In Vitro and In Vivo Activities of Macrolide Derivatives against
            <i>Mycobacterium tuberculosis</i>

Falzari, Kanakeshwari; Zhu, Zhaohai; Pan, Dahua; Liu, Huiwen; Hongmanee, Poonpilas; Franzblau, Scott G.

doi:10.1128/aac.49.4.1447-1454.2005

Cited by 202 publications

(252 citation statements)

References 26 publications

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“…To provide further proof-of-principle data to support the notion that specific inhibitors of mPTPB may be effective antiTB agents, we tested I-A09 against the classical Mtb Erdman strain in a model of active TB infection performed in a mouse macrophage J774A.1 cell line (32). Cultures of macrophages infected with actively growing Mtb were treated with 10 μM I-A09 starting on Day 0 and the cultures were allowed to incubate for a further seven days before assessment of the remaining bacterial load in the cells (Fig.…”

Section: Resultsmentioning

confidence: 99%

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Targeting mycobacterium protein tyrosine phosphatase B for antituberculosis agents

Zhou¹,

He²,

Zhang

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

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Protein tyrosine phosphatases are often exploited and subverted by pathogenic bacteria to cause human diseases. The tyrosine phosphatase mPTPB from Mycobacterium tuberculosis is an essential virulence factor that is secreted by the bacterium into the cytoplasm of macrophages, where it mediates mycobacterial survival in the host. Consequently, there is considerable interest in understanding the mechanism by which mPTPB evades the host immune responses, and in developing potent and selective mPTPB inhibitors as unique antituberculosis (antiTB) agents. We uncovered that mPTPB subverts the innate immune responses by blocking the ERK1/2 and p38 mediated IL-6 production and promoting host cell survival by activating the Akt pathway. We identified a potent and selective mPTPB inhibitor I-A09 with highly efficacious cellular activity, from a combinatorial library of bidentate benzofuran salicylic acid derivatives assembled by click chemistry. We demonstrated that inhibition of mPTPB with I-A09 in macrophages reverses the altered host immune responses induced by the bacterial phosphatase and prevents TB growth in host cells. The results provide the necessary proof-of-principle data to support the notion that specific inhibitors of the mPTPB may serve as effective antiTB therapeutics.combinatorial chemistry | pathogen-host interaction | phosphatase inhibitor | signaling mechanism

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Section: Resultsmentioning

confidence: 99%

“…Inhibition of growth of M. tuberculosis Erdman (ATCC 35801) in a macrophage cell culture was assessed as previously described (32). J774A.1 cells were grown to confluency in 75 cm 2 cell culture flasks in DMEM medium containing 10% FBS.…”

Section: Methodsmentioning

confidence: 99%

Targeting mycobacterium protein tyrosine phosphatase B for antituberculosis agents

Zhou¹,

He²,

Zhang

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

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223

205

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“…As expected, the evaluation of MBCs against Mtb H 37 Rv (Table 2) showed that the 6-hydrogenquinolones, like clinical FQs, are bactericidal and kill Mtb at concentrations close to those that cause inhibition. Finally, all the compounds resulted to be not toxic against Vero cells (26) at the concentration tested of 102 lM.…”

Section: Mycobacterium Tuberculosis Inhibitory Activitymentioning

confidence: 99%

“…Similarly, cytotoxicities were determined on Vero cells according to a published procedure (26). The MBC was determined for Mtb H 37 Rv by subculturing onto a drug-free solid medium and counting of CFU following exposure in Middlebrook 7H9 medium supplemented with drug concentrations equivalent to and higher than the previously determined MICs against the same strains.…”

Section: Biologic Evaluationmentioning

confidence: 99%

6‐Hydrogen‐8‐Methylquinolones Active Against Replicating and Non‐replicating Mycobacterium tuberculosis

et al. 2012

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The screening of an in-house quinolones library against Mycobacterium tuberculosis (Mtb) H 37 Rv, followed by a first cycle of optimization, yielded 6-hydrogen-8-methyl derivatives endowed with good potency. The antitubercular activity also encompassed the bacteria in a non-replicating state (NRP-TB) with minimum inhibitory concentration values lower than those of the reference agent, moxifloxacin. Among the best compounds, 11w and 11ai, characterized by a properly substituted piperidine at the C-7 position, were active against single-drug-resistant (SDR-TB) Mtb strains, maintaining overall good potency also against ciprofloxacin-resistant Mtb. This study expands the body of SAR around antitubercular quinolones leading to reconsider the role played by the usual fluorine atom at the C-6 position. Further elaboration of the 6-hydrogen-8-methylquinolone scaffold, with a particular focus on the C-7 position, is expected to give even more potent congeners holding promise for shortening the current anti-TB regimen.Key words: 6-desfluoroquinolones, antitubercular agents, multidrug resistance, non-replicating bacteria, quinolone SAR Abbreviations: 6-DFQs, 6-desfluoroquinolones; CipR, ciprofloxacinresistant; DOTS, Directly Observed Therapy Short-course; EMB, ethambutol; FQs, fluoroquinolones; INH, isoniazid; LORA, low oxygen recovery assay; MABA, microplate Alamar Blue assay; MBC, minimum bactericidal concentration; MDR-TB, multidrug-resistant Mtb; MIC, minimum inhibitory concentration; Mtb, Mycobacterium tuberculosis; NCEs, new chemical entities; NRP-TB, non-replicating persistent Mtb; PZA, pyrazinamide; RMP, rifampin; SAR, structure-activity relationships; SDR-TB, single-drugresistant Mtb; TB, tuberculosis; XDR-TB, extensively drug-resistant Mtb.Received 3 May 2012, revised 31 July 2012 and accepted for publication 2 August 2012 Tuberculosis (TB) is an old and re-emerging disease that spreads at alarming rate. Mycobacterium tuberculosis (Mtb) is responsible for 8.8 million new active cases and 1.5 million deaths in 2010, and one-third of the world's population is estimated to be latently infected with TB. About 95% of the tuberculosis cases and deaths occur in the developing countries, but there has also been a recent, highly publicized, resurgence of TB also in developed ones.a This pandemic is complicated by the co-infection with HIV (15% of new cases worldwide are HIV positive) and the emergence of multidrug-resistant (MDR-TB) and extensively drug-resistant (XDR-TB) Mtb strains.b The current recommended therapeutic strategy, namely Directly Observed Therapy, Short-course (DOTS) is based on the co-administration of four drugs, namely rifampin (RMP), isoniazid (INH), pyrazinamide (PZA), and ethambutol (EMB) for 2 months, followed by a prolonged treatment with INH and RMP for an additional 4-7 months.c The cause of the long-period treatment is the peculiar ability of Mtb to survive in a non-replicating persistent (NRP-TB) state while withstanding chemotherapy. These features highlight the need to develop well-tolerated...

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“…Substitutions of C1401A/T or G1483T led to kanamycin resistance (6). Mycobacteria belonging to M. tuberculosis complex have intrinsic resistance to macrolides (7,8). The resistance has been attributed to erm genes, which are 23 S rRNA methyltransferases (9).…”

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confidence: 99%

Structural and Functional Characterization of Rv2966c Protein Reveals an RsmD-like Methyltransferase from Mycobacterium tuberculosis and the Role of Its N-terminal Domain in Target Recognition

Kumar

Saigal²,

Malhotra³

et al. 2011

Journal of Biological Chemistry

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In Vitro and In Vivo Activities of Macrolide Derivatives against Mycobacterium tuberculosis

Cited by 202 publications

References 26 publications

Targeting mycobacterium protein tyrosine phosphatase B for antituberculosis agents

Targeting mycobacterium protein tyrosine phosphatase B for antituberculosis agents

6‐Hydrogen‐8‐Methylquinolones Active Against Replicating and Non‐replicating Mycobacterium tuberculosis

Structural and Functional Characterization of Rv2966c Protein Reveals an RsmD-like Methyltransferase from Mycobacterium tuberculosis and the Role of Its N-terminal Domain in Target Recognition

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