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1. Novel chemical entities inhibiting Mycobacterium tuberculosis growth identified by phenotypic high-throughput screening

Author

Anuradha Kumar, Somsundaram Chettiar, Brian S. Brown, Julie Early, Juliane Ollinger, Megan Files, Mai A. Bailey, Aaron Korkegian, Devon Dennison, Matthew McNeil, James Metz, Augustine Osuma, Michael Curtin, Aaron Kunzer, Gail Freiberg, Milan Bruncko, Dale Kempf, and Tanya Parish

Subjects
Medicine, Science
Abstract

Abstract We performed a high-throughput phenotypic whole cell screen of Mycobacterium tuberculosis against a diverse chemical library of approximately 100,000 compounds from the AbbVie corporate collection and identified 24 chemotypes with anti-tubercular activity. We selected two series for further exploration and conducted structure–activity relationship studies with new analogs for the 4-phenyl piperidines (4PP) and phenylcyclobutane carboxamides (PCB). Strains with mutations in MmpL3 demonstrated resistance to both compound series. We isolated resistant mutants for the two series and found mutations in MmpL3. These data suggest that MmpL3 is the target, or mechanism of resistance for both series.

Published
2022
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4. Identification of 2-Amino Benzothiazoles with Bactericidal Activity against Mycobacterium tuberculosis

Author

Shilah Bonnett, Jo-Ann Jee, Somsundaram Chettiar, Yulia Ovechkina, Aaron Korkegian, Eric Greve, Joshua Odingo, and Tanya Parish

Subjects
antitubercular, drug discovery, antibiotic, protein secretion, bactericidal activity, tuberculosis, Microbiology, QR1-502
Abstract

ABSTRACT We identified an amino-benzothiazole scaffold from a whole-cell screen against recombinant Mycobacterium tuberculosis under expressing the essential signal peptidase LepB. The seed molecule had 2-fold higher activity against the LepB hypomorph. Through a combination of purchase and chemical synthesis, we explored the structure-activity relationship for this series; 34 analogs were tested for antitubercular activity and for cytotoxicity against eukaryotic cells. We identified molecules with improved potency and reduced cytotoxicity. However, molecules did not appear to target LepB directly and did not inhibit protein secretion. Key compounds showed good permeability, low protein binding, and lack of CYP inhibition, but metabolic stability was poor with short half-lives. The seed molecule showed good bactericidal activity against both replicating and nonreplicating bacteria, as well as potency against intracellular M. tuberculosis in murine macrophages. Overall, the microbiological properties of the series are attractive if metabolic stability can be improved, and identification of the target could assist in the development of this series. IMPORTANCE Mycobacterium tuberculosis, the causative agent of tuberculosis, is a serious global health problem requiring the development of new therapeutics. We previously ran a high-throughput screen and identified a series of compounds with antitubercular activity. In this paper, we test analogs of our hit molecules for activity against M. tuberculosis, as well as for activity against eukaryotic cells. We identified molecules with improved selectivity. Our molecules killed both replicating and nonreplicating bacteria but did not work by targeting protein secretion.

Published
2023
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5. Spirocycle MmpL3 Inhibitors with Improved hERG and Cytotoxicity Profiles as Inhibitors of Mycobacterium tuberculosis Growth

Author

Peter C. Ray, Margaret Huggett, Penelope A. Turner, Malcolm Taylor, Laura A. T. Cleghorn, Julie Early, Anuradha Kumar, Shilah A. Bonnett, Lindsay Flint, Douglas Joerss, James Johnson, Aaron Korkegian, Steven Mullen, Abraham L. Moure, Susan H. Davis, Dinakaran Murugesan, Michael Mathieson, Nicola Caldwell, Curtis A. Engelhart, Dirk Schnappinger, Ola Epemolu, Fabio Zuccotto, Jennifer Riley, Paul Scullion, Laste Stojanovski, Lisa Massoudi, Gregory T. Robertson, Anne J. Lenaerts, Gail Freiberg, Dale J. Kempf, Thierry Masquelin, Philip A. Hipskind, Joshua Odingo, Kevin D. Read, Simon R. Green, Paul G. Wyatt, and Tanya Parish

Subjects
Chemistry, QD1-999
Published
2021
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6. Novel Trifluoromethyl Pyrimidinone Compounds With Activity Against Mycobacterium tuberculosis

Author

Erik Hembre, Julie V. Early, Joshua Odingo, Catherine Shelton, Olena Anoshchenko, Junitta Guzman, Lindsay Flint, Devon Dennison, Matthew B. McNeil, Aaron Korkegian, Yulia Ovechkina, Paul Ornstein, Thierry Masquelin, Philip A. Hipskind, and Tanya Parish

Subjects
tuberculosis, anti-tubercular, bactericidal ability, whole cell activity, pyrimidinones, Chemistry, QD1-999
Abstract

The identification and development of new anti-tubercular agents are a priority research area. We identified the trifluoromethyl pyrimidinone series of compounds in a whole-cell screen against Mycobacterium tuberculosis. Fifteen primary hits had minimum inhibitory concentrations (MICs) with good potency IC90 is the concentration at which M. tuberculosis growth is inhibited by 90% (IC90 < 5 μM). We conducted a structure–activity relationship investigation for this series. We designed and synthesized an additional 44 molecules and tested all analogs for activity against M. tuberculosis and cytotoxicity against the HepG2 cell line. Substitution at the 5-position of the pyrimidinone with a wide range of groups, including branched and straight chain alkyl and benzyl groups, resulted in active molecules. Trifluoromethyl was the preferred group at the 6-position, but phenyl and benzyl groups were tolerated. The 2-pyridyl group was required for activity; substitution on the 5-position of the pyridyl ring was tolerated but not on the 6-position. Active molecules from the series demonstrated low selectivity, with cytotoxicity against eukaryotic cells being an issue. However, there were active and non-cytotoxic molecules; the most promising molecule had an MIC (IC90) of 4.9 μM with no cytotoxicity (IC50 > 100 μM). The series was inactive against Gram-negative bacteria but showed good activity against Gram-positive bacteria and yeast. A representative molecule from this series showed rapid concentration-dependent bactericidal activity against replicating M. tuberculosis bacilli with ~4 log kill in

Published
2021
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7. InhA inhibitors have activity against non-replicating Mycobacterium tuberculosis.

Author

Lindsay Flint, Aaron Korkegian, and Tanya Parish

Subjects
Medicine, Science
Abstract

We previously identified a diazaborine series with potential for development as a new tuberculosis drug. This series has activity in vitro and in vivo and targets cell wall biosynthesis via inhibition of InhA. The overall aim of this study was to determine whether InhA inhibitors have activity against non-replicating Mycobacterium tuberculosis. We tested the ability of two molecules of the diazaborine series to kill non-replicating M. tuberculosis in the nutrient starvation model; both molecules were bactericidal, reducing viability by >3 logs in 21 days. Activity showed similar kill rates to other InhA inhibitors (isoniazid and NITD-916). We conclude that inhibition of InhA is bactericidal against nutrient-starved non-replicating M. tuberculosis.

Published
2020
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9. Identification of cyclic hexapeptides natural products with inhibitory potency against Mycobacterium tuberculosis

Author

Sheo B. Singh, Joshua Odingo, Mai A. Bailey, Bjorn Sunde, Aaron Korkegian, Theresa O’Malley, Yulia Ovechkina, Thomas R. Ioerger, James C. Sacchettini, Katherine Young, David B. Olsen, and Tanya Parish

Subjects
Mycobacteria, Antibacterial, Natural product, Anti-tubercular, Antibiotic resistance, Medicine, Biology (General), QH301-705.5, Science (General), Q1-390
Abstract

Abstract Objective Our aim was to identify natural products with anti-tubercular activity. Results A set of ~ 500 purified natural product compounds was screened for inhibition against the human pathogen Mycobacterium tuberculosis. A series of cyclic hexapeptides with anti-tubercular activity was identified. Five analogs from a set of sixteen closely related compounds were active, with minimum inhibitory concentrations ranging from 2.3 to 8.9 μM. Eleven structural analogs had no significant activity (MIC > 20 μM) demonstrating structure activity relationship. Sequencing of resistant mutant isolates failed to identify changes accounting for the resistance phenotype.

Published
2018
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12. Identification of 2-amino benzothiazoles with bactericidal activity againstMycobacterium tuberculosis

Author

Shilah Bonnett, Jo-Ann Jee, Somsundaram Chettiar, Yulia Ovechkina, Aaron Korkegian, Eric Greve, Joshua Odingo, and Tanya Parish

Abstract

We identified an amino-benzothiazole scaffold from a whole cell screen against recombinantMycobacterium tuberculosisunder expressing the essential signal peptidase LepB. The seed molecule had two-fold higher activity against the LepB hypomorph. Through a combination of purchase and chemical synthesis we explored the structure activity relationship for this series; 34 analogs were tested for anti-tubercular activity and for cytotoxicity against eukaryotic cells. We identified molecules with improved potency and reduced cytotoxicity. However, molecules did not appear to target LepB directly and did not inhibit protein secretion. Key compounds showed good permeability, low protein binding, and lack of CYP inhibition, but metabolic stability was poor with short half-lives. The seed molecule showed good bactericidal activity against both replicating and non-replicating bacteria, as well as potency against intracellularM. tuberculosisin murine macrophages. Overall, the microbiological properties of the series are attractive if metabolic stability can be improved, and identification of the target could assist in development of this series.

Published
2022

15. Spirocycle MmpL3 Inhibitors with Improved hERG and Cytotoxicity Profiles as Inhibitors of Mycobacterium tuberculosis Growth

Author

Tanya Parish, Lindsay Flint, Anuradha Kumar, Lisa M. Massoudi, Paul Scullion, Gregory T. Robertson, Shilah A. Bonnett, Simon Green, Nicola Caldwell, Jennifer Riley, Gail M. Freiberg, Philip Arthur Hipskind, Michael Mathieson, Thierry Masquelin, Laste Stojanovski, Curtis A. Engelhart, Margaret Huggett, Dinakaran Murugesan, Abraham Lopez Moure, Fabio Zuccotto, Julie V. Early, Ola Epemolu, Paul G. Wyatt, Dale J. Kempf, Kevin D. Read, Susan Davis, Laura A. T. Cleghorn, James Johnson, Steven Mullen, Malcolm Taylor, Anne J. Lenaerts, Penelope A. Turner, Peter C. Ray, Joshua Odingo, Dirk Schnappinger, Aaron Korkegian, and Douglas Joerss

Subjects
0303 health sciences, Tuberculosis, biology, 030306 microbiology, Chemistry, General Chemical Engineering, Phenotypic screening, hERG, General Chemistry, Pharmacology, medicine.disease, biology.organism_classification, In vitro, Article, 3. Good health, Mycobacterium tuberculosis, 03 medical and health sciences, Minimum inhibitory concentration, In vivo, biology.protein, medicine, Cytotoxicity, QD1-999, 030304 developmental biology
Abstract

With the emergence of multi-drug-resistant strains of Mycobacterium tuberculosis, there is a pressing need for new oral drugs with novel mechanisms of action. A number of scaffolds with potent anti-tubercular in vitro activity have been identified from phenotypic screening that appear to target MmpL3. However, the scaffolds are typically lipophilic, which facilitates partitioning into hydrophobic membranes, and several contain basic amine groups. Highly lipophilic basic amines are typically cytotoxic against mammalian cell lines and have associated off-target risks, such as inhibition of human ether-a-go-go related gene (hERG) and IKr potassium current modulation. The spirocycle compound 3 was reported to target MmpL3 and displayed promising efficacy in a murine model of acute tuberculosis (TB) infection. However, this highly lipophilic monobasic amine was cytotoxic and inhibited the hERG ion channel. Herein, the related spirocycles (1-2) are described, which were identified following phenotypic screening of the Eli Lilly corporate library against M. tuberculosis. The novel N-alkylated pyrazole portion offered improved physicochemical properties, and optimization led to identification of a zwitterion series, exemplified by lead 29, with decreased HepG2 cytotoxicity as well as limited hERG ion channel inhibition. Strains with mutations in MmpL3 were resistant to 29, and under replicating conditions, 29 demonstrated bactericidal activity against M. tuberculosis. Unfortunately, compound 29 had no efficacy in an acute model of TB infection; this was most likely due to the in vivo exposure remaining above the minimal inhibitory concentration for only a limited time.

Published
2021

16. Triazolopyrimidines Target Aerobic Respiration in Mycobacterium tuberculosis

Author

Catherine Shelton, Matthew McNeil, Renee Allen, Lindsay Flint, Dara Russell, Bryan Berube, Aaron Korkegian, Yulia Ovechkina, and Tanya Parish

Subjects
Electron Transport Complex IV, Pharmacology, Infectious Diseases, Respiration, Antitubercular Agents, Cytochromes, Humans, Pharmacology (medical), Mycobacterium tuberculosis
Abstract

We previously identified a series of triazolopyrimidines with antitubercular activity. We determined that Mycobacterium tuberculosis strains with mutations in QcrB, a subunit of the cytochrome bcc-aa3 supercomplex, were resistant.

Published
2022

18. Triazolopyrimidines target aerobic respiration in Mycobacterium tuberculosis

Author

Dara Russell, Lindsay Flint, Catherine Shelton, Bryan J. Berube, Matthew B. McNeil, Tanya Parish, Aaron Korkegian, and Yulia Ovechkina

Subjects
Oxidase test, Tuberculosis, Strain (chemistry), Cytochrome, biology, Cytochrome bc1, Chemistry, Cellular respiration, Intracellular parasite, medicine.disease, biology.organism_classification, Microbiology, Mycobacterium tuberculosis, biology.protein, medicine
Abstract

We previously identified a series of triazolopyrimidines with anti-tubercular activity. We determined that Mycobacterium tuberculosis strains with mutations in a component of the cytochrome bc1 system (QcrB) were resistant to the series. A cytochrome bd oxidase deletion strain was also more sensitive to this series. We isolated resistant mutants, all of which had mutations in Rv1339. Compounds were active against intracellular bacteria but did not inhibit mitochondrial respiration in human HepG2 cells. These data are consistent with triazolopyrimidines acting via inhibition of M. tuberculosis QcrB.

Published
2021

20. Novel Trifluoromethyl Pyrimidinone Compounds With Activity Against Mycobacterium tuberculosis

Author

Hembre, Erik, primary, Early, Julie V., additional, Odingo, Joshua, additional, Shelton, Catherine, additional, Anoshchenko, Olena, additional, Guzman, Junitta, additional, Flint, Lindsay, additional, Dennison, Devon, additional, McNeil, Matthew B., additional, Korkegian, Aaron, additional, Ovechkina, Yulia, additional, Ornstein, Paul, additional, Masquelin, Thierry, additional, Hipskind, Philip A., additional, and Parish, Tanya, additional

Published
2021
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21. Design, synthesis and SAR of antitubercular benzylpiperazine ureas

Author

Evans C. Coutinho, Rohan Chitral, Kavita Raikuvar, Afreen A. Khan, Jayashree Puttur, Santosh Nandan, Krishna R. Iyer, Sohal Satish, Amitkumar Kori, Deepali Desle, Tanya Parish, Basantkumar Sharma, Aaron Korkegian, and Elvis A. F. Martis

Subjects
Stereochemistry, medicine.drug_class, Antitubercular Agents, Microbial Sensitivity Tests, 010402 general chemistry, Antimycobacterial, Ring (chemistry), 01 natural sciences, Catalysis, Piperazines, Inorganic Chemistry, chemistry.chemical_compound, Structure-Activity Relationship, Furan, Drug Discovery, medicine, Molecule, Urea, Physical and Theoretical Chemistry, Molecular Biology, Benzylpiperazine, Molecular Structure, 010405 organic chemistry, Organic Chemistry, General Medicine, Mycobacterium tuberculosis, 0104 chemical sciences, Molecular Docking Simulation, Piperazine, chemistry, Design synthesis, Information Systems, medicine.drug
Abstract

N-furfuryl piperazine ureas disclosed by scientists at GSK Tres Cantos were chosen as antimycobacterial hits from a phenotypic whole-cell screen. Bioisosteric replacement of the furan ring in the GSK Tres Cantos molecules with a phenyl ring led to molecule (I) with an MIC of 1 μM against Mtb H37Rv, low cellular toxicity (HepG2 IC50 ~ 80 μM), good DMPK properties and specificity for Mtb. With the aim of delineating the SAR associated with (I), fifty-five analogs were synthesized and screened against Mtb. The SAR suggests that the piperazine ring, benzyl urea and piperonyl moieties are essential signatures of this series. Active compounds in this series are metabolically stable, have low cellular toxicity and are valuable leads for optimization. Molecular docking suggests these molecules occupy the Q0 site of QcrB like Q203. Bioisosteric replacement of N-furfuryl piperazine-1-carboxamides yielded molecule (I) a novel lead with satisfactory PD, metabolism, and toxicity profiles.

Published
2020

22. Identification of Morpholino Thiophenes as Novel Mycobacterium tuberculosis Inhibitors, Targeting QcrB

Author

Cleghorn, Laura A T, Ray, Peter C, Odingo, Joshua, Kumar, Anuradha, Wescott, Heather, Korkegian, Aaron, Masquelin, Thierry, Lopez Moure, Abraham, Wilson, Caroline, Davis, Susan, Huggett, Margaret, Turner, Penelope, Smith, Alasdair, Epemolu, Ola, Zuccotto, Fabio, Riley, Jennifer, Scullion, Paul, Shishikura, Yoko, Ferguson, Liam, Rullas, Joaquin, Guijarro, Laura, Read, Kevin D, Green, Simon R, Hipskind, Phil, Parish, Tanya, and Wyatt, Paul G

Subjects
Mice, Structure-Activity Relationship, Morpholines, Chlorocebus aethiops, Antitubercular Agents, Animals, Cytochromes c, Mycobacterium tuberculosis, Thiophenes, Oxidoreductases, Vero Cells, Article, Cercopithecus aethiops
Abstract

With the emergence of multidrug-resistant strains of Mycobacterium tuberculosis there is a pressing need for new oral drugs with novel mechanisms of action. Herein, we describe the identification of a novel morpholino-thiophenes (MOT) series following phenotypic screening of the Eli Lilly corporate library against M. tuberculosis strain H37Rv. The design, synthesis, and structure-activity relationships of a range of analogues around the confirmed actives are described. Optimized leads with potent whole cell activity against H37Rv, no cytotoxicity flags, and in vivo efficacy in an acute murine model of infection are described. Mode-of-action studies suggest that the novel scaffold targets QcrB, a subunit of the menaquinol cytochrome c oxidoreductase, part of the bc1-aa3-type cytochrome c oxidase complex that is responsible for driving oxygen-dependent respiration.

Published
2018

23. Spirocycle MmpL3 Inhibitors with Improved hERG and Cytotoxicity Profiles as Inhibitors of Mycobacterium tuberculosis Growth

Author

Ray, Peter C., primary, Huggett, Margaret, additional, Turner, Penelope A., additional, Taylor, Malcolm, additional, Cleghorn, Laura A. T., additional, Early, Julie, additional, Kumar, Anuradha, additional, Bonnett, Shilah A., additional, Flint, Lindsay, additional, Joerss, Douglas, additional, Johnson, James, additional, Korkegian, Aaron, additional, Mullen, Steven, additional, Moure, Abraham L., additional, Davis, Susan H., additional, Murugesan, Dinakaran, additional, Mathieson, Michael, additional, Caldwell, Nicola, additional, Engelhart, Curtis A., additional, Schnappinger, Dirk, additional, Epemolu, Ola, additional, Zuccotto, Fabio, additional, Riley, Jennifer, additional, Scullion, Paul, additional, Stojanovski, Laste, additional, Massoudi, Lisa, additional, Robertson, Gregory T., additional, Lenaerts, Anne J., additional, Freiberg, Gail, additional, Kempf, Dale J., additional, Masquelin, Thierry, additional, Hipskind, Philip A., additional, Odingo, Joshua, additional, Read, Kevin D., additional, Green, Simon R., additional, Wyatt, Paul G., additional, and Parish, Tanya, additional

Published
2021
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24. Design, synthesis and SAR of antitubercular benzylpiperazine ureas

Author

Satish, Sohal, primary, Chitral, Rohan, additional, Kori, Amitkumar, additional, Sharma, Basantkumar, additional, Puttur, Jayashree, additional, Khan, Afreen A., additional, Desle, Deepali, additional, Raikuvar, Kavita, additional, Korkegian, Aaron, additional, Martis, Elvis A. F., additional, Iyer, Krishna R., additional, Coutinho, Evans C., additional, Parish, Tanya, additional, and Nandan, Santosh, additional

Published
2021
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26. Efficacy and Improved Resistance Potential of a Cofactor-Independent InhA Inhibitor of Mycobacterium tuberculosis in the C3HeB/FeJ Mouse Model

Author

Jason Halladay, Tanya Parish, Wai Choi, Vincent Hernandez, Anne J. Lenaerts, Anthony J. Smith, Matthew B. McNeil, Gregory T. Robertson, Victoria A. Ektnitphong, Michael S. Scherman, Pamela Berry, Weimin Mao, Aaron Korkegian, Devon Dennison, Yi Xia, Yasheen Zhou, David S. Carter, and M. R. K. Alley

Subjects
Boron Compounds, isoniazid, caseum, Tuberculosis, Hydrocarbons, Fluorinated, necrotic lesions, Antitubercular Agents, Microbial Sensitivity Tests, Microbiology, Mycobacterium tuberculosis, Mice, 03 medical and health sciences, Antibiotic resistance, Pharmacotherapy, Drug Development, Extracellular, Animals, Medicine, Inhibins, Experimental Therapeutics, Pharmacology (medical), antimicrobial resistance, C3HeB/FeJ mice, Lung, Tuberculosis, Pulmonary, 030304 developmental biology, Pharmacology, Aza Compounds, Mice, Inbred C3H, 0303 health sciences, biology, 030306 microbiology, business.industry, INHA, Isoniazid, Editor's Pick, biology.organism_classification, medicine.disease, Bacterial Load, Disease Models, Animal, Infectious Diseases, tuberculosis, Drug development, Female, business, medicine.drug
Abstract

AN12855 is a direct, cofactor-independent inhibitor of InhA in Mycobacterium tuberculosis. In the C3HeB/FeJ mouse model with caseous necrotic lung lesions, AN12855 proved efficacious with a significantly lower resistance frequency than isoniazid., AN12855 is a direct, cofactor-independent inhibitor of InhA in Mycobacterium tuberculosis. In the C3HeB/FeJ mouse model with caseous necrotic lung lesions, AN12855 proved efficacious with a significantly lower resistance frequency than isoniazid. AN12855 drug levels were better retained in necrotic lesions and caseum where the majority of hard to treat, extracellular bacilli reside. Owing to these combined attributes, AN12855 represents a promising alternative to the frontline antituberculosis agent isoniazid.

Published
2019

27. 8-Hydroxyquinolines are bactericidal against Mycobacterium tuberculosis

Author

Joshua O, Odingo, Julie V, Early, Jake, Smith, James, Johnson, Mai A, Bailey, Megan, Files, Junitta, Guzman, Juliane, Ollinger, Aaron, Korkegian, Anuradha, Kumar, Yulia, Ovechkina, and Tanya, Parish

Subjects
Microbial Viability, structure–activity relationship, Molecular Structure, Antitubercular Agents, Hep G2 Cells, Microbial Sensitivity Tests, Mycobacterium tuberculosis, Oxyquinoline, Structure-Activity Relationship, antibacterial, tuberculosis, Chlorocebus aethiops, Hydroxyquinolines, Animals, Humans, hydroxyquinoline, Vero Cells, Research Articles, Research Article
Abstract

There is an urgent need for new treatments effective against Mycobacterium tuberculosis, the causative agent of tuberculosis. The 8‐hydroxyquinoline series is a privileged scaffold with anticancer, antifungal, and antibacterial activities. We conducted a structure–activity relationship study of the series regarding its antitubercular activity using 26 analogs. The 8‐hydroxyquinolines showed good activity against M. tuberculosis, with minimum inhibitory concentrations (MIC90) of 4 log kill at 10× MIC over 14 days. The majority of the compounds demonstrated cytotoxicity (IC50 of

Published
2018

28. Synthesis and biological evaluation of aryl-oxadiazoles as inhibitors of Mycobacterium tuberculosis

Author

Martinez-Grau, Maria Angeles, Valcarcel, Isabel C. Gonzalez, Early, Julie V., Gessner, Richard Klaus, de Melo, Candice Soares, de la Nava, Eva Maria Martin, Korkegian, Aaron, Ovechkina, Yulia, Flint, Lindsay, Gravelle, Anisa, Cramer, Jeff W., Desai, Prashant V., Street, Leslie J., Odingo, Joshua, Masquelin, Thierry, Chibale, Kelly, and Parish, Tanya

Published
2018
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31. Construction of an overexpression library for Mycobacterium tuberculosis

Author

Melief, Eduard, Kokoczka, Rachel, Files, Megan, Bailey, Mai Ann, Alling, Torey, Li, Hongye, Ahn, James, Misquith, Ayesha, Korkegian, Aaron, Roberts, David, Sacchettini, James, and Parish, Tanya

Subjects
Methods Manuscript
Abstract

There is a pressing need to develop novel anti-tubercular drugs. High-throughput phenotypic screening yields chemical series that inhibit bacterial growth. Target identification for such series is challenging, but necessary for optimization of target engagement and the development of series into clinical drugs. We constructed a library of recombinant Mycobacterium tuberculosis strains each expressing a single protein from an inducible promoter as a tool for target identification. The library of 1733 clones was arrayed in 96-well plates for rapid screening and monitoring growth. The library contains the majority of the annotated essential genes as well as genes involved in cell wall and fatty acid biosynthesis, virulence factors, regulatory proteins, efflux, and respiration pathways. We evaluated the growth kinetics and plasmid stability over three passages for each clone in the library. We determined expression levels (mRNA and/or protein) in 396 selected clones. We screened the entire library and identified the Alr-expressing clone as the only recombinant strain, which grew in the presence of d-cycloserine (DCS). We confirmed that the Alr-expressing clone was resistant to DCS (7-fold shift in minimum inhibitory concentration). The library represents a new tool that can be used to screen for compound resistance and other phenotypes.

Published
2018

32. Identification of cyclic hexapeptides natural products with inhibitory potency against Mycobacterium tuberculosis

Author

Tanya Parish, David B. Olsen, Mai A. Bailey, Aaron Korkegian, Katherine Young, Theresa O’Malley, Bjorn Sunde, Sheo B. Singh, Yulia Ovechkina, James C. Sacchettini, Thomas R. Ioerger, and Joshua Odingo

Subjects
Antibiotic resistance, Mutant, Antitubercular Agents, lcsh:Medicine, Human pathogen, Microbial Sensitivity Tests, Natural product, Microbiology, Mycobacterium tuberculosis, chemistry.chemical_compound, Structure-Activity Relationship, Anti-tubercular, Structure–activity relationship, Humans, lcsh:Science (General), lcsh:QH301-705.5, Biological Products, biology, lcsh:R, Mycobacteria, biology.organism_classification, Phenotype, Antibacterial, Inhibitory potency, Research Note, chemistry, lcsh:Biology (General), Oligopeptides, lcsh:Q1-390
Abstract

Objective Our aim was to identify natural products with anti-tubercular activity. Results A set of ~ 500 purified natural product compounds was screened for inhibition against the human pathogen Mycobacterium tuberculosis. A series of cyclic hexapeptides with anti-tubercular activity was identified. Five analogs from a set of sixteen closely related compounds were active, with minimum inhibitory concentrations ranging from 2.3 to 8.9 μM. Eleven structural analogs had no significant activity (MIC > 20 μM) demonstrating structure activity relationship. Sequencing of resistant mutant isolates failed to identify changes accounting for the resistance phenotype.

Published
2018

33. Discovery of a cofactor-independent inhibitor of Mycobacterium tuberculosis InhA

Author

Pamela Berry, Yasheen Zhou, David S. Carter, Jason Halladay, Courtney Hastings, Vincent Hernandez, Bjorn Sunde, Weimin Mao, James C. Sacchettini, Aaron Korkegian, Wai Choi, Peter J. Tonge, Mrk Alley, Anne J. Lenaerts, Yi Xia, Gregory T. Robertson, Michael S. Scherman, Tanya Parish, Lisa K. Woolhiser, Veronica Gruppo, Lindsay Flint, Thomas R. Ioerger, Theresa O’Malley, and Matthew B. McNeil

Subjects
0301 basic medicine, Drug, Tuberculosis, Health, Toxicology and Mutagenesis, media_common.quotation_subject, 030106 microbiology, Plant Science, Reductase, Biochemistry, Genetics and Molecular Biology (miscellaneous), Microbiology, Mycobacterium tuberculosis, 03 medical and health sciences, Medicine, Research Articles, media_common, chemistry.chemical_classification, Ecology, biology, business.industry, INHA, Isoniazid, medicine.disease, biology.organism_classification, In vitro, 3. Good health, 030104 developmental biology, Enzyme, chemistry, business, medicine.drug, Research Article
Abstract

AN12855 is a novel cofactor-independent inhibitor of Mycobacterium tuberculosis InhA. AN12855 has potent activity against M. tuberculosis, good oral bioavailability, and comparable efficacy to isoniazid in infection models., New antitubercular agents are needed to combat the spread of multidrug- and extensively drug-resistant strains of Mycobacterium tuberculosis. The frontline antitubercular drug isoniazid (INH) targets the mycobacterial enoyl-ACP reductase, InhA. Resistance to INH is predominantly through mutations affecting the prodrug-activating enzyme KatG. Here, we report the identification of the diazaborines as a new class of direct InhA inhibitors. The lead compound, AN12855, exhibited in vitro bactericidal activity against replicating bacteria and was active against several drug-resistant clinical isolates. Biophysical and structural investigations revealed that AN12855 binds to and inhibits the substrate-binding site of InhA in a cofactor-independent manner. AN12855 showed good drug exposure after i.v. and oral delivery, with 53% oral bioavailability. Delivered orally, AN12855 exhibited dose-dependent efficacy in both an acute and chronic murine model of tuberculosis infection that was comparable with INH. Combined, AN12855 is a promising candidate for the development of new antitubercular agents.

Published
2018

34. Synthesis and biological evaluation of aryl-oxadiazoles as inhibitors of Mycobacterium tuberculosis

Author

Maria Angeles, Martinez-Grau, Isabel C Gonzalez, Valcarcel, Julie V, Early, Richard Klaus, Gessner, Candice Soares, de Melo, Eva Maria Martin, de la Nava, Aaron, Korkegian, Yulia, Ovechkina, Lindsay, Flint, Anisa, Gravelle, Jeff W, Cramer, Prashant V, Desai, Leslie J, Street, Joshua, Odingo, Thierry, Masquelin, Kelly, Chibale, and Tanya, Parish

Subjects
Antibacterial, Oxadiazoles, Structure-Activity Relationship, Dose-Response Relationship, Drug, Molecular Structure, Phenotypic screening, Microbial Sensitivity Tests, Mycobacterium tuberculosis, Article, ComputingMethodologies_COMPUTERGRAPHICS, Anti-Bacterial Agents
Abstract

Graphical abstract, Highlights • We conducted SAR for the aryl-oxadiazole series with anti-bacterial activity against Mycobacterium tuberculosis. • Improved compounds have sub-micromolar butyrate-specific activity. • Compounds are not cytotoxic against eukaryotic cells. • A basic nitrogen in the linker and salt formation improved aqueous solubility., Despite increased research efforts to find new treatments for tuberculosis in recent decades, compounds with novel mechanisms of action are still required. We previously identified a series of novel aryl-oxadiazoles with anti-tubercular activity specific for bacteria using butyrate as a carbon source. We explored the structure activity relationship of this series. Structural modifications were performed in all domains to improve potency and physico-chemical properties. A number of compounds displayed sub-micromolar activity against M. tuberculosis utilizing butyrate, but not glucose as the carbon source. Compounds showed no or low cytotoxicity against eukaryotic cells. Three compounds were profiled in mouse pharmacokinetic studies. Plasma clearance was low to moderate but oral exposure suggested solubility-limited drug absorption in addition to first pass metabolism. The presence of a basic nitrogen in the linker slightly increased solubility, and salt formation optimized aqueous solubility. Our findings suggest that the 1,3,4-oxadiazoles are useful tools and warrant further investigation.

Published
2018

35. Efficacy and Improved Resistance Potential of a Cofactor-Independent InhA Inhibitor of Mycobacterium tuberculosis in the C3HeB/FeJ Mouse Model

Author

Robertson, Gregory T., primary, Ektnitphong, Victoria A., additional, Scherman, Michael S., additional, McNeil, Matthew B., additional, Dennison, Devon, additional, Korkegian, Aaron, additional, Smith, Anthony J., additional, Halladay, Jason, additional, Carter, David S., additional, Xia, Yi, additional, Zhou, Yasheen, additional, Choi, Wai, additional, Berry, Pamela W., additional, Mao, Weimin, additional, Hernandez, Vincent, additional, Alley, M. R. K., additional, Parish, Tanya, additional, and Lenaerts, Anne J., additional

Published
2019
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36. 8‐Hydroxyquinolines are bactericidal againstMycobacterium tuberculosis

Author

Odingo, Joshua O., primary, Early, Julie V., additional, Smith, Jake, additional, Johnson, James, additional, Bailey, Mai A., additional, Files, Megan, additional, Guzman, Junitta, additional, Ollinger, Juliane, additional, Korkegian, Aaron, additional, Kumar, Anuradha, additional, Ovechkina, Yulia, additional, and Parish, Tanya, additional

Published
2019
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37. Mutations in the Essential Arabinosyltransferase EmbC Lead to Alterations in Mycobacterium tuberculosis Lipoarabinomannan

Author

Tanya Parish, David M. Roberts, Rachel Blair, and Aaron Korkegian

Subjects
Lipopolysaccharides, Signal peptide, Tuberculosis, Blotting, Western, Molecular Sequence Data, Antitubercular Agents, Protein Sorting Signals, Microbiology, Biochemistry, Protein Structure, Secondary, law.invention, Mycobacterium tuberculosis, Bacterial Proteins, law, medicine, Amino Acid Sequence, Pentosyltransferases, Molecular Biology, Ethambutol, Aspartic Acid, Genes, Essential, Microbial Viability, Lipoarabinomannan, Sequence Homology, Amino Acid, biology, Reverse Transcriptase Polymerase Chain Reaction, Mycobacterium smegmatis, Gene Expression Regulation, Bacterial, Cell Biology, bacterial infections and mycoses, biology.organism_classification, medicine.disease, carbohydrates (lipids), Essential gene, Mutation, Recombinant DNA, lipids (amino acids, peptides, and proteins), Asparagine, medicine.drug
Abstract

The Mycobacterium tuberculosis cell wall is a complex structure essential for the viability of the organism and its interaction with the host. The glycolipid lipoarabinomannan (LAM) plays an important role in mediating host-bacteria interactions and is involved in modulation of the immune response. The arabinosyltransferase EmbC required for LAM biosynthesis is essential. We constructed recombinant strains of M. tuberculosis expressing a variety of alleles of EmbC. We demonstrated that EmbC has a functional signal peptide in M. tuberculosis. Over- or underexpression of EmbC resulted in reduced or increased sensitivity to ethambutol, respectively. The C-terminal domain of EmbC was essential for activity because truncated alleles were unable to mediate LAM production in Mycobacterium smegmatis and were unable to complement an embC deletion in M. tuberculosis. The C-terminal domain of the closely related arabinosyltransferase EmbB was unable to complement the function of the EmbC C-terminal domain. Two functional motifs were identified. The GT-C motif contains two aspartate residues essential for function in the DDX motif. The proline-rich region contains two highly conserved asparagines (Asn-638 and Asn-652). Mutation of these residues was tolerated, but loss of Asn-638 resulted in the synthesis of truncated LAM, which appeared to lack arabinose branching. All embC alleles that were incapable of complementing LAM production in M. smegmatis were not viable in M. tuberculosis, supporting the hypothesis that LAM itself is essential in M. tuberculosis.

Published
2014

38. Mechanisms of resistance against NITD-916, a direct inhibitor of Mycobacterium tuberculosis InhA

Author

Matthew B, McNeil, Devon, Dennison, Catherine, Shelton, Lindsay, Flint, Aaron, Korkegian, and Tanya, Parish

Subjects
Bacterial Proteins, Genotype, Pyridines, Drug Resistance, Bacterial, Mutation, Antitubercular Agents, Isoniazid, Microbial Sensitivity Tests, Mycobacterium tuberculosis, Oxidoreductases, Promoter Regions, Genetic, Polymorphism, Single Nucleotide, Article
Abstract

Isoniazid inhibits Mycobacterium tuberculosis InhA and is a key component of drug regimens that treat tuberculosis. However, the high rate of resistance against isoniazid is a contributing factor to the emergence of multi-drug resistance strains of M. tuberculosis. The 4-hydroxy-2-pyridine NITD-916 is a direct inhibitor of M. tuberculosis InhA that has comparable efficacy to isoniazid in mouse models of TB infection but a lower frequency of resistance. To characterize resistance mechanisms against NITD-916 we isolated resistant mutants in H37Rv (Euro-American lineage) and HN878 (East-Asian lineage) strains of M. tuberculosis. The resistance frequency was similar in both strains. Mutations were identified in residues within or near to the active of InhA or in the fabG1inhA promoter region. All mutants were resistant to NITD-916 but were not cross resistant to isoniazid, despite homology to SNPs identified in isoniazid resistant clinical isolates.

Published
2017

39. The 7-phenyl benzoxaborole series is active against Mycobacterium tuberculosis

Author

Aaron, Korkegian, Theresa, O'Malley, Yi, Xia, Yasheen, Zhou, David S, Carter, Bjorn, Sunde, Lindsay, Flint, Dean, Thompson, Thomas R, Ioerger, Jim, Sacchettini, M R K, Alley, and Tanya, Parish

Subjects
Boron Compounds, Bacterial Proteins, Dose-Response Relationship, Drug, THP-1 Cells, Drug Resistance, Bacterial, Mutation, Humans, NADH Dehydrogenase, Microbial Sensitivity Tests, Mycobacterium tuberculosis, Bridged Bicyclo Compounds, Heterocyclic, Article
Abstract

We identified a series of novel 7-phenyl benzoxaborole compounds with activity against Mycobacterium tuberculosis. Compounds had a range of activity with inhibitory concentrations (IC90) as low as 5.1 μM and no cytotoxicity against eukaryotic cells (IC50 > 50 μM). Compounds were active against intracellular mycobacteria cultured in THP-1 macrophages. We isolated and characterized resistant mutants with mutations in NADH dehydrogenase (Ndh) or the regulatory protein Mce3R. Mutations suggest that Ndh may be the target of this series.

Published
2017

40. A Novel 6-Benzyl Ether Benzoxaborole Is Active against Mycobacterium tuberculosis

Author

Yong-Kang Zhang, Lindsay Flint, Thomas R. Ioerger, Theresa O’Malley, M. R. K. Alley, Nipul Patel, Aaron Korkegian, James C. Sacchettini, Bjorn Sunde, Tanya Parish, and Yi Xia

Subjects
0301 basic medicine, Antitubercular Agents, Ether, Drug resistance, Microbial Sensitivity Tests, Microbiology, Mycobacterium tuberculosis, 03 medical and health sciences, chemistry.chemical_compound, Mechanisms of Resistance, Cell Line, Tumor, antitubercular, Drug Resistance, Bacterial, Tuberculosis, Multidrug-Resistant, Humans, Pharmacology (medical), Cytotoxicity, IC50, Tuberculosis, Pulmonary, Pharmacology, drug resistance, 030102 biochemistry & molecular biology, biology, Chemistry, Intracellular parasite, Hep G2 Cells, Antimicrobial, biology.organism_classification, In vitro, 3. Good health, 030104 developmental biology, Infectious Diseases, antimicrobial
Abstract

We identified a novel 6-benzyl ether benzoxaborole with potent activity against Mycobacterium tuberculosis . The compound had an MIC of 2 μM in liquid medium. The compound was also able to prevent growth on solid medium at 0.8 μM and was active against intracellular bacteria (50% inhibitory concentration [IC 50 ] = 3.6 μM) without cytotoxicity against eukaryotic cells (IC 50 > 100 μM). We isolated resistant mutants (MIC ≥ 100 μM), which had mutations in Rv1683, Rv3068c, and Rv0047c.

Published
2017

41. The synthesis and evaluation of triazolopyrimidines as anti-tubercular agents

Author

Edison S, Zuniga, Aaron, Korkegian, Steven, Mullen, Erik J, Hembre, Paul L, Ornstein, Guillermo, Cortez, Kallolmay, Biswas, Naresh, Kumar, Jeffrey, Cramer, Thierry, Masquelin, Philip A, Hipskind, Joshua, Odingo, and Tanya, Parish

Subjects
Structure-Activity Relationship, Pyrimidines, Antitubercular Agents, Animals, Humans, Tuberculosis, Anti-tubercular activity, Microbial Sensitivity Tests, Mycobacterium tuberculosis, Triazoles, Triazolopyrimidines, Article, ComputingMethodologies_COMPUTERGRAPHICS
Abstract

Graphical abstract, We identified a di-substituted triazolopyrimidine with anti-tubercular activity against Mycobacterium tuberculosis. Three segments of the scaffold were examined rationally to establish a structure-activity relationship with the goal of improving potency and maintaining good physicochemical properties. A number of compounds displayed sub-micromolar activity against Mycobacterium tuberculosis with no cytotoxicity against eukaryotic cells. Non-substituted aromatic rings at C5 and a two-carbon chain connecting a terminal aromatic at C7 were preferred features; the presence of NH at C7 and a lack of substituent at C2 were essential for potency. We identified compounds with acceptable metabolic stability in rodent and human liver microsomes. Our findings suggest that the easily-synthesized triazolopyrimidines are a promising class of potent anti-tubercular agents and warrant further investigation in our search for new drugs to fight tuberculosis.

Published
2017

42. Discovery of a cofactor-independent inhibitor ofMycobacterium tuberculosisInhA

Author

Xia, Yi, primary, Zhou, Yasheen, additional, Carter, David S, additional, McNeil, Matthew B, additional, Choi, Wai, additional, Halladay, Jason, additional, Berry, Pamela W, additional, Mao, Weimin, additional, Hernandez, Vincent, additional, O'Malley, Theresa, additional, Korkegian, Aaron, additional, Sunde, Bjorn, additional, Flint, Lindsay, additional, Woolhiser, Lisa K, additional, Scherman, Michael S, additional, Gruppo, Veronica, additional, Hastings, Courtney, additional, Robertson, Gregory T, additional, Ioerger, Thomas R, additional, Sacchettini, Jim, additional, Tonge, Peter J, additional, Lenaerts, Anne J, additional, Parish, Tanya, additional, and Alley, MRK, additional

Published
2018
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44. Identification of cyclic hexapeptides natural products with inhibitory potency against Mycobacterium tuberculosis

Author

Singh, Sheo B., primary, Odingo, Joshua, additional, Bailey, Mai A., additional, Sunde, Bjorn, additional, Korkegian, Aaron, additional, O’Malley, Theresa, additional, Ovechkina, Yulia, additional, Ioerger, Thomas R., additional, Sacchettini, James C., additional, Young, Katherine, additional, Olsen, David B., additional, and Parish, Tanya, additional

Published
2018
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45. A Target-Based Whole Cell Screen Approach To Identify Potential Inhibitors of Mycobacterium tuberculosis Signal Peptidase

Author

Shilah A, Bonnett, Juliane, Ollinger, Susantha, Chandrasekera, Stephanie, Florio, Theresa, O'Malley, Megan, Files, Jo-Ann, Jee, James, Ahn, Allen, Casey, Yulia, Ovechkina, David, Roberts, Aaron, Korkegian, and Tanya, Parish

Subjects
phenylhydrazones, Serine Endopeptidases, Antitubercular Agents, Membrane Proteins, Microbial Sensitivity Tests, Mycobacterium tuberculosis, Article, Kinetics, Structure-Activity Relationship, Bacterial Proteins, tuberculosis, signal peptidase, phenotypic screen, Humans, Enzyme Inhibitors
Abstract

The general secretion (Sec) pathway is a conserved essential pathway in bacteria and is the primary route of protein export across the cytoplasmic membrane. During protein export, the signal peptidase LepB catalyzes the cleavage of the signal peptide and subsequent release of mature proteins into the extracellular space. We developed a target-based whole cell assay to screen for potential inhibitors of LepB, the sole signal peptidase in Mycobacterium tuberculosis, using a strain engineered to underexpress LepB (LepB-UE). We screened 72,000 compounds against both the Lep-UE and wild-type (wt) strains. We identified the phenylhydrazone (PHY) series as having higher activity against the LepB-UE strain. We conducted a limited structure–activity relationship determination around a representative PHY compound with differential activity (MICs of 3.0 μM against the LepB-UE strain and 18 μM against the wt); several analogues were less potent against the LepB overexpressing strain. A number of chemical modifications around the hydrazone moiety resulted in improved potency. Inhibition of LepB activity was observed for a number of compounds in a biochemical assay using cell membrane fraction derived from M. tuberculosis. Compounds did not increase cell permeability, dissipate membrane potential, or inhibit an unrelated mycobacterial enzyme, suggesting a specific mode of action related to the LepB secretory mechanism.

Published
2016

46. Corrigendum to 'Mechanisms of resistance against NITD-916, a direct inhibitor of Mycobacterium tuberculosis InhA' [Tuberculosis 107 (December 2017) 133–136]

Author

Devon Dennison, Tanya Parish, Lindsay Flint, Matthew B. McNeil, Aaron Korkegian, and Catherine Shelton

Subjects
Microbiology (medical), Tuberculosis, biology, business.industry, INHA, Immunology, medicine.disease, biology.organism_classification, Microbiology, Virology, Mycobacterium tuberculosis, Infectious Diseases, Medicine, business
Published
2018

48. 8‐Hydroxyquinolines are bactericidal against Mycobacterium tuberculosis.

Author

Odingo, Joshua O., Early, Julie V., Smith, Jake, Johnson, James, Bailey, Mai A., Files, Megan, Guzman, Junitta, Ollinger, Juliane, Korkegian, Aaron, Kumar, Anuradha, Ovechkina, Yulia, and Parish, Tanya

Subjects
MYCOBACTERIUM tuberculosis, STRUCTURE-activity relationships, TUBERCULOSIS
Abstract

There is an urgent need for new treatments effective against Mycobacterium tuberculosis, the causative agent of tuberculosis. The 8‐hydroxyquinoline series is a privileged scaffold with anticancer, antifungal, and antibacterial activities. We conducted a structure–activity relationship study of the series regarding its antitubercular activity using 26 analogs. The 8‐hydroxyquinolines showed good activity against M. tuberculosis, with minimum inhibitory concentrations (MIC90) of <5 μM for some analogs. Small substitutions at C5 resulted in the most potent activity. Substitutions at C2 generally decreased potency, although a sub‐family of 2‐styryl‐substituted analogs retained activity. Representative compounds demonstrated bactericidal activity against replicating M. tuberculosis with >4 log kill at 10× MIC over 14 days. The majority of the compounds demonstrated cytotoxicity (IC50 of <100 μM). Further development of this series as antitubercular agents should address the cytotoxicity liability. However, the 8‐hydroxyquinoline series represents a useful tool for chemical genomics to identify novel targets in M. tuberculosis. [ABSTRACT FROM AUTHOR]

Published
2019
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49. Computational Thermostabilization of an Enzyme

Author

Margaret E. Black, David Baker, Aaron Korkegian, and Barry L. Stoddard

Subjects
Models, Molecular, Protein Denaturation, Protein Folding, Protein Conformation, Molecular Sequence Data, Bacterial growth, Crystallography, X-Ray, Protein Engineering, medicine.disease_cause, Catalysis, Protein Structure, Secondary, Article, Cytosine Deaminase, Metabolic engineering, Transformation, Genetic, Yeasts, Enzyme Stability, Hydrolase, Escherichia coli, medicine, Point Mutation, Computer Simulation, Amino Acid Sequence, chemistry.chemical_classification, Mutation, Binding Sites, Multidisciplinary, Circular Dichroism, Point mutation, Temperature, Protein engineering, Kinetics, Enzyme, chemistry, Biochemistry, Mutagenesis, Site-Directed, Thermodynamics, Protein folding, Monte Carlo Method, Software
Abstract

Thermostabilizing an enzyme while maintaining its activity for industrial or biomedical applications can be difficult with traditional selection methods. We describe a rapid computational approach that identified three mutations within a model enzyme that produced a 10°C increase in apparent melting temperature T m and a 30-fold increase in half-life at 50°C, with no reduction in catalytic efficiency. The effects of the mutations were synergistic, giving an increase in excess of the sum of their individual effects. The redesigned enzyme induced an increased, temperature-dependent bacterial growth rate under conditions that required its activity, thereby coupling molecular and metabolic engineering.

Published
2005

50. A Target-Based Whole Cell Screen Approach To Identify Potential Inhibitors of Mycobacterium tuberculosis Signal Peptidase

Author

Bonnett, Shilah A., primary, Ollinger, Juliane, additional, Chandrasekera, Susantha, additional, Florio, Stephanie, additional, O’Malley, Theresa, additional, Files, Megan, additional, Jee, Jo-Ann, additional, Ahn, James, additional, Casey, Allen, additional, Ovechkina, Yulia, additional, Roberts, David, additional, Korkegian, Aaron, additional, and Parish, Tanya, additional

Published
2016
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