Your search keyword '"Panduga V"' showing total 20 results

1. A drug-drug interaction study and physiologically based pharmacokinetic modelling to assess the effect of an oral 5-lipoxygenase activating protein inhibitor on the pharmacokinetics of oral midazolam.

Author

Knöchel J, Panduga V, Nelander K, Heijer M, Lindstedt EL, Ali H, Aurell M, Ödesjö H, Forte P, Connolly K, Ericsson H, and MacPhee I

Subjects

Humans, Male, Adult, Young Adult, Administration, Oral, Area Under Curve, Cytochrome P-450 CYP3A Inhibitors pharmacology, Cytochrome P-450 CYP3A Inhibitors pharmacokinetics, Dose-Response Relationship, Drug, Midazolam pharmacokinetics, Midazolam administration & dosage, Drug Interactions, Cytochrome P-450 CYP3A metabolism, Models, Biological

Abstract

Aims: Early clinical studies have indicated that the pharmacokinetics of Atuliflapon (AZD5718) are time and dose dependent. The reason(s) for these findings is(are) not fully understood, but pre-clinical profiling suggests that time-dependent CYP3A4 inhibition cannot be excluded. In clinical practice, Atuliflapon will be co-administered with CYP3A4 substrates; thus, it is important to determine the impact of Atuliflapon on the pharmacokinetics (PK) of CYP3A4 substrates. The aim of this study was to evaluate the effect of Atuliflapon on the pharmacokinetics of a sensitive CYP3A4 substrate, midazolam, and to explore if the time-/dose-dependent effect seen after repeated dosing could be an effect of change in CYP3A4 activity., Methods: Open-label, fixed-sequence study in healthy volunteers to assess the PK of midazolam alone and in combination with Atuliflapon. Fourteen healthy male subjects received single oral dose of midazolam 2 mg on days 1 and 7 and single oral doses of Atuliflapon (125 mg) from days 2 to 7. A physiologically based pharmacokinetic (PBPK) model was developed to assess this drug-drug interaction., Results: Mean midazolam values of maximum plasma concentration (C max ) and area under the curve (AUC) to infinity were increased by 39% and 56%, respectively, when co-administered with Atuliflapon vs. midazolam alone. The PBPK model predicted a 27% and 44% increase in AUC and a 23% and 35% increase in C max of midazolam following its co-administrations with two predicted therapeutically relevant doses of Atuliflapon., Conclusions: Atuliflapon is a weak inhibitor of CYP3A4; this was confirmed by the validated PBPK model. This weak inhibition is predicted to have a minor PK effect on CYP3A4 metabolized drugs., (© 2024 AstraZeneca. British Journal of Clinical Pharmacology published by John Wiley & Sons Ltd on behalf of British Pharmacological Society.)

Published

2024

2. Scaffold Morphing To Identify Novel DprE1 Inhibitors with Antimycobacterial Activity.

Author

R MM, Shandil R, Panda M, Sadler C, Ambady A, Panduga V, Kumar N, Mahadevaswamy J, Sreenivasaiah M, Narayan A, Guptha S, Sharma S, Sambandamurthy VK, Ramachandran V, Mallya M, Cooper C, Mdluli K, Butler S, Tommasi R, Iyer PS, Narayanan S, Chatterji M, and Shirude PS

Abstract

We report a novel benzimidazole (BI) based DprE1 inhibitor that resulted from scaffold morphing of a 1,4-azaindole series. The clinical progression of the 1,4-azaindole series from our previous work validates the potential of exploring newer chemical entities with antimycobacterial activity driven via a noncovalent inhibition of the decaprenylphosphoryl-β-d-ribose-2'-epimerase (DprE1). The representative compounds from the new scaffold reported in this study exhibited an improved solubility and higher free plasma fraction, while retaining potent DprE1 inhibition and antimycobacterial activity. A representative compound from the benzimidazole series demonstrated good efficacy in a murine model of tuberculosis. Furthermore, molecular modeling of the BI scaffold suggests plausible modes of binding in the active site of DprE1 enzyme from Mycobacterium tuberculosis that can be used for further exploration of the series., Competing Interests: The authors declare no competing financial interest., (Copyright © 2019 American Chemical Society.)

Published

2019

3. Evaluation of the metabolism, bioactivation and pharmacokinetics of triaminopyrimidine analogs toward selection of a potential candidate for antimalarial therapy.

Author

Srivastava A, Panduga V, Saralaya R, K R P, Hameed S, Solapure S, and Hosagrahara VP

Subjects

Acetylcysteine metabolism, Animals, Bile metabolism, Biotransformation, Glutathione metabolism, Humans, Microsomes, Liver metabolism, Quinones, Rats, Sulfhydryl Compounds metabolism, Antimalarials metabolism

Abstract

1. During the course of metabolic profiling of lead Compound 1, glutathione (GSH) conjugates were detected in rat bile, suggesting the formation of reactive intermediate precursor(s). This was confirmed by the identification of GSH and N-acetylcysteine (NAC) conjugates in microsomal incubations. 2. It was proposed that bioactivation of Compound 1 occurs via the formation of a di-iminoquinone reactive intermediate through the involvement of the C-2 and C-5 nitrogens of the pyrimidine core. 3. To further investigate this hypothesis, structural analogs with modifications at the C-5 nitrogen were studied for metabolic activation in human liver microsomes supplemented with GSH/NAC. 4. Compounds 1 and 2, which bear secondary nitrogens at the C-5 of the pyrimidine core, were observed to form significant amounts of GSH/NAC-conjugates in vitro, whereas compounds with tertiary nitrogens at C-5 (Compound 3 and 4) formed no such conjugates. 5. These observations provide evidence that electron/hydrogen abstraction is required for the bioactivation of the triaminopyrimidines, potentially via a di-iminoquinone intermediate. The lack of a hydrogen and/or steric hindrance rendered Compound 3 and 4 incapable of forming thiol conjugates. 6. This finding enabled advancement of compound 4, with a desirable potency, safety and PK profile, as a lead candidate for further development in the treatment of malaria.

Published

2017

4. Ipratropium is 'luminally recycled' by an inter-play between apical uptake and efflux transporters in Calu-3 bronchial epithelial cell layers.

Author

Panduga V, Stocks MJ, and Bosquillon C

Subjects

Biological Transport, Cell Line, Tumor, Dextrans pharmacology, Drug Liberation, Fluorescein-5-isothiocyanate analogs & derivatives, Fluorescein-5-isothiocyanate pharmacology, Glycopyrrolate pharmacology, Humans, Tiotropium Bromide pharmacology, Bronchi cytology, Bronchodilator Agents pharmacology, Cholinergic Antagonists pharmacology, Epithelial Cells metabolism, Ipratropium pharmacology

Abstract

The mechanism by which quaternized anticholinergic bronchodilators permeate the airway epithelium remains controversial to date. In order to elucidate the role of drug transporters, ipratropium bidirectional transport as well as accumulation and release studies were performed in layers of the broncho-epithelial cell line Calu-3 grown at an air-liquid interface, in presence or absence of a range of transporter inhibitors. Unexpectedly, a higher transepithelial permeability was observed in the secretory direction, with an apparent efflux ratio of > 4. Concentration-dependent and inhibitor studies demonstrated the drug intracellular uptake was carrier-mediated. Interestingly, monitoring drug release post cell loading revealed the presence of an efficient efflux system on the apical side of the cell layers. Acting in concert, apical transporters seem to promote the 'luminal recycling' of the drug and hence, limit its transcellular transport. The data are in agreement with an apical Organic Cation Transporter (OCT) being involved in this process but also suggest the participation of unknown uptake and efflux transporters sensitive to probenecid. This study suggests the absorption of ipratropium across the pulmonary barrier is primarily governed by paracellular passive diffusion but transporters might play a significant role in controlling the drug local concentrations in the lungs., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

5. Discovery of Imidazo[1,2-a]pyridine Ethers and Squaramides as Selective and Potent Inhibitors of Mycobacterial Adenosine Triphosphate (ATP) Synthesis.

Author

Tantry SJ, Markad SD, Shinde V, Bhat J, Balakrishnan G, Gupta AK, Ambady A, Raichurkar A, Kedari C, Sharma S, Mudugal NV, Narayan A, Naveen Kumar CN, Nanduri R, Bharath S, Reddy J, Panduga V, Prabhakar KR, Kandaswamy K, Saralaya R, Kaur P, Dinesh N, Guptha S, Rich K, Murray D, Plant H, Preston M, Ashton H, Plant D, Walsh J, Alcock P, Naylor K, Collier M, Whiteaker J, McLaughlin RE, Mallya M, Panda M, Rudrapatna S, Ramachandran V, Shandil R, Sambandamurthy VK, Mdluli K, Cooper CB, Rubin H, Yano T, Iyer P, Narayanan S, Kavanagh S, Mukherjee K, Balasubramanian V, Hosagrahara VP, Solapure S, Ravishankar S, and Hameed P S

Subjects

Animals, Antitubercular Agents chemistry, Antitubercular Agents pharmacokinetics, Antitubercular Agents pharmacology, Ethers chemistry, Ethers pharmacokinetics, Ethers pharmacology, Ethers therapeutic use, Humans, Mice, Mice, Inbred BALB C, Models, Molecular, Pyridines chemistry, Pyridines pharmacokinetics, Pyridines pharmacology, Quinine chemistry, Quinine pharmacokinetics, Quinine pharmacology, Quinine therapeutic use, Tuberculosis metabolism, Adenosine Triphosphate metabolism, Antitubercular Agents therapeutic use, Mycobacterium tuberculosis drug effects, Pyridines therapeutic use, Quinine analogs & derivatives, Tuberculosis drug therapy

Abstract

The approval of bedaquiline to treat tuberculosis has validated adenosine triphosphate (ATP) synthase as an attractive target to kill Mycobacterium tuberculosis (Mtb). Herein, we report the discovery of two diverse lead series imidazo[1,2-a]pyridine ethers (IPE) and squaramides (SQA) as inhibitors of mycobacterial ATP synthesis. Through medicinal chemistry exploration, we established a robust structure-activity relationship of these two scaffolds, resulting in nanomolar potencies in an ATP synthesis inhibition assay. A biochemical deconvolution cascade suggested cytochrome c oxidase as the potential target of IPE class of molecules, whereas characterization of spontaneous resistant mutants of SQAs unambiguously identified ATP synthase as its molecular target. Absence of cross resistance against bedaquiline resistant mutants suggested a different binding site for SQAs on ATP synthase. Furthermore, SQAs were found to be noncytotoxic and demonstrated efficacy in a mouse model of tuberculosis infection.

Published

2017

6. In silico-based high-throughput screen for discovery of novel combinations for tuberculosis treatment.

Author

Singh R, Ramachandran V, Shandil R, Sharma S, Khandelwal S, Karmarkar M, Kumar N, Solapure S, Saralaya R, Nanduri R, Panduga V, Reddy J, Prabhakar KR, Rajagopalan S, Rao N, Narayanan S, Anandkumar A, Balasubramanian V, and Datta S

Subjects

Animals, Mice, Mice, Inbred BALB C, Microbial Sensitivity Tests, Antitubercular Agents therapeutic use, Ethambutol therapeutic use, Isoniazid therapeutic use, Rifampin therapeutic use, Tuberculosis drug therapy

Abstract

There are currently 18 drug classes for the treatment of tuberculosis, including those in the development pipeline. An in silico simulation enabled combing the innumerably large search space to derive multidrug combinations. Through the use of ordinary differential equations (ODE), we constructed an in silico kinetic platform in which the major metabolic pathways in Mycobacterium tuberculosis and the mechanisms of the antituberculosis drugs were integrated into a virtual proteome. The optimized model was used to evaluate 816 triplets from the set of 18 drugs. The experimentally derived cumulative fractional inhibitory concentration (∑FIC) value was within twofold of the model prediction. Bacterial enumeration revealed that a significant number of combinations that were synergistic for growth inhibition were also synergistic for bactericidal effect. The in silico-based screen provided new starting points for testing in a mouse model of tuberculosis, in which two novel triplets and five novel quartets were significantly superior to the reference drug triplet of isoniazid, rifampin, and ethambutol (HRE) or the quartet of HRE plus pyrazinamide (HREZ)., (Copyright © 2015, Singh et al.)

Published

2015

7. Triaminopyrimidine is a fast-killing and long-acting antimalarial clinical candidate.

Author

Hameed P S, Solapure S, Patil V, Henrich PP, Magistrado PA, Bharath S, Murugan K, Viswanath P, Puttur J, Srivastava A, Bellale E, Panduga V, Shanbag G, Awasthy D, Landge S, Morayya S, Koushik K, Saralaya R, Raichurkar A, Rautela N, Roy Choudhury N, Ambady A, Nandishaiah R, Reddy J, Prabhakar KR, Menasinakai S, Rudrapatna S, Chatterji M, Jiménez-Díaz MB, Martínez MS, Sanz LM, Coburn-Flynn O, Fidock DA, Lukens AK, Wirth DF, Bandodkar B, Mukherjee K, McLaughlin RE, Waterson D, Rosenbrier-Ribeiro L, Hickling K, Balasubramanian V, Warner P, Hosagrahara V, Dudley A, Iyer PS, Narayanan S, Kavanagh S, and Sambandamurthy VK

Subjects

Amines pharmacology, Animals, Drug Evaluation, Preclinical, Drug Resistance, Microbial, Guinea Pigs, Half-Life, Rats, Antimalarials pharmacology, Plasmodium falciparum drug effects, Pyrimidines pharmacology

Abstract

The widespread emergence of Plasmodium falciparum (Pf) strains resistant to frontline agents has fuelled the search for fast-acting agents with novel mechanism of action. Here, we report the discovery and optimization of novel antimalarial compounds, the triaminopyrimidines (TAPs), which emerged from a phenotypic screen against the blood stages of Pf. The clinical candidate (compound 12) is efficacious in a mouse model of Pf malaria with an ED99 <30 mg kg(-1) and displays good in vivo safety margins in guinea pigs and rats. With a predicted half-life of 36 h in humans, a single dose of 260 mg might be sufficient to maintain therapeutic blood concentration for 4-5 days. Whole-genome sequencing of resistant mutants implicates the vacuolar ATP synthase as a genetic determinant of resistance to TAPs. Our studies highlight the potential of TAPs for single-dose treatment of Pf malaria in combination with other agents in clinical development.

Published

2015

8. 1,4-azaindole, a potential drug candidate for treatment of tuberculosis.

Author

Chatterji M, Shandil R, Manjunatha MR, Solapure S, Ramachandran V, Kumar N, Saralaya R, Panduga V, Reddy J, Prabhakar KR, Sharma S, Sadler C, Cooper CB, Mdluli K, Iyer PS, Narayanan S, and Shirude PS

Subjects

Animals, Antitubercular Agents chemical synthesis, Antitubercular Agents pharmacokinetics, Dogs, Drug Therapy, Combination, Female, Humans, Indoles chemical synthesis, Indoles pharmacokinetics, Male, Mice, Mice, Inbred BALB C, Pyridines chemical synthesis, Pyridines pharmacokinetics, Rats, Antitubercular Agents therapeutic use, Indoles therapeutic use, Pyridines therapeutic use, Tuberculosis, Pulmonary drug therapy

Abstract

New therapeutic strategies against multidrug-resistant (MDR) and extensively drug-resistant (XDR) Mycobacterium tuberculosis are urgently required to combat the global tuberculosis (TB) threat. Toward this end, we previously reported the identification of 1,4-azaindoles, a promising class of compounds with potent antitubercular activity through noncovalent inhibition of decaprenylphosphoryl-β-D-ribose 2'-epimerase (DprE1). Further, this series was optimized to improve its physicochemical properties and pharmacokinetics in mice. Here, we describe the short-listing of a potential clinical candidate, compound 2, that has potent cellular activity, drug-like properties, efficacy in mouse and rat chronic TB infection models, and minimal in vitro safety risks. We also demonstrate that the compounds, including compound 2, have no antagonistic activity with other anti-TB drugs. Moreover, compound 2 shows synergy with PA824 and TMC207 in vitro, and the synergy effect is translated in vivo with TMC207. The series is predicted to have a low clearance in humans, and the predicted human dose for compound 2 is ≤1 g/day. Altogether, our data suggest that a 1,4-azaindole (compound 2) is a promising candidate for the development of a novel anti-TB drug., (Copyright © 2014, American Society for Microbiology. All Rights Reserved.)

Published

2014

9. N-aryl-2-aminobenzimidazoles: novel, efficacious, antimalarial lead compounds.

Author

Ramachandran S, Hameed P S, Srivastava A, Shanbhag G, Morayya S, Rautela N, Awasthy D, Kavanagh S, Bharath S, Reddy J, Panduga V, Prabhakar KR, Saralaya R, Nanduri R, Raichurkar A, Menasinakai S, Achar V, Jiménez-Díaz MB, Martínez MS, Angulo-Barturen I, Ferrer S, Sanz LM, Gamo FJ, Duffy S, Avery VM, Waterson D, Lee MC, Coburn-Flynn O, Fidock DA, Iyer PS, Narayanan S, Hosagrahara V, and Sambandamurthy VK

Subjects

Aminopyridines pharmacokinetics, Aminopyridines pharmacology, Animals, Antimalarials pharmacokinetics, Antimalarials pharmacology, Benzimidazoles pharmacokinetics, Benzimidazoles pharmacology, Hepatocytes metabolism, Humans, Malaria drug therapy, Malaria mortality, Mice, SCID, Microsomes, Liver metabolism, Plasmodium berghei drug effects, Plasmodium falciparum drug effects, Rats, Structure-Activity Relationship, Aminopyridines chemistry, Antimalarials chemistry, Benzimidazoles chemistry

Abstract

From the phenotypic screening of the AstraZeneca corporate compound collection, N-aryl-2-aminobenzimidazoles have emerged as novel hits against the asexual blood stage of Plasmodium falciparum (Pf). Medicinal chemistry optimization of the potency against Pf and ADME properties resulted in the identification of 12 as a lead molecule. Compound 12 was efficacious in the P. berghei (Pb) model of malaria. This compound displayed an excellent pharmacokinetic profile with a long half-life (19 h) in rat blood. This profile led to an extended survival of animals for over 30 days following a dose of 50 mg/kg in the Pb malaria model. Compound 12 retains its potency against a panel of Pf isolates with known mechanisms of resistance. The fast killing observed in the in vitro parasite reduction ratio (PRR) assay coupled with the extended survival highlights the promise of this novel chemical class for the treatment of malaria.

Published

2014

10. Aminoazabenzimidazoles, a novel class of orally active antimalarial agents.

Author

Hameed P S, Chinnapattu M, Shanbag G, Manjrekar P, Koushik K, Raichurkar A, Patil V, Jatheendranath S, Rudrapatna SS, Barde SP, Rautela N, Awasthy D, Morayya S, Narayan C, Kavanagh S, Saralaya R, Bharath S, Viswanath P, Mukherjee K, Bandodkar B, Srivastava A, Panduga V, Reddy J, Prabhakar KR, Sinha A, Jiménez-Díaz MB, Martínez MS, Angulo-Barturen I, Ferrer S, Sanz LM, Gamo FJ, Duffy S, Avery VM, Magistrado PA, Lukens AK, Wirth DF, Waterson D, Balasubramanian V, Iyer PS, Narayanan S, Hosagrahara V, Sambandamurthy VK, and Ramachandran S

Subjects

Animals, Antimalarials chemistry, Benzimidazoles pharmacokinetics, Benzimidazoles pharmacology, Biological Availability, Cell Line, Tumor, Cell Survival drug effects, High-Throughput Screening Assays, Humans, Inhibitory Concentration 50, Mice, Small Molecule Libraries, Structure-Activity Relationship, Antimalarials pharmacology, Benzimidazoles therapeutic use, Malaria, Falciparum drug therapy, Plasmodium falciparum drug effects

Abstract

Whole-cell high-throughput screening of the AstraZeneca compound library against the asexual blood stage of Plasmodium falciparum (Pf) led to the identification of amino imidazoles, a robust starting point for initiating a hit-to-lead medicinal chemistry effort. Structure-activity relationship studies followed by pharmacokinetics optimization resulted in the identification of 23 as an attractive lead with good oral bioavailability. Compound 23 was found to be efficacious (ED90 of 28.6 mg·kg(-1)) in the humanized P. falciparum mouse model of malaria (Pf/SCID model). Representative compounds displayed a moderate to fast killing profile that is comparable to that of chloroquine. This series demonstrates no cross-resistance against a panel of Pf strains with mutations to known antimalarial drugs, thereby suggesting a novel mechanism of action for this chemical class.

Published

2014

11. Lead optimization of 1,4-azaindoles as antimycobacterial agents.

Author

Shirude PS, Shandil RK, Manjunatha MR, Sadler C, Panda M, Panduga V, Reddy J, Saralaya R, Nanduri R, Ambady A, Ravishankar S, Sambandamurthy VK, Humnabadkar V, Jena LK, Suresh RS, Srivastava A, Prabhakar KR, Whiteaker J, McLaughlin RE, Sharma S, Cooper CB, Mdluli K, Butler S, Iyer PS, Narayanan S, and Chatterji M

Subjects

Alcohol Oxidoreductases, Animals, Antitubercular Agents pharmacokinetics, Antitubercular Agents pharmacology, Bacterial Proteins antagonists & inhibitors, Cyclic Nucleotide Phosphodiesterases, Type 6 antagonists & inhibitors, Disease Models, Animal, Humans, Indoles pharmacokinetics, Mice, Mycobacterium tuberculosis drug effects, Oxidoreductases antagonists & inhibitors, Rats, Structure-Activity Relationship, Antitubercular Agents chemical synthesis, Indoles chemical synthesis

Abstract

In a previous report, we described the discovery of 1,4-azaindoles, a chemical series with excellent in vitro and in vivo antimycobacterial potency through noncovalent inhibition of decaprenylphosphoryl-β-d-ribose-2'-epimerase (DprE1). Nevertheless, high mouse metabolic turnover and phosphodiesterase 6 (PDE6) off-target activity limited its advancement. Herein, we report lead optimization of this series, culminating in potent, metabolically stable compounds that have a robust pharmacokinetic profile without any PDE6 liability. Furthermore, we demonstrate efficacy for 1,4-azaindoles in a rat chronic TB infection model. We believe that compounds from the 1,4-azaindole series are suitable for in vivo combination and safety studies.

Published

2014

12. 4-aminoquinolone piperidine amides: noncovalent inhibitors of DprE1 with long residence time and potent antimycobacterial activity.

Author

Naik M, Humnabadkar V, Tantry SJ, Panda M, Narayan A, Guptha S, Panduga V, Manjrekar P, Jena LK, Koushik K, Shanbhag G, Jatheendranath S, Manjunatha MR, Gorai G, Bathula C, Rudrapatna S, Achar V, Sharma S, Ambady A, Hegde N, Mahadevaswamy J, Kaur P, Sambandamurthy VK, Awasthy D, Narayan C, Ravishankar S, Madhavapeddi P, Reddy J, Prabhakar K, Saralaya R, Chatterji M, Whiteaker J, McLaughlin B, Chiarelli LR, Riccardi G, Pasca MR, Binda C, Neres J, Dhar N, Signorino-Gelo F, McKinney JD, Ramachandran V, Shandil R, Tommasi R, Iyer PS, Narayanan S, Hosagrahara V, Kavanagh S, Dinesh N, and Ghorpade SR

Subjects

Alcohol Oxidoreductases, Amides pharmacokinetics, Amides pharmacology, Animals, Antitubercular Agents pharmacokinetics, Antitubercular Agents pharmacology, Catalytic Domain, Cell Line, Tumor, Drug Resistance, Bacterial, Genome, Bacterial, Humans, Kinetics, Microbial Sensitivity Tests, Molecular Docking Simulation, Mutation, Mycobacterium tuberculosis enzymology, Mycobacterium tuberculosis genetics, Piperidines pharmacokinetics, Piperidines pharmacology, Protein Binding, Quinolones pharmacokinetics, Quinolones pharmacology, Rats, Wistar, Stereoisomerism, Structure-Activity Relationship, Amides chemistry, Antitubercular Agents chemistry, Bacterial Proteins antagonists & inhibitors, Mycobacterium tuberculosis drug effects, Oxidoreductases antagonists & inhibitors, Piperidines chemistry, Quinolones chemistry

Abstract

4-Aminoquinolone piperidine amides (AQs) were identified as a novel scaffold starting from a whole cell screen, with potent cidality on Mycobacterium tuberculosis (Mtb). Evaluation of the minimum inhibitory concentrations, followed by whole genome sequencing of mutants raised against AQs, identified decaprenylphosphoryl-β-d-ribose 2'-epimerase (DprE1) as the primary target responsible for the antitubercular activity. Mass spectrometry and enzyme kinetic studies indicated that AQs are noncovalent, reversible inhibitors of DprE1 with slow on rates and long residence times of ∼100 min on the enzyme. In general, AQs have excellent leadlike properties and good in vitro secondary pharmacology profile. Although the scaffold started off as a single active compound with moderate potency from the whole cell screen, structure-activity relationship optimization of the scaffold led to compounds with potent DprE1 inhibition (IC50 < 10 nM) along with potent cellular activity (MIC = 60 nM) against Mtb.

Published

2014

13. Novel N-linked aminopiperidine-based gyrase inhibitors with improved hERG and in vivo efficacy against Mycobacterium tuberculosis.

Author

Hameed P S, Patil V, Solapure S, Sharma U, Madhavapeddi P, Raichurkar A, Chinnapattu M, Manjrekar P, Shanbhag G, Puttur J, Shinde V, Menasinakai S, Rudrapatana S, Achar V, Awasthy D, Nandishaiah R, Humnabadkar V, Ghosh A, Narayan C, Ramya VK, Kaur P, Sharma S, Werngren J, Hoffner S, Panduga V, Kumar CN, Reddy J, Kumar K N M, Ganguly S, Bharath S, Bheemarao U, Mukherjee K, Arora U, Gaonkar S, Coulson M, Waterson D, Sambandamurthy VK, and de Sousa SM

Subjects

Acute Disease, Administration, Oral, Animals, Antitubercular Agents pharmacokinetics, Antitubercular Agents pharmacology, Bacterial Proteins antagonists & inhibitors, Bacterial Proteins genetics, Bacterial Proteins metabolism, Biological Availability, Chronic Disease, DNA Gyrase genetics, DNA Gyrase metabolism, Drug Resistance, Bacterial, ERG1 Potassium Channel, Fluoroquinolones pharmacology, Humans, Macrophages drug effects, Macrophages microbiology, Mice, Inbred BALB C, Microbial Sensitivity Tests, Molecular Docking Simulation, Mutation, Mycobacterium tuberculosis enzymology, Piperidines pharmacokinetics, Piperidines pharmacology, Protein Subunits genetics, Protein Subunits metabolism, Rats, Stereoisomerism, Structure-Activity Relationship, Topoisomerase II Inhibitors pharmacokinetics, Topoisomerase II Inhibitors pharmacology, Tuberculosis, Pulmonary drug therapy, Antitubercular Agents chemical synthesis, Ether-A-Go-Go Potassium Channels antagonists & inhibitors, Mycobacterium tuberculosis drug effects, Piperidines chemical synthesis, Topoisomerase II Inhibitors chemical synthesis

Abstract

DNA gyrase is a clinically validated target for developing drugs against Mycobacterium tuberculosis (Mtb). Despite the promise of fluoroquinolones (FQs) as anti-tuberculosis drugs, the prevalence of pre-existing resistance to FQs is likely to restrict their clinical value. We describe a novel class of N-linked aminopiperidinyl alkyl quinolones and naphthyridones that kills Mtb by inhibiting the DNA gyrase activity. The mechanism of inhibition of DNA gyrase was distinct from the fluoroquinolones, as shown by their ability to inhibit the growth of fluoroquinolone-resistant Mtb. Biochemical studies demonstrated this class to exert its action via single-strand cleavage rather than double-strand cleavage, as seen with fluoroquinolones. The compounds are highly bactericidal against extracellular as well as intracellular Mtb. Lead optimization resulted in the identification of potent compounds with improved oral bioavailability and reduced cardiac ion channel liability. Compounds from this series are efficacious in various murine models of tuberculosis.

Published

2014

14. Benzimidazoles: novel mycobacterial gyrase inhibitors from scaffold morphing.

Author

Hameed P S, Raichurkar A, Madhavapeddi P, Menasinakai S, Sharma S, Kaur P, Nandishaiah R, Panduga V, Reddy J, Sambandamurthy VK, and Sriram D

Abstract

Type II topoisomerases are well conserved across the bacterial species, and inhibition of DNA gyrase by fluoroquinolones has provided an attractive option for treatment of tuberculosis (TB). However, the emergence of fluoroquinolone-resistant strains of Mycobacterium tuberculosis (Mtb) poses a threat for its sustainability. A scaffold hopping approach using the binding mode of novel bacterial topoisomerase inhibitors (NBTIs) led to the identification of a novel class of benzimidazoles as DNA gyrase inhibitors with potent anti-TB activity. Docking of benzimidazoles to a NBTI bound crystal structure suggested that this class of compound makes key contacts in the enzyme active site similar to the reported NBTIs. This observation was further confirmed through the measurement of DNA gyrase inhibition, and activity against Mtb strains harboring mutations that confer resistance to aminopiperidines based NBTIs and Mtb strains resistant to moxifloxacin. Structure-activity relationship modification at the C-7 position of the left-hand side ring provided further avenue to improve hERG selectivity for this chemical series that has been the major challenges for NBTIs.

Published

2014

15. Optimization of pyrrolamides as mycobacterial GyrB ATPase inhibitors: structure-activity relationship and in vivo efficacy in a mouse model of tuberculosis.

Author

P SH, Solapure S, Mukherjee K, Nandi V, Waterson D, Shandil R, Balganesh M, Sambandamurthy VK, Raichurkar AK, Deshpande A, Ghosh A, Awasthy D, Shanbhag G, Sheikh G, McMiken H, Puttur J, Reddy J, Werngren J, Read J, Kumar M, R M, Chinnapattu M, Madhavapeddi P, Manjrekar P, Basu R, Gaonkar S, Sharma S, Hoffner S, Humnabadkar V, Subbulakshmi V, and Panduga V

Subjects

Animals, Cell Line, Humans, Mice, Mycobacterium tuberculosis drug effects, Structure-Activity Relationship, Antitubercular Agents pharmacology, Antitubercular Agents therapeutic use, Mycobacterium tuberculosis pathogenicity, Tuberculosis drug therapy

Abstract

Moxifloxacin has shown excellent activity against drug-sensitive as well as drug-resistant tuberculosis (TB), thus confirming DNA gyrase as a clinically validated target for discovering novel anti-TB agents. We have identified novel inhibitors in the pyrrolamide class which kill Mycobacterium tuberculosis through inhibition of ATPase activity catalyzed by the GyrB domain of DNA gyrase. A homology model of the M. tuberculosis H37Rv GyrB domain was used for deciphering the structure-activity relationship and binding interactions of inhibitors with mycobacterial GyrB enzyme. Proposed binding interactions were later confirmed through cocrystal structure studies with the Mycobacterium smegmatis GyrB ATPase domain. The most potent compound in this series inhibited supercoiling activity of DNA gyrase with a 50% inhibitory concentration (IC50) of <5 nM, an MIC of 0.03 μg/ml against M. tuberculosis H37Rv, and an MIC90 of <0.25 μg/ml against 99 drug-resistant clinical isolates of M. tuberculosis. The frequency of isolating spontaneous resistant mutants was ∼10(-6) to 10(-8), and the point mutation mapped to the M. tuberculosis GyrB domain (Ser208 Ala), thus confirming its mode of action. The best compound tested for in vivo efficacy in the mouse model showed a 1.1-log reduction in lung CFU in the acute model and a 0.7-log reduction in the chronic model. This class of GyrB inhibitors could be developed as novel anti-TB agents.

Published

2014

16. Azaindoles: noncovalent DprE1 inhibitors from scaffold morphing efforts, kill Mycobacterium tuberculosis and are efficacious in vivo.

Author

Shirude PS, Shandil R, Sadler C, Naik M, Hosagrahara V, Hameed S, Shinde V, Bathula C, Humnabadkar V, Kumar N, Reddy J, Panduga V, Sharma S, Ambady A, Hegde N, Whiteaker J, McLaughlin RE, Gardner H, Madhavapeddi P, Ramachandran V, Kaur P, Narayan A, Guptha S, Awasthy D, Narayan C, Mahadevaswamy J, Vishwas KG, Ahuja V, Srivastava A, Prabhakar KR, Bharath S, Kale R, Ramaiah M, Choudhury NR, Sambandamurthy VK, Solapure S, Iyer PS, Narayanan S, and Chatterji M

Subjects

Alcohol Oxidoreductases, Animals, Antitubercular Agents pharmacokinetics, Antitubercular Agents therapeutic use, Drug Discovery, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacokinetics, Enzyme Inhibitors pharmacology, Enzyme Inhibitors therapeutic use, Indoles pharmacokinetics, Indoles pharmacology, Indoles therapeutic use, Mice, Rats, Tuberculosis, Multidrug-Resistant drug therapy, Antitubercular Agents pharmacology, Bacterial Proteins antagonists & inhibitors, Indoles chemical synthesis, Mycobacterium tuberculosis drug effects, Oxidoreductases antagonists & inhibitors

Abstract

We report 1,4-azaindoles as a new inhibitor class that kills Mycobacterium tuberculosis in vitro and demonstrates efficacy in mouse tuberculosis models. The series emerged from scaffold morphing efforts and was demonstrated to noncovalently inhibit decaprenylphosphoryl-β-D-ribose2'-epimerase (DprE1). With "drug-like" properties and no expectation of pre-existing resistance in the clinic, this chemical class has the potential to be developed as a therapy for drug-sensitive and drug-resistant tuberculosis.

Published

2013

17. Thiazolopyridine ureas as novel antitubercular agents acting through inhibition of DNA Gyrase B.

Author

Kale MG, Raichurkar A, P SH, Waterson D, McKinney D, Manjunatha MR, Kranthi U, Koushik K, Jena Lk, Shinde V, Rudrapatna S, Barde S, Humnabadkar V, Madhavapeddi P, Basavarajappa H, Ghosh A, Ramya VK, Guptha S, Sharma S, Vachaspati P, Kumar KN, Giridhar J, Reddy J, Panduga V, Ganguly S, Ahuja V, Gaonkar S, Kumar CN, Ogg D, Tucker JA, Boriack-Sjodin PA, de Sousa SM, Sambandamurthy VK, and Ghorpade SR

Subjects

Animals, Antitubercular Agents administration & dosage, Antitubercular Agents chemistry, Disease Models, Animal, Dose-Response Relationship, Drug, Mice, Mice, Inbred BALB C, Models, Molecular, Molecular Structure, Mycobacterium tuberculosis enzymology, Pyridines administration & dosage, Pyridines chemistry, Structure-Activity Relationship, Topoisomerase II Inhibitors administration & dosage, Topoisomerase II Inhibitors chemistry, Urea analogs & derivatives, Urea chemistry, Antitubercular Agents pharmacology, DNA Gyrase metabolism, Mycobacterium tuberculosis drug effects, Pyridines pharmacology, Topoisomerase II Inhibitors pharmacology, Tuberculosis drug therapy, Urea pharmacology

Abstract

A pharmacophore-based search led to the identification of thiazolopyridine ureas as a novel scaffold with antitubercular activity acting through inhibition of DNA Gyrase B (GyrB) ATPase. Evaluation of the binding mode of thiazolopyridines in a Mycobacterium tuberculosis (Mtb) GyrB homology model prompted exploration of the side chains at the thiazolopyridine ring C-5 position to access the ribose/solvent pocket. Potent compounds with GyrB IC50 ≤ 1 nM and Mtb MIC ≤ 0.1 μM were obtained with certain combinations of side chains at the C-5 position and heterocycles at the C-6 position of the thiazolopyridine core. Substitutions at C-5 also enabled optimization of the physicochemical properties. Representative compounds were cocrystallized with Streptococcus pneumoniae (Spn) ParE; these confirmed the binding modes predicted by the homology model. The target link to GyrB was confirmed by genetic mapping of the mutations conferring resistance to thiazolopyridine ureas. The compounds are bactericidal in vitro and efficacious in vivo in an acute murine model of tuberculosis.

Published

2013

18. In vitro and in vivo efficacy of β-lactams against replicating and slowly growing/nonreplicating Mycobacterium tuberculosis.

Author

Solapure S, Dinesh N, Shandil R, Ramachandran V, Sharma S, Bhattacharjee D, Ganguly S, Reddy J, Ahuja V, Panduga V, Parab M, Vishwas KG, Kumar N, Balganesh M, and Balasubramanian V

Subjects

Animals, Disease Models, Animal, Drug Therapy, Combination, Female, Humans, Meropenem, Mice, Mice, Inbred BALB C, Microbial Sensitivity Tests standards, Mycobacterium tuberculosis growth & development, Streptomycin pharmacology, Treatment Outcome, Tuberculosis, Pulmonary microbiology, Amoxicillin-Potassium Clavulanate Combination administration & dosage, Amoxicillin-Potassium Clavulanate Combination pharmacokinetics, Amoxicillin-Potassium Clavulanate Combination pharmacology, Amoxicillin-Potassium Clavulanate Combination therapeutic use, Anti-Bacterial Agents administration & dosage, Anti-Bacterial Agents pharmacokinetics, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents therapeutic use, Clavulanic Acid administration & dosage, Clavulanic Acid pharmacokinetics, Clavulanic Acid pharmacology, Clavulanic Acid therapeutic use, Mycobacterium tuberculosis drug effects, Thienamycins administration & dosage, Thienamycins pharmacokinetics, Thienamycins pharmacology, Thienamycins therapeutic use, Tuberculosis, Pulmonary drug therapy, beta-Lactams administration & dosage, beta-Lactams pharmacokinetics, beta-Lactams pharmacology, beta-Lactams therapeutic use

Abstract

Beta-lactams, in combination with beta-lactamase inhibitors, are reported to have activity against Mycobacterium tuberculosis bacteria growing in broth, as well as inside the human macrophage. We tested representative beta-lactams belonging to 3 different classes for activity against replicating M. tuberculosis in broth and nonreplicating M. tuberculosis under hypoxia, as well as against streptomycin-starved M. tuberculosis strain 18b (ss18b) in the presence or absence of clavulanate. Most of the combinations showed bactericidal activity against replicating M. tuberculosis, with up to 200-fold improvement in potency in the presence of clavulanate. None of the combinations, including those containing meropenem, imipenem, and faropenem, killed M. tuberculosis under hypoxia. However, faropenem- and meropenem-containing combinations killed strain ss18b moderately. We tested the bactericidal activities of meropenem-clavulanate and amoxicillin-clavulanate combinations in the acute and chronic aerosol infection models of tuberculosis in BALB/c mice. Based on pharmacokinetic/pharmacodynamic indexes reported for beta-lactams against other bacterial pathogens, a cumulative percentage of a 24-h period that the drug concentration exceeds the MIC under steady-state pharmacokinetic conditions (%TMIC) of 20 to 40% was achieved in mice using a suitable dosing regimen. Both combinations showed marginal reduction in lung CFU compared to the late controls in the acute model, whereas both were inactive in the chronic model.

Published

2013

19. Effect of repeated dosing on rifampin exposure in BALB/c mice.

Author

Hosagrahara V, Reddy J, Ganguly S, Panduga V, Ahuja V, Parab M, and Giridhar J

Subjects

Administration, Intravenous, Administration, Oral, Animals, Cytochrome P-450 Enzyme System metabolism, Mice, Mice, Inbred BALB C, Microsomes, Liver enzymology, Microsomes, Liver metabolism, Rifampin blood, Time Factors, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Microsomes, Liver drug effects, Rifampin administration & dosage, Rifampin pharmacokinetics

Abstract

The discovery of novel therapeutics for the treatment of tuberculosis involves routine testing in a mouse model over four weeks of daily dosing with test compounds. In this model, daily oral administration of rifampin (10 mg/kg) showed significantly lower plasma exposure on day 5 compared to day 1. The absence of PXR-mediated induction of mouse Cyp3a isoforms was confirmed in the present study by incubating liver microsomes prepared from control and rifampin treated mice with probe substrates of CYP3A. To test whether the reduction in exposure was due to Pgp-mediated efflux, verapamil, a known Pgp inhibitor, was dosed to the rifampin pre-treated mice which led to an increase in exposure to that obtained after a single dose of rifampin, suggesting the role of Pgp induction in reducing exposure to rifampin. To further confirm Pgp induction in rifampin treated mice, digoxin, a known substrate of Pgp, was administered to the rifampin pre-treated mice, and a significant drop in the digoxin exposure was observed compared to the control group. Collectively, our results show that repeated administration of rifampin in mice leads to a reduction in oral exposure due to induction of Pgp-mediated efflux of rifampin, and not via induction of CYP3A isoforms., (Copyright © 2013 Elsevier B.V. All rights reserved.)

Published

2013

20. Effect of coadministration of moxifloxacin and rifampin on Mycobacterium tuberculosis in a murine aerosol infection model.

Author

Balasubramanian V, Solapure S, Gaonkar S, Mahesh Kumar KN, Shandil RK, Deshpande A, Kumar N, Vishwas KG, Panduga V, Reddy J, Ganguly S, Louie A, and Drusano GL

Subjects

Animals, Antitubercular Agents administration & dosage, Antitubercular Agents pharmacokinetics, Aza Compounds administration & dosage, Aza Compounds pharmacokinetics, Fluoroquinolones, Mice, Mice, Inbred BALB C, Moxifloxacin, Quinolines administration & dosage, Quinolines pharmacokinetics, Rifampin administration & dosage, Rifampin pharmacokinetics, Tuberculosis, Pulmonary microbiology, Antitubercular Agents therapeutic use, Aza Compounds therapeutic use, Mycobacterium tuberculosis drug effects, Mycobacterium tuberculosis pathogenicity, Quinolines therapeutic use, Rifampin therapeutic use, Tuberculosis, Pulmonary drug therapy

Abstract

Coadministration of moxifloxacin and rifampin was evaluated in a murine model of Mycobacterium tuberculosis pulmonary infection to determine whether the finding of antagonism documented in a hollow-fiber infection model could be recapitulated in vivo. Colony counts were followed in a no-treatment control group, groups administered moxifloxacin or rifampin monotherapy, and a group administered a combination of the two agents. Following 18 days of once-daily oral administration to mice infected with M. tuberculosis, there was a reduction in the plasma exposure to rifampin that decreased further when rifampin was coadministered with moxifloxacin. Pharmacodynamic analysis demonstrated a mild antagonistic interaction between moxifloxacin and rifampin with respect to cell kill in the mouse model for tuberculosis (TB). No emergence of resistance was noted over 28 days of therapy, even with monotherapy. This was true even though one of the agents in the combination (moxifloxacin) induces error-prone replication. The previously noted antagonism with respect to cell kill shown in the hollow-fiber infection model was recapitulated in the murine TB lung model, although to a lesser extent.

Published

2012