶/吡咯烷为原料,在乙酰胺/尿素/硫脲的存在下,以n -取代苯甲醛为原料,采用一锅法合成了最佳的10个化合物,收率为54.60% ~ 85.47%。用色谱和光谱工具对合成的化合物进行了表征。在微孔板Alamar Blue assay (MABA)中,化合物IIb1、IIIc2、IIIb1和IIb5的最低抑制浓度分别为1.6µg/mL、3.12µg/mL和12.5µg/mL,而标准利福平的抑制浓度为0.8µg/mL。使用结核分枝杆菌旋转酶超缠绕检测试剂盒进行的MTB旋转酶超缠绕试验表明,与浓度为60 μ g/mL的MFX相比,浓度为300 μ g/mL的化合物IIb5显示出旋转酶抑制作用。在使用人乳腺癌细胞系MCF-7进行的MTT试验中,化合物IIc2、IIb5和IIb1在研究开始7-48小时和72小时时的IC50值分别为2.57µM、12.54µM和12.75µM,而阿霉素的IC50值为1.10µM。基于这些观察结果,n -甲基哌嗪类化合物可作为先导/药效团,用于合理设计抗MTB回旋酶的有效分子,以对抗日益严重的耐多药结核病问题。
Design, docking, synthesis, and in vitro evaluation of potent anti-tubercular agents targeting DNA Gyrase
Tuberculosis caused by Mycobacterium tuberculosis has been reported to infect about two-third of the global population and to continuously develop multidrug resistance. DNA gyrase, a type II topoisomerase, is a promising target of the quinolone class of drugs in the treatment of tuberculosis.
The present study is focused on the design and synthesis of newer nitrogen heterocyclics containing indole, n-methyl piperazine, piperidine, and pyrrolidine ring structures
Initially designed compounds were evaluated for their affinity to the DNA gyrase target. The molecular docking performed using FlexX indicated compounds IIb5 (1-(R)-(4-hydroxyphenyl)(4-methylpiperazin-1-yl)methyl)-3-((S)-(4-hydroxyphenyl)(4-methylpiperazin-1-yl)methyl)urea and IIc5 ((1-(R)-(4-hydroxyphenyl)(4-methylpiperazin-1-yl)methyl)-3-((S)-(4-hydroxyphenyl)(4-methylpiperazin-1-yl)methyl) thiourea to exhibit promising binding affinity (dock score of -15.01 and -13.77) when compared to the reference MFX moxifloxacin (dock score -4.40) with the target 5BS8 (DNA gyrase). Further, the best 10 compounds were synthesized by one-pot synthesis employing the reaction of indole/N-methyl piperazine/piperidine/pyrrolidine with N-substituted benzaldehydes in the presence of acetamide/urea/thiourea to afford the compounds in 54.60% to 85.47% yield. The synthesized compounds were suitably characterized using chromatographic and spectroscopic tools.
In the microplate Alamar Blue assay (MABA), compounds IIb1, IIIc2, IIIb1, and IIb5 exhibited good minimum inhibitory concentrations of 1.6µg/mL, 3.12µg/mL, and 12.5µg/mL, respectively, when compared to the standard rifampicin with 0.8µg/mL inhibitory concentration. The MTB gyrase supercoiling assay performed using Mycobacterium tuberculosis gyrase supercoiling assay kit demonstrated compound IIb5 at a concentration of 300µg/mL to show gyrase inhibition in comparison to MFX at 60 µg/mL. In the MTT assay performed using the human breast cancer cell line MCF-7, compounds IIc2, IIb5, and IIb1 showed IC50 values of 2.57µM, 12.54µM, and 12.75µM, respectively, compared to doxorubicin (1.10µM) at 7-48hrs and 72hrs of the study.
Based on these observations, N-methyl piperazine class of compounds can serve as a lead/pharmacophore for the rational design of potent molecules against MTB gyrase to combat the growing issue of MDR-TB.
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