Your search keyword '"Alumasa JN"' showing total 22 results

1. Antibiotic that inhibits trans -translation blocks binding of EF-Tu to tmRNA but not to tRNA.

Author

Marathe N, Nguyen HA, Alumasa JN, Kuzmishin Nagy AB, Vazquez M, Dunham CM, and Keiler KC

Subjects

Anti-Bacterial Agents pharmacology, RNA-Binding Proteins genetics, Protein Biosynthesis, RNA, Bacterial genetics, RNA, Transfer metabolism, Peptide Elongation Factor Tu genetics, Peptide Elongation Factors genetics

Abstract

Importance: Elongation factor thermo-unstable (EF-Tu) is a universally conserved translation factor that mediates productive interactions between tRNAs and the ribosome. In bacteria, EF-Tu also delivers transfer-messenger RNA (tmRNA)-SmpB to the ribosome during trans -translation. We report the first small molecule, KKL-55, that specifically inhibits EF-Tu activity in trans -translation without affecting its activity in normal translation. KKL-55 has broad-spectrum antibiotic activity, suggesting that compounds targeted to the tmRNA-binding interface of EF-Tu could be developed into new antibiotics to treat drug-resistant infections., Competing Interests: The authors declare no conflict of interest.

Published

2023

2. Pathogen-specific antimicrobials engineered de novo through membrane-protein biomimicry.

Author

Simonson AW, Mongia AS, Aronson MR, Alumasa JN, Chan DC, Lawanprasert A, Howe MD, Bolotsky A, Mal TK, George C, Ebrahimi A, Baughn AD, Proctor EA, Keiler KC, and Medina SH

Subjects

Bacterial Outer Membrane drug effects, Bacterial Proteins genetics, Humans, Lung drug effects, Lung microbiology, Molecular Mimicry, Peptides genetics, Anti-Bacterial Agents pharmacology, Membrane Proteins genetics, Mycobacterium tuberculosis drug effects, Peptides pharmacology

Abstract

Precision antimicrobials aim to kill pathogens without damaging commensal bacteria in the host, and thereby cure disease without antibiotic-associated dysbiosis. Here we report the de novo design of a synthetic host defence peptide that targets a specific pathogen by mimicking key molecular features of the pathogen's channel-forming membrane proteins. By exploiting physical and structural vulnerabilities within the pathogen's cellular envelope, we designed a peptide sequence that undergoes instructed tryptophan-zippered assembly within the mycolic acid-rich outer membrane of Mycobacterium tuberculosis to specifically kill the pathogen without collateral toxicity towards lung commensal bacteria or host tissue. These mycomembrane-templated assemblies elicit rapid mycobactericidal activity and enhance the potency of antibiotics by improving their otherwise poor diffusion across the rigid M. tuberculosis envelope with respect to agents that exploit transmembrane protein channels for antimycobacterial activity. This biomimetic strategy may aid the design of other narrow-spectrum antimicrobial peptides.

Published

2021

3. trans-Translation inhibitors bind to a novel site on the ribosome and clear Neisseria gonorrhoeae in vivo.

Author

Aron ZD, Mehrani A, Hoffer ED, Connolly KL, Srinivas P, Torhan MC, Alumasa JN, Cabrera M, Hosangadi D, Barbor JS, Cardinale SC, Kwasny SM, Morin LR, Butler MM, Opperman TJ, Bowlin TL, Jerse A, Stagg SM, Dunham CM, and Keiler KC

Subjects

Animals, Bacterial Proteins genetics, Bacterial Proteins metabolism, Binding Sites genetics, Caco-2 Cells, Female, Gonorrhea microbiology, Gonorrhea prevention & control, Humans, Mice, Neisseria gonorrhoeae genetics, Protein Biosynthesis genetics, Protein Synthesis Inhibitors chemistry, RNA, Bacterial genetics, RNA, Bacterial metabolism, Ribosomal Proteins genetics, Ribosomal Proteins metabolism, Ribosomes genetics, Ribosomes metabolism, Neisseria gonorrhoeae drug effects, Protein Biosynthesis drug effects, Protein Synthesis Inhibitors pharmacology, Ribosomes drug effects

Abstract

Bacterial ribosome rescue pathways that remove ribosomes stalled on mRNAs during translation have been proposed as novel antibiotic targets because they are essential in bacteria and are not conserved in humans. We previously reported the discovery of a family of acylaminooxadiazoles that selectively inhibit trans-translation, the main ribosome rescue pathway in bacteria. Here, we report optimization of the pharmacokinetic and antibiotic properties of the acylaminooxadiazoles, producing MBX-4132, which clears multiple-drug resistant Neisseria gonorrhoeae infection in mice after a single oral dose. Single particle cryogenic-EM studies of non-stop ribosomes show that acylaminooxadiazoles bind to a unique site near the peptidyl-transfer center and significantly alter the conformation of ribosomal protein bL27, suggesting a novel mechanism for specific inhibition of trans-translation by these molecules. These results show that trans-translation is a viable therapeutic target and reveal a new conformation within the bacterial ribosome that may be critical for ribosome rescue pathways.

Published

2021

4. Antibacterial kaneoheoic acids A-F from a Hawaiian fungus Fusarium sp. FM701.

Author

Uz Zaman KA, Wu X, Hu Z, Yoshida W, Hou S, Saito J, Avad KA, Hevener KE, Alumasa JN, and Cao S

Subjects

Anti-Bacterial Agents pharmacology, Fungi, Hawaii, Microbial Sensitivity Tests, Fusarium, Polyketides pharmacology

Abstract

Alarming rate of resistance to the existing antibiotics exhibits the importance of developing new antibiotic molecules from relatively under explored sources as well as implementing alternative approaches like antibiotic adjuvants. Six previously undescribed fungal polyketides, kaneoheoic acids A-F (1-6) were isolated from a fungal strain Fusarium sp. FM701 which was collected from a muddy sample of Hawaiian beach. The structures of these six compounds were elucidated by spectroscopic interpretation, including HRESIMS and NMR, and electronic circular dichroism (ECD) analysis. All six compounds that were inactive when tested alone showed significant antibacterial activity against Staphylococcus aureus and Bacillus subtilis, in the range of 10-80 μg/mL when assayed in combination with either chloramphenicol (half of the MIC, 1 μg/mL), an FDA approved antibiotic or disulfiram (6 μg/mL), an established antibiotic adjuvant that augmented the activity of antibiotics., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2021

5. Comparison of Proteomic Responses as Global Approach to Antibiotic Mechanism of Action Elucidation.

Author

Senges CHR, Stepanek JJ, Wenzel M, Raatschen N, Ay Ü, Märtens Y, Prochnow P, Vázquez Hernández M, Yayci A, Schubert B, Janzing NBM, Warmuth HL, Kozik M, Bongard J, Alumasa JN, Albada B, Penkova M, Lukežič T, Sorto NA, Lorenz N, Miller RG, Zhu B, Benda M, Stülke J, Schäkermann S, Leichert LI, Scheinpflug K, Brötz-Oesterhelt H, Hertweck C, Shaw JT, Petković H, Brunel JM, Keiler KC, Metzler-Nolte N, and Bandow JE

Subjects

Bacillus subtilis, Bacterial Proteins genetics, Tetracyclines, Anti-Bacterial Agents pharmacology, Proteomics

Abstract

New antibiotics are urgently needed to address the mounting resistance challenge. In early drug discovery, one of the bottlenecks is the elucidation of targets and mechanisms. To accelerate antibiotic research, we provide a proteomic approach for the rapid classification of compounds into those with precedented and unprecedented modes of action. We established a proteomic response library of Bacillus subtilis covering 91 antibiotics and comparator compounds, and a mathematical approach was developed to aid data analysis. Comparison of proteomic responses (CoPR) allows the rapid identification of antibiotics with dual mechanisms of action as shown for atypical tetracyclines. It also aids in generating hypotheses on mechanisms of action as presented for salvarsan (arsphenamine) and the antirheumatic agent auranofin, which is under consideration for repurposing. Proteomic profiling also provides insights into the impact of antibiotics on bacterial physiology through analysis of marker proteins indicative of the impairment of cellular processes and structures. As demonstrated for trans -translation, a promising target not yet exploited clinically, proteomic profiling supports chemical biology approaches to investigating bacterial physiology., (Copyright © 2020 Senges et al.)

Published

2020

6. A Small-Molecule Inhibitor of trans -Translation Synergistically Interacts with Cathelicidin Antimicrobial Peptides To Impair Survival of Staphylococcus aureus.

Author

Huang Y, Alumasa JN, Callaghan LT, Baugh RS, Rae CD, Keiler KC, and McGillivray SM

Subjects

Cell Line, Tumor, Drug Synergism, HeLa Cells, Humans, Methicillin Resistance drug effects, Microbial Sensitivity Tests, Staphylococcal Infections microbiology, Cathelicidins, Anti-Bacterial Agents pharmacology, Antimicrobial Cationic Peptides pharmacology, Small Molecule Libraries pharmacology, Staphylococcal Infections drug therapy, Staphylococcus aureus drug effects

Abstract

Staphylococcus aureus is a leading cause of infection in the United States, and due to the rapid development of resistance, new antibiotics are constantly needed. trans -Translation is a particularly promising antibiotic target because it is conserved in many bacterial species, is critical for bacterial survival, and is unique among prokaryotes. We have investigated the potential of KKL-40, a small-molecule inhibitor of trans -translation, and find that it inhibits both methicillin-susceptible and methicillin-resistant strains of S. aureus KKL-40 is also effective against Gram-positive pathogens, including a vancomycin-resistant strain of Enterococcus faecalis , Bacillus subtilis , and Streptococcus pyogenes , although its performance with Gram-negative pathogens is mixed. KKL-40 synergistically interacts with the human antimicrobial peptide LL-37, a member of the cathelicidin family, to inhibit S. aureus but not other antibiotics tested, including daptomycin, kanamycin, or erythromycin. KKL-40 is not cytotoxic to HeLa cells at concentrations that are 100-fold higher than the effective MIC. We also find that S. aureus develops minimal resistance to KKL-40 even after multiday passage at sublethal concentrations. Therefore, trans -translation inhibitors could be a particularly promising drug target against S. aureus , not only because of their ability to inhibit bacterial growth but also because of their potential to simultaneously render S. aureus more susceptible to host antimicrobial peptides., (Copyright © 2019 American Society for Microbiology.)

Published

2019

7. Tetrazole-Based trans -Translation Inhibitors Kill Bacillus anthracis Spores To Protect Host Cells.

Author

Alumasa JN, Goralski TDP, and Keiler KC

Subjects

Animals, Cell Line, Ciprofloxacin pharmacology, Macrophages microbiology, Mice, Microbial Sensitivity Tests, RAW 264.7 Cells, Anthrax prevention & control, Anti-Bacterial Agents pharmacology, Bacillus anthracis drug effects, Benzamides pharmacology, Protein Synthesis Inhibitors pharmacology, Spores, Bacterial drug effects, Tetrazoles pharmacology

Abstract

Bacillus anthracis , the causative agent of anthrax, remains a significant threat to humans, including potential use in bioterrorism and biowarfare. The capacity to engineer strains with increased pathogenicity coupled with the ease of disseminating lethal doses of B. anthracis spores makes it necessary to identify chemical agents that target and kill spores. Here, we demonstrate that a tetrazole-based trans -translation inhibitor, KKL-55, is bactericidal against vegetative cells of B. anthracis in culture. Using a fluorescent analog, we show that this class of compounds colocalizes with developing endospores and bind purified spores in vitro KKL-55 was effective against spores at concentrations close to its MIC for vegetative cells. Spore germination was inhibited at 1.2× MIC, and spores were killed at 2× MIC. In contrast, ciprofloxacin killed germinants at concentrations close to its MIC but did not prevent germination even at 32× MIC. Because toxins are released by germinants, macrophages infected by B. anthracis spores are killed early in the germination process. At ≥2× MIC, KKL-55 protected macrophages from death after infection with B. anthracis spores. Ciprofloxacin required concentrations of ≥8× MIC to exhibit a similar effect. Taken together, these data indicate that KKL-55 and related tetrazoles are good lead candidates for therapeutics targeting B. anthracis spores and suggest that there is an early requirement for trans -translation in germinating spores., (Copyright © 2017 American Society for Microbiology.)

Published

2017

8. Ribosome Rescue Inhibitors Kill Actively Growing and Nonreplicating Persister Mycobacterium tuberculosis Cells.

Author

Alumasa JN, Manzanillo PS, Peterson ND, Lundrigan T, Baughn AD, Cox JS, and Keiler KC

Subjects

Antitubercular Agents chemistry, Benzamides chemistry, Drug Resistance, Bacterial drug effects, Microbial Sensitivity Tests, Molecular Docking Simulation, Mycobacterium tuberculosis genetics, Oxadiazoles chemistry, RNA, Ribosomal, 23S chemistry, Small Molecule Libraries chemistry, Antitubercular Agents pharmacology, Benzamides pharmacology, Mycobacterium tuberculosis drug effects, Oxadiazoles pharmacology, RNA, Ribosomal, 23S antagonists & inhibitors, Small Molecule Libraries pharmacology

Abstract

The emergence of Mycobacterium tuberculosis (MTB) strains that are resistant to most or all available antibiotics has created a severe problem for treating tuberculosis and has spurred a quest for new antibiotic targets. Here, we demonstrate that trans-translation is essential for growth of MTB and is a viable target for development of antituberculosis drugs. We also show that an inhibitor of trans-translation, KKL-35, is bactericidal against MTB under both aerobic and anoxic conditions. Biochemical experiments show that this compound targets helix 89 of the 23S rRNA. In silico molecular docking predicts a binding pocket for KKL-35 adjacent to the peptidyl-transfer center in a region not targeted by conventional antibiotics. Computational solvent mapping suggests that this pocket is a druggable hot spot for small molecule binding. Collectively, our findings reveal a new target for antituberculosis drug development and provide critical insight on the mechanism of antibacterial action for KKL-35 and related 1,3,4-oxadiazole benzamides.

Published

2017

9. Inhibitors of Ribosome Rescue Arrest Growth of Francisella tularensis at All Stages of Intracellular Replication.

Author

Goralski TD, Dewan KK, Alumasa JN, Avanzato V, Place DE, Markley RL, Katkere B, Rabadi SM, Bakshi CS, Keiler KC, and Kirimanjeswara GS

Subjects

Animals, Cell Survival drug effects, Interferon-gamma pharmacology, Liver microbiology, Macrophages microbiology, Mice, Microbial Sensitivity Tests, RAW 264.7 Cells, Virulence drug effects, Anti-Bacterial Agents pharmacology, Francisella tularensis drug effects, Oxadiazoles pharmacology, Ribosomes drug effects

Abstract

Bacteria require at least one pathway to rescue ribosomes stalled at the ends of mRNAs. The primary pathway for ribosome rescue is trans-translation, which is conserved in >99% of sequenced bacterial genomes. Some species also have backup systems, such as ArfA or ArfB, which can rescue ribosomes in the absence of sufficient trans-translation activity. Small-molecule inhibitors of ribosome rescue have broad-spectrum antimicrobial activity against bacteria grown in liquid culture. These compounds were tested against the tier 1 select agent Francisella tularensis to determine if they can limit bacterial proliferation during infection of eukaryotic cells. The inhibitors KKL-10 and KKL-40 exhibited exceptional antimicrobial activity against both attenuated and fully virulent strains of F. tularensis in vitro and during ex vivo infection. Addition of KKL-10 or KKL-40 to macrophages or liver cells at any time after infection by F. tularensis prevented further bacterial proliferation. When macrophages were stimulated with the proinflammatory cytokine gamma interferon before being infected by F. tularensis, addition of KKL-10 or KKL-40 reduced intracellular bacteria by >99%, indicating that the combination of cytokine-induced stress and a nonfunctional ribosome rescue pathway is fatal to F. tularensis Neither KKL-10 nor KKL-40 was cytotoxic to eukaryotic cells in culture. These results demonstrate that ribosome rescue is required for F. tularensis growth at all stages of its infection cycle and suggest that KKL-10 and KKL-40 are good lead compounds for antibiotic development., (Copyright © 2016, American Society for Microbiology. All Rights Reserved.)

Published

2016

10. Clicking on trans-translation drug targets.

Author

Alumasa JN and Keiler KC

Published

2015

11. Identification of inhibitors of a bacterial sigma factor using a new high-throughput screening assay.

Author

El-Mowafi SA, Sineva E, Alumasa JN, Nicoloff H, Tomsho JW, Ades SE, and Keiler KC

Subjects

Anti-Bacterial Agents chemistry, Bacterial Proteins antagonists & inhibitors, Bacterial Proteins genetics, Bacterial Proteins metabolism, Escherichia coli drug effects, Escherichia coli genetics, Gene Expression Regulation, Bacterial, Inteins drug effects, Inteins genetics, Luminescent Proteins genetics, Lysine, Metabolic Networks and Pathways drug effects, Peptides, Cyclic genetics, Peptides, Cyclic metabolism, Protein Splicing, Reproducibility of Results, Sigma Factor genetics, Anti-Bacterial Agents pharmacology, High-Throughput Screening Assays methods, Sigma Factor antagonists & inhibitors, Sigma Factor metabolism, Small Molecule Libraries pharmacology

Abstract

Gram-negative bacteria are formidable pathogens because their cell envelope presents an adaptable barrier to environmental and host-mediated challenges. The stress response pathway controlled by the alternative sigma factor σ(E) is critical for maintenance of the cell envelope. Because σ(E) is required for the virulence or viability of several Gram-negative pathogens, it might be a useful target for antibiotic development. To determine if small molecules can inhibit the σ(E) pathway, and to permit high-throughput screening for antibiotic lead compounds, a σ(E) activity assay that is compatible with high-throughput screening was developed and validated. The screen employs a biological assay with positive readout. An Escherichia coli strain was engineered to express yellow fluorescent protein (YFP) under negative regulation by the σ(E) pathway, such that inhibitors of the pathway increase the production of YFP. To validate the screen, the reporter strain was used to identify σ(E) pathway inhibitors from a library of cyclic peptides. Biochemical characterization of one of the inhibitory cyclic peptides showed that it binds σ(E), inhibits RNA polymerase holoenzyme formation, and inhibits σ(E)-dependent transcription in vitro. These results demonstrate that alternative sigma factors can be inhibited by small molecules and enable high-throughput screening for inhibitors of the σ(E) pathway., (Copyright © 2015, American Society for Microbiology. All Rights Reserved.)

Published

2015

12. Cell-based assay to identify inhibitors of the Hfq-sRNA regulatory pathway.

Author

El-Mowafi SA, Alumasa JN, Ades SE, and Keiler KC

Subjects

Biological Assay methods, Escherichia coli genetics, Gene Expression Regulation, Bacterial genetics, Protein Binding genetics, RNA, Bacterial genetics, Signal Transduction genetics, Virulence genetics, Escherichia coli Proteins genetics, Host Factor 1 Protein genetics, RNA, Small Untranslated genetics

Abstract

Noncoding small RNAs (sRNAs) act in conjunction with the RNA chaperone Hfq to regulate gene expression in bacteria. Because Hfq is required for virulence in several bacterial pathogens, the Hfq-sRNA system is an attractive target for antibiotic development. A reporter strain in which the expression of yellow fluorescent protein (YFP) is controlled by Hfq-sRNA was engineered to identify inhibitors of this system. A reporter that is targeted by Hfq in conjunction with the RybB sRNA was used in a genetic screen to identify inhibitors from a library of cyclic peptides produced in Escherichia coli using split-intein circular ligation of peptides and proteins (SICLOPPS), an intein-based technology. One cyclic peptide identified in this screen, RI20, inhibited Hfq-mediated repression of gene expression in conjunction with both RybB and an unrelated sRNA, MicF. Gel mobility shift assays showed that RI20 inhibited binding of Hfq to RybB and MicF with similar Ki values. These data suggest that RI20 inhibits Hfq activity by blocking interactions with sRNAs and provide a paradigm for inhibiting virulence genes in Gram-negative pathogens., (Copyright © 2014, American Society for Microbiology. All Rights Reserved.)

Published

2014

13. The potential of trans-translation inhibitors as antibiotics.

Author

Keiler KC and Alumasa JN

Subjects

Anti-Bacterial Agents chemistry, Bacteria drug effects, Drug Discovery, RNA, Bacterial genetics, RNA, Bacterial metabolism, Anti-Bacterial Agents pharmacology, Bacteria genetics, Protein Biosynthesis drug effects

Published

2013

14. Small molecule inhibitors of trans-translation have broad-spectrum antibiotic activity.

Author

Ramadoss NS, Alumasa JN, Cheng L, Wang Y, Li S, Chambers BS, Chang H, Chatterjee AK, Brinker A, Engels IH, and Keiler KC

Subjects

Anti-Bacterial Agents pharmacology, Biological Assay, Codon, Terminator genetics, Drug Design, Drug Resistance, Bacterial genetics, Escherichia coli growth & development, Escherichia coli metabolism, Gene Library, Humans, Luciferases genetics, Nucleic Acid Conformation, RNA, Bacterial chemistry, RNA, Bacterial metabolism, Ribosomes genetics, Anti-Bacterial Agents biosynthesis, Escherichia coli genetics, Protein Biosynthesis physiology, RNA, Bacterial genetics, Small Molecule Libraries

Abstract

The trans-translation pathway for protein tagging and ribosome release plays a critical role for viability and virulence in a wide range of pathogens but is not found in animals. To explore the use of trans-translation as a target for antibiotic development, a high-throughput screen and secondary screening assays were used to identify small molecule inhibitors of the pathway. Compounds that inhibited protein tagging and proteolysis of tagged proteins were recovered from the screen. One of the most active compounds, KKL-35, inhibited the trans-translation tagging reaction with an IC50 = 0.9 µM. KKL-35 and other compounds identified in the screen exhibited broad-spectrum antibiotic activity, validating trans-translation as a target for drug development. This unique target could play a key role in combating strains of pathogenic bacteria that are resistant to existing antibiotics.

Published

2013

15. Cytostatic versus cytocidal activities of chloroquine analogues and inhibition of hemozoin crystal growth.

Author

Gorka AP, Alumasa JN, Sherlach KS, Jacobs LM, Nickley KB, Brower JP, de Dios AC, and Roepe PD

Subjects

Antimalarials metabolism, Cells, Cultured, Chloroquine analogs & derivatives, Chloroquine metabolism, Crystallization, Cytostatic Agents metabolism, Cytotoxins metabolism, Erythrocytes parasitology, Hemeproteins antagonists & inhibitors, Humans, Inhibitory Concentration 50, Kinetics, Phospholipids chemistry, Phospholipids pharmacology, Plasmodium falciparum growth & development, Plasmodium falciparum metabolism, Antimalarials pharmacology, Chloroquine pharmacology, Cytostatic Agents pharmacology, Cytotoxins pharmacology, Erythrocytes drug effects, Heme chemistry, Hemeproteins chemistry, Plasmodium falciparum drug effects

Abstract

We report an improved, nonhazardous, high-throughput assay for in vitro quantification of antimalarial drug inhibition of β-hematin (hemozoin) crystallization performed under conditions that are more physiological relative to previous assays. The assay uses the differential detergent solubility of crystalline and noncrystalline forms of heme and is optimized via the use of lipid catalyst. Using this assay, we quantify the effect of pH on the crystal growth-inhibitory activities of current quinoline antimalarials, evaluate the catalytic efficiencies of different lipids, and test for a possible correlation between hemozoin inhibition by drugs versus their antiplasmodial activity. Consistent with several previous reports, we found a good correlation between hemozoin inhibition potency versus cytostatic antiplasmodial potency (50% inhibitory concentration) for a series of chloroquine (CQ) analogues. However, we found no correlation between hemozoin inhibition potency and cytocidal antiplasmodial potency (50% lethal dose) for the same drugs, suggesting that cellular targets for these two layers of 4-aminoquinoline drug activity differ. This important concept is also explored further for QN and its stereoisomers in the accompanying paper (A. P. Gorka, K. S. Sherlach, A. C. de Dios, and P. D. Roepe, Antimicrob. Agents Chemother. 57:365-374, 2013).

Published

2013

16. Pharmacological inhibition of the ClpXP protease increases bacterial susceptibility to host cathelicidin antimicrobial peptides and cell envelope-active antibiotics.

Author

McGillivray SM, Tran DN, Ramadoss NS, Alumasa JN, Okumura CY, Sakoulas G, Vaughn MM, Zhang DX, Keiler KC, and Nizet V

Subjects

Amino Acid Sequence, Bacillus anthracis drug effects, Bacillus anthracis genetics, Cell Membrane metabolism, Drug Resistance, Bacterial, Drug Synergism, Methicillin-Resistant Staphylococcus aureus drug effects, Molecular Sequence Data, Staphylococcus aureus drug effects, Staphylococcus aureus growth & development, Tetrazoles pharmacology, Cathelicidins, Anti-Bacterial Agents pharmacology, Antimicrobial Cationic Peptides pharmacology, Bacteria drug effects, Endopeptidase Clp antagonists & inhibitors, Escherichia coli Proteins antagonists & inhibitors, Protease Inhibitors pharmacology

Abstract

The ClpXP protease is a critical bacterial intracellular protease that regulates protein turnover in many bacterial species. Here we identified a pharmacological inhibitor of the ClpXP protease, F2, and evaluated its action in Bacillus anthracis and Staphylococcus aureus. We found that F2 exhibited synergistic antimicrobial activity with cathelicidin antimicrobial peptides and antibiotics that target the cell well and/or cell membrane, such as penicillin and daptomycin, in B. anthracis and drug-resistant strains of S. aureus. ClpXP inhibition represents a novel therapeutic strategy to simultaneously sensitize pathogenic bacteria to host defenses and pharmaceutical antibiotics.

Published

2012

17. Antiplasmodial and antiproliferative pseudoguaianolides of Athroisma proteiforme from the Madagascar Dry Forest.

Author

Pan E, Gorka AP, Alumasa JN, Slebodnick C, Harinantenaina L, Brodie PJ, Roepe PD, Randrianaivo R, Birkinshaw C, and Kingston DG

Subjects

Antimalarials chemistry, Antineoplastic Agents, Phytogenic chemistry, Drug Screening Assays, Antitumor, Female, Flavonoids chemistry, Flavonoids isolation & purification, Humans, Inhibitory Concentration 50, Lactones chemistry, Madagascar, Molecular Structure, Sesquiterpenes chemistry, Trees, Antimalarials isolation & purification, Antimalarials pharmacology, Antineoplastic Agents, Phytogenic isolation & purification, Antineoplastic Agents, Phytogenic pharmacology, Asteraceae chemistry, Flavonoids pharmacology, Lactones isolation & purification, Lactones pharmacology, Plasmodium falciparum drug effects, Sesquiterpenes isolation & purification, Sesquiterpenes pharmacology

Abstract

Investigation of extracts from the plant Athroisma proteiforme (Humbert) Mattf. (Asteraceae) for antimalarial activity led to the isolation of the five new sesquiterpene lactones 1-5 together with centaureidin (6). The structures of the new compounds were deduced from analyses of physical and spectroscopic data, and the absolute configuration of compound 1 was confirmed by an X-ray crystallographic study. Athrolides C (3) and D (4) both showed antiplasmodial activities with IC50 values of 6.6 (3) and 7.2 μM (4) against the HB3 strain and 5.5 (3) and 4.2 μM (4) against the Dd2 strain of the malarial parasite Plasmodium falciparum. The isolates 1-6 also showed antiproliferative activity against A2780 human ovarian cancer cells, with IC50 values ranging from 0.4 to 2.5 μM.

Published

2011

18. The hydroxyl functionality and a rigid proximal N are required for forming a novel non-covalent quinine-heme complex.

Author

Alumasa JN, Gorka AP, Casabianca LB, Comstock E, de Dios AC, and Roepe PD

Subjects

Amodiaquine chemistry, Antimalarials chemical synthesis, Antimalarials pharmacology, Chloroquine chemistry, Dimerization, Dose-Response Relationship, Drug, Hemeproteins chemistry, Hydroxyl Radical pharmacology, Inhibitory Concentration 50, Magnetic Resonance Spectroscopy, Malaria, Falciparum drug therapy, Malaria, Falciparum metabolism, Malaria, Falciparum pathology, Nitrogen pharmacology, Plasmodium falciparum drug effects, Quinine analogs & derivatives, Quinine chemical synthesis, Quinine pharmacology, Antimalarials chemistry, Hemin chemistry, Hydroxyl Radical chemistry, Nitrogen chemistry, Quinine chemistry

Abstract

Quinoline antimalarial drugs bind both monomeric and dimeric forms of free heme, with distinct preferences depending on the chemical environment. Under biological conditions, chloroquine (CQ) appears to prefer to bind to μ-oxo dimeric heme, while quinine (QN) preferentially binds monomer. To further explore this important distinction, we study three newly synthesized and several commercially available QN analogues lacking various functional groups. We find that removal of the QN hydroxyl lowers heme affinity, hemozoin (Hz) inhibition efficiency, and antiplasmodial activity. Elimination of the rigid quinuclidyl ring has similar effects, but elimination of either the vinyl or methoxy group does not. Replacing the quinuclidyl N with a less rigid tertiary aliphatic N only partially restores activity. To further study these trends, we probe drug-heme interactions via NMR studies with both Fe and Zn protoporphyrin IX (FPIX, ZnPIX) for QN, dehydroxyQN (DHQN), dequinuclidylQN (DQQN), and deamino-dequinuclidylQN (DADQQN). Magnetic susceptibility measurements in the presence of FPIX demonstrate that these compounds differentially perturb FPIX monomer-dimer equilibrium. We also isolate the QN-FPIX complex formed under mild aqueous conditions and analyze it by mass spectrometry, as well as fluorescence, vibrational, and solid-state NMR spectroscopies. The data elucidate key features of QN pharmacology and allow us to propose a refined model for the preferred binding of QN to monomeric FPIX under biologically relevant conditions. With this model in hand, we also propose how QN, CQ, and amodiaquine (AQ) differ in their ability to inhibit Hz formation., (Copyright © 2010 Elsevier Inc. All rights reserved.)

Published

2011

19. Antimalarial drugs and heme in detergent micelles: An NMR study.

Author

Casabianca LB, Kallgren JB, Natarajan JK, Alumasa JN, Roepe PD, Wolf C, and de Dios AC

Subjects

Hydrogen-Ion Concentration, Molecular Structure, Primaquine chemistry, Quaternary Ammonium Compounds chemistry, Sodium Dodecyl Sulfate chemistry, Antimalarials chemistry, Detergents chemistry, Heme chemistry, Magnetic Resonance Spectroscopy methods, Micelles

Abstract

Proton nuclear magnetic resonance relaxation times were measured for the protons of micelles formed by the detergents sodium dodecyl sulfate, dodecyltrimethyl ammonium bromide, and polyethylene glycol sorbitan monolaureate in the presence of ferriprotoporphyrin IX and the antimalarial drugs chloroquine, 7-chloro-4-quinolyl 4-N,N-diethylaminobutyl sulfide, and primaquine. Diffusion coefficients were extracted from pulsed gradient NMR experiments to evaluate the degree of association of these drugs with the detergent micelles. Results indicate that at low or neutral pH when the quinolyl N is protonated, chloroquine does not associate with neutral or cationic detergent micelles. For this reason, chloroquine's interaction with heme perturbs the partitioning of heme between the aqueous medium and detergent micelles.

Published

2009

20. Antiproliferative and antimalarial anthraquinones of Scutia myrtina from the Madagascar forest.

Author

Hou Y, Cao S, Brodie PJ, Callmander MW, Ratovoson F, Rakotobe EA, Rasamison VE, Ratsimbason M, Alumasa JN, Roepe PD, and Kingston DG

Subjects

Animals, Anthraquinones isolation & purification, Anthraquinones pharmacology, Antimalarials isolation & purification, Antimalarials pharmacology, Antineoplastic Agents, Phytogenic isolation & purification, Antineoplastic Agents, Phytogenic pharmacology, Cell Line, Tumor, Humans, Madagascar, Plant Bark chemistry, Plant Extracts chemistry, Plasmodium falciparum drug effects, Anthraquinones chemistry, Antimalarials chemistry, Antineoplastic Agents, Phytogenic chemistry, Rhamnaceae chemistry

Abstract

Bioassay-guided fractionation of an ethanol extract of a Madagascar collection of the bark of Scutia myrtina led to the isolation of three new anthrone-anthraquinones, scutianthraquinones A, B and C (1-3), one new bisanthrone-anthraquinone, scutianthraquinone D (4), and the known anthraquinone, aloesaponarin I (5). The structures of all compounds were determined using a combination of 1D and 2D NMR experiments, including COSY, TOCSY, HSQC, HMBC, and ROESY sequences, and mass spectrometry. All the isolated compounds were tested against the A2780 human ovarian cancer cell line for antiproliferative activities, and against the chloroquine-resistant Plasmodium falciparum strains Dd2 and FCM29 for antiplasmodial activities. Compounds 1, 2 and 4 showed weak antiproliferative activities against the A2780 ovarian cancer cell line, while compounds 1-4 exhibited moderate antiplasmodial activities against P. falciparum Dd2 and compounds 1, 2, and 4 exhibited moderate antiplasmodial activities against P. falciparum FCM29.

Published

2009

21. Quinine and chloroquine differentially perturb heme monomer-dimer equilibrium.

Author

Casabianca LB, An D, Natarajan JK, Alumasa JN, Roepe PD, Wolf C, and de Dios AC

Subjects

Chloroquine, Dimerization, Hydrogen-Ion Concentration, Magnetic Resonance Spectroscopy, Magnetics, Quinine, Heme chemistry, Hemin chemistry

Abstract

Nuclear magnetic resonance (NMR) measurements of magnetic susceptibility have been utilized to study the equilibrium between two forms (high-spin monomer vs the antiferromagnetically coupled mu-oxo dimer) of ferriprotoporphyrin(IX) as a function of pH. The pH dependence of this equilibrium is significantly altered by the addition of either chloroquine or quinine. Chloroquine promotes the mu-oxo dimer whereas quinine promotes the monomer.

Published

2008

22. 4-N-, 4-S-, and 4-O-chloroquine analogues: influence of side chain length and quinolyl nitrogen pKa on activity vs chloroquine resistant malaria.

Author

Natarajan JK, Alumasa JN, Yearick K, Ekoue-Kovi KA, Casabianca LB, de Dios AC, Wolf C, and Roepe PD

Subjects

Animals, Antimalarials chemistry, Antimalarials pharmacology, Benzothiazoles, Chloroquine pharmacology, Diamines, Fluorescent Dyes, Intercalating Agents, Models, Molecular, Organic Chemicals, Parasitic Sensitivity Tests, Quinolines, Structure-Activity Relationship, Antimalarials chemical synthesis, Chloroquine analogs & derivatives, Chloroquine chemical synthesis, Drug Resistance, Plasmodium falciparum drug effects

Abstract

Using predictions from heme-quinoline antimalarial complex structures, previous modifications of chloroquine (CQ), and hypotheses for chloroquine resistance (CQR), we synthesize and assay CQ analogues that test structure-function principles. We vary side chain length for both monoethyl and diethyl 4-N CQ derivatives. We alter the pKa of the quinolyl N by introducing alkylthio or alkoxy substituents into the 4 position and vary side chain length for these analogues. We introduce an additional titratable amino group to the side chain of 4-O analogues with promising CQR strain selectivity and increase activity while retaining selectivity. We solve atomic resolution structures for complexes formed between representative 4-N, 4-S, and 4-O derivatives vs mu-oxo dimeric heme, measure binding constants for monomeric vs dimeric heme, and quantify hemozoin (Hz) formation inhibition in vitro. The data provide additional insight for the design of CQ analogues with improved activity vs CQR malaria.

Published

2008