Your search keyword '"globomycin"' showing total 22 results

1. Identification and heterologous expression of the globomycin biosynthetic gene cluster

Author

Daniel Oves-Costales, Tetiana Gren, Eva Baggesgaard Sterndorff, Jesús Martín, Francisco Javier Ortiz-López, Tue S. Jørgensen, Xinglin Jiang, Fernando Román-Hurtado, Fernando Reyes, Olga Genilloud, and Tilmann Weber

Subjects

Globomycin, Signal peptidase II, Cyclic lipodepsipeptide, Genome mining, CRISPR-cBEST, Heterologous expression, Biotechnology, TP248.13-248.65, Biology (General), QH301-705.5

Abstract

Globomycin is a cyclic lipodepsipeptide originally isolated from several Streptomyces species which displays strong and selective antibacterial activity against Gram-negative pathogens. Its mode of action is based on the competitive inhibition of the lipoprotein signal peptidase II (LspA), which is absent in eukaryotes and considered an attractive target for the development of new antibiotics. Despite its interesting biological properties, the gene cluster encoding its biosynthesis has not yet been identified. In this study we employed a genome-mining approach in the globomycin-producing Streptomyces sp. CA-278952 to identify a candidate gene cluster responsible for its biosynthesis. A null mutant was constructed using CRISPR base editing where production was abolished, strongly suggesting its involvement in the biosynthesis. The putative gene cluster was then cloned and heterologously expressed in Streptomyces albus J1074 and Streptomyces coelicolor M1146, therefore unambiguously linking globomycin and its biosynthetic gene cluster. Our work paves the way for the biosynthesis of new globomycin derivatives with improved pharmacological properties.

Published

2023

2. Identification and heterologous expression of the globomycin biosynthetic gene cluster.

Author

Oves-Costales, Daniel, Gren, Tetiana, Sterndorff, Eva Baggesgaard, Martín, Jesús, Ortiz-López, Francisco Javier, Jørgensen, Tue S., Xinglin Jiang, Román-Hurtado, Fernando, Reyes, Fernando, Genilloud, Olga, and Weber, Tilmann

Subjects

*SIGNAL peptidases, *CRISPRS, *ANTIBIOTICS, *LIPOPROTEINS, *PHARMACOLOGY

Abstract

Globomycin is a cyclic lipodepsipeptide originally isolated from several Streptomyces species which displays strong and selective antibacterial activity against Gram-negative pathogens. Its mode of action is based on the competitive inhibition of the lipoprotein signal peptidase II (LspA), which is absent in eukaryotes and considered an attractive target for the development of new antibiotics. Despite its interesting biological properties, the gene cluster encoding its biosynthesis has not yet been identified. In this study we employed a genome-mining approach in the globomycin-producing Streptomyces sp. CA-278952 to identify a candidate gene cluster responsible for its biosynthesis. A null mutant was constructed using CRISPR base editing where production was abolished, strongly suggesting its involvement in the biosynthesis. The putative gene cluster was then cloned and heterologously expressed in Streptomyces albus J1074 and Streptomyces coelicolor M1146, therefore unambiguously linking globomycin and its biosynthetic gene cluster. Our work paves the way for the biosynthesis of new globomycin derivatives with improved pharmacological properties. [ABSTRACT FROM AUTHOR]

Published

2023

3. Deletion of a previously uncharacterized lipoprotein lirL confers resistance to an inhibitor of type II signal peptidase in Acinetobacter baumannii.

Author

Ke-Jung Huang, Pantua, Homer, Jingyu Diao, Skippington, Elizabeth, Volny, Michael, Sandoval, Wendy, Tiku, Varnesh, Yutian Peng, Sagolla, Meredith, Donghong Yan, Jing Kang, Katakam, Anand Kumar, Michaelian, Nairie, Reichelt, Mike, Man-Wah Tan, Austin, Cary D., Min Xu, Hanan, Emily, and Kapadia, Sharookh B.

Subjects

*ACINETOBACTER baumannii, *PEPTIDASE, *PEPTIDES, *GRAM-negative bacteria, *GENETIC counseling, *CELL division

Abstract

Acinetobacter baumannii is a clinically important, predominantly health care-associated gram-negative bacterium with high rates of emerging resistance worldwide. Given the urgent need for novel antibacterial therapies against A. baumannii, we focused on inhibiting lipoprotein biosynthesis, a pathway that is essential for envelope biogenesis in gram-negative bacteria. The natural product globomycin, which inhibits the essential type II signal peptidase prolipoprotein signal peptidase (LspA), is ineffective against wild-type A. baumannii clinical isolates due to its poor penetration through the outer membrane. Here, we describe a globomycin analog, G5132, that is more potent against wild-type and clinical A. baumannii isolates. Mutations leading to G5132 resistance in A. baumannii map to the signal peptide of a single hypothetical gene, which we confirm encodes an alanine-rich lipoprotein and have renamed lirL (prolipoprotein signal peptidase inhibitor resistance lipoprotein). LirL is a highly abundant lipoprotein primarily localized to the inner membrane. Deletion of lirL leads to G5132 resistance, inefficient cell division, increased sensitivity to serum, and attenuated virulence. Signal peptide mutations that confer resistance to G5132 lead to the accumulation of diacylglyceryl-modified LirL prolipoprotein in untreated cells without significant loss in cell viability, suggesting that these mutations overcome a block in lipoprotein biosynthetic flux by decreasing LirL prolipoprotein substrate sensitivity to processing by LspA. This study characterizes a lipoprotein that plays a critical role in resistance to LspA inhibitors and validates lipoprotein biosynthesis as a antibacterial target in A. baumannii. [ABSTRACT FROM AUTHOR]

Published

2022

4. Unstable Mechanisms of Resistance to Inhibitors of Escherichia coli Lipoprotein Signal Peptidase

Author

Homer Pantua, Elizabeth Skippington, Marie-Gabrielle Braun, Cameron L. Noland, Jingyu Diao, Yutian Peng, Susan L. Gloor, Donghong Yan, Jing Kang, Anand Kumar Katakam, Janina Reeder, Georgette M. Castanedo, Keira Garland, Laszlo Komuves, Meredith Sagolla, Cary D. Austin, Jeremy Murray, Yiming Xu, Zora Modrusan, Min Xu, Emily J. Hanan, and Sharookh B. Kapadia

Subjects

heteroresistance, lipoprotein, Lpp, LspA, globomycin, Microbiology, QR1-502

Abstract

ABSTRACT Clinical development of antibiotics with novel mechanisms of action to kill pathogenic bacteria is challenging, in part, due to the inevitable emergence of resistance. A phenomenon of potential clinical importance that is broadly overlooked in preclinical development is heteroresistance, an often-unstable phenotype in which subpopulations of bacterial cells show decreased antibiotic susceptibility relative to the dominant population. Here, we describe a new globomycin analog, G0790, with potent activity against the Escherichia coli type II signal peptidase LspA and uncover two novel resistance mechanisms to G0790 in the clinical uropathogenic E. coli strain CFT073. Building on the previous finding that complete deletion of Lpp, the major Gram-negative outer membrane lipoprotein, leads to globomycin resistance, we also find that an unexpectedly modest decrease in Lpp levels mediated by insertion-based disruption of regulatory elements is sufficient to confer G0790 resistance and increase sensitivity to serum killing. In addition, we describe a heteroresistance phenotype mediated by genomic amplifications of lspA that result in increased LspA levels sufficient to overcome inhibition by G0790 in culture. These genomic amplifications are highly unstable and are lost after as few as two subcultures in the absence of G0790, which places amplification-containing resistant strains at high risk of being misclassified as susceptible by routine antimicrobial susceptibility testing. In summary, our study uncovers two vastly different mechanisms of resistance to LspA inhibitors in E. coli and emphasizes the importance of considering the potential impact of unstable and heterogenous phenotypes when developing antibiotics for clinical use. IMPORTANCE Despite increasing evidence suggesting that antibiotic heteroresistance can lead to treatment failure, the significance of this phenomena in the clinic is not well understood, because many clinical antibiotic susceptibility testing approaches lack the resolution needed to reliably classify heteroresistant strains. Here we present G0790, a new globomycin analog and potent inhibitor of the Escherichia coli type II signal peptidase LspA. We demonstrate that in addition to previously known mechanisms of resistance to LspA inhibitors, unstable genomic amplifications containing lspA can lead to modest yet biologically significant increases in LspA protein levels that confer a heteroresistance phenotype.

Published

2020

5. Components Subcellular Localization: Identification of Lipoproteins Using Globomycin and Radioactive Palmitate.

Author

Buddelmeijer N

Subjects

Cell Membrane, Palmitates, Peptides, Lipoproteins

Abstract

Bacterial lipoproteins are characterized by fatty acids, derived from membrane phospholipids, which are covalently attached to their amino terminus via posttranslational modification in the cytoplasmic membrane. Here, I describe the detection of one of the intermediate forms of lipoprotein, diacylglyceryl-prolipoprotein, using 3 H-palmitate labeling and inhibition of signal peptidase II (Lsp) by globomycin and detection by fluorography., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2024

6. Countering Gram-Negative Antibiotic Resistance: Recent Progress in Disrupting the Outer Membrane with Novel Therapeutics

Author

Kelly M. Lehman and Marcin Grabowicz

Subjects

outer membrane, BamA, LptD, Bam, Lpt, Lol, arylomycin, globomycin, Therapeutics. Pharmacology, RM1-950

Abstract

Gram-negative bacteria shield themselves from antibiotics by producing an outer membrane (OM) that forms a formidable permeability barrier. Multidrug resistance among these organisms is a particularly acute problem that is exacerbated by the OM. The poor penetrance of many available antibiotics prevents their clinical use, and efforts to discover novel classes of antibiotics against Gram-negative bacteria have been unsuccessful for almost 50 years. Recent insights into how the OM is built offer new hope. Several essential multiprotein molecular machines (Bam, Lpt, and Lol) work in concert to assemble the barrier and offer a swathe of new targets for novel therapeutic development. Murepavadin has been at the vanguard of these efforts, but its recently reported phase III clinical trial toxicity has tempered the anticipation of imminent new clinical options. Nonetheless, the many concerted efforts aimed at breaking down the OM barrier provide a source of ongoing optimism for what may soon come through the development pipeline. We will review the current state of drug development against the OM assembly targets, highlighting insightful new discovery approaches and strategies.

Published

2019

7. Unstable Mechanisms of Resistance to Inhibitors of Escherichia coli Lipoprotein Signal Peptidase

Author

Donghong Yan, Keira Garland, Marie-Gabrielle Braun, Yiming Xu, Anand Kumar Katakam, Emily J. Hanan, Yutian Peng, Jing Kang, Meredith Sagolla, Jingyu Diao, Homer Pantua, Cary D. Austin, Cameron L. Noland, Sharookh B. Kapadia, Georgette Castanedo, Zora Modrusan, Min Xu, Susan L. Gloor, Janina Reeder, Elizabeth Skippington, László G. Kömüves, and Jeremy Murray

Subjects

globomycin, medicine.drug_class, Lipoproteins, Antibiotics, Population, Lpp, Biology, Lipoprotein signal peptidase, medicine.disease_cause, Microbiology, Coli strain, Mice, Bacterial Proteins, Enterobacteriaceae, Virology, Drug Resistance, Bacterial, medicine, Escherichia coli, Animals, Aspartic Acid Endopeptidases, Humans, Uropathogenic Escherichia coli, heteroresistance, education, Escherichia coli Infections, Genetics, education.field_of_study, lipoprotein, Pathogenic bacteria, Therapeutics and Prevention, Phenotype, QR1-502, Anti-Bacterial Agents, Mice, Inbred C57BL, LspA, Female, Bacterial outer membrane, Peptides, Research Article

Abstract

Despite increasing evidence suggesting that antibiotic heteroresistance can lead to treatment failure, the significance of this phenomena in the clinic is not well understood, because many clinical antibiotic susceptibility testing approaches lack the resolution needed to reliably classify heteroresistant strains. Here we present G0790, a new globomycin analog and potent inhibitor of the Escherichia coli type II signal peptidase LspA. We demonstrate that in addition to previously known mechanisms of resistance to LspA inhibitors, unstable genomic amplifications containing lspA can lead to modest yet biologically significant increases in LspA protein levels that confer a heteroresistance phenotype., Clinical development of antibiotics with novel mechanisms of action to kill pathogenic bacteria is challenging, in part, due to the inevitable emergence of resistance. A phenomenon of potential clinical importance that is broadly overlooked in preclinical development is heteroresistance, an often-unstable phenotype in which subpopulations of bacterial cells show decreased antibiotic susceptibility relative to the dominant population. Here, we describe a new globomycin analog, G0790, with potent activity against the Escherichia coli type II signal peptidase LspA and uncover two novel resistance mechanisms to G0790 in the clinical uropathogenic E. coli strain CFT073. Building on the previous finding that complete deletion of Lpp, the major Gram-negative outer membrane lipoprotein, leads to globomycin resistance, we also find that an unexpectedly modest decrease in Lpp levels mediated by insertion-based disruption of regulatory elements is sufficient to confer G0790 resistance and increase sensitivity to serum killing. In addition, we describe a heteroresistance phenotype mediated by genomic amplifications of lspA that result in increased LspA levels sufficient to overcome inhibition by G0790 in culture. These genomic amplifications are highly unstable and are lost after as few as two subcultures in the absence of G0790, which places amplification-containing resistant strains at high risk of being misclassified as susceptible by routine antimicrobial susceptibility testing. In summary, our study uncovers two vastly different mechanisms of resistance to LspA inhibitors in E. coli and emphasizes the importance of considering the potential impact of unstable and heterogenous phenotypes when developing antibiotics for clinical use.

Published

2020

8. Deletion of a previously uncharacterized lipoprotein lirL confers resistance to an inhibitor of type II signal peptidase in Acinetobacter baumannii .

Author

Huang KJ, Pantua H, Diao J, Skippington E, Volny M, Sandoval W, Tiku V, Peng Y, Sagolla M, Yan D, Kang J, Katakam AK, Michaelian N, Reichelt M, Tan MW, Austin CD, Xu M, Hanan E, and Kapadia SB

Subjects

Peptides pharmacology, Protein Sorting Signals genetics, Acinetobacter baumannii drug effects, Acinetobacter baumannii enzymology, Acinetobacter baumannii genetics, Anti-Bacterial Agents pharmacology, Aspartic Acid Endopeptidases genetics, Bacterial Proteins genetics, Drug Resistance, Bacterial genetics, Furans pharmacology, Gene Deletion, Lipoproteins biosynthesis, Lipoproteins genetics, Protease Inhibitors pharmacology, Pyridines pharmacology

Abstract

Acinetobacter baumannii is a clinically important, predominantly health care-associated gram-negative bacterium with high rates of emerging resistance worldwide. Given the urgent need for novel antibacterial therapies against A. baumannii , we focused on inhibiting lipoprotein biosynthesis, a pathway that is essential for envelope biogenesis in gram-negative bacteria. The natural product globomycin, which inhibits the essential type II signal peptidase prolipoprotein signal peptidase (LspA), is ineffective against wild-type A. baumannii clinical isolates due to its poor penetration through the outer membrane. Here, we describe a globomycin analog, G5132, that is more potent against wild-type and clinical A. baumannii isolates. Mutations leading to G5132 resistance in A. baumannii map to the signal peptide of a single hypothetical gene, which we confirm encodes an alanine-rich lipoprotein and have renamed lirL (prolipoprotein signal peptidase inhibitor resistance lipoprotein). LirL is a highly abundant lipoprotein primarily localized to the inner membrane. Deletion of lirL leads to G5132 resistance, inefficient cell division, increased sensitivity to serum, and attenuated virulence. Signal peptide mutations that confer resistance to G5132 lead to the accumulation of diacylglyceryl-modified LirL prolipoprotein in untreated cells without significant loss in cell viability, suggesting that these mutations overcome a block in lipoprotein biosynthetic flux by decreasing LirL prolipoprotein substrate sensitivity to processing by LspA. This study characterizes a lipoprotein that plays a critical role in resistance to LspA inhibitors and validates lipoprotein biosynthesis as a antibacterial target in A. baumannii .

Published

2022

9. Conformational Analysis of Globomycin With a Signal Peptidase II Inhibitory Activity Using Molecular Dynamics Simulation.

Author

Kiho, Toshihiro, Iwata, Yoriko, Kogen, Hiroshi, and Miyamoto, Shuichi

Subjects

*CONFORMATIONAL analysis, *SIGNAL peptidases, *MOLECULES, *SIMULATION methods & models, *GRAM-negative bacteria, *CELL membranes

Abstract

Globomycin (1), a 19-membered cyclic depsipeptide, exhibited an antibiotic activity against gram-negative bacteria by inhibiting signal peptidase II in the cytoplasmic membrane. Although only one conformation of 1 was observed for the crystal structure, it was revealed by 1H NMR spectroscopic analysis that 1 exists as a mixture of two rotational isomers in solution (CDCl3 and CD3OD). A conformational analysis of 1 was, therefore, performed by high-temperature molecular dynamics simulation in combination with 1H NMR analysis to elucidate the conformations in solution. The relative ratio of the major and minor isomers present, which differs depending on the solvent, was then derived from their relative energy differences obtained in the conformational analysis. The difference in the relative ratios corresponded with that calculated from the 1H NMR analysis. Finally, the predicted conformations in solution were compared with that of the X-ray crystal structure to find local and global differences that characterize these conformations. [ABSTRACT FROM AUTHOR]

Published

2003

10. Total synthesis and NMR conformational study of signal peptidase II inhibitors, globomycin and SF-1902 A5

Author

Kiho, Toshihiro, Nakayama, Mizuka, and Kogen, Hiroshi

Subjects

*ANTIBIOTICS, *MACROCYCLIC compounds, *NUCLEAR magnetic resonance

Abstract

A stereoselective total synthesis of an antibiotic, globomycin (1a), and its congener, SF-1902 A5 (1b), was achieved. Two convergent macrocyclization routes via macrolactamization or macrolactonization to form 1a are described. A conformational study by means of NMR spectroscopy was performed in several solvents. The 1H NMR spectrum of 1a indicated that the amide proton of only the l-allo-Thr residue was involved in the hydrogen bonding. The structure in solution phase was different from the X-ray structure. [Copyright &y& Elsevier]

Published

2003

11. Inhibition of colicin synthesis by the antibiotic globomycin.

Author

Cavard, Danièle

Abstract

The antibiotic globomycin, an inhibitor of LspA (the lipoprotein signal peptidase), inhibited synthesis of colicin by Escherichia coli cells grown in rich medium. This inhibition was stronger in cells with mutation(s) within either the colicin operon, which is located on a plasmid, or the host chromosome. This phenotype was called Gbc (globomycin blocks colicin synthesis). The Gbc phenotype was affected by growth conditions since it was partially or totally suppressed in cells subjected to high temperatures, treated with sodium azide, or grown in minimal medium. The Gbc phenotype observed with colicin-A-producing cells was more severe in strains carrying plasmids with a deletion within caa (the first gene of the colicin A operon), which encodes colicin A, than in cells with the wild-type caa gene. The Gbc phenotype was alleviated by a null mutation in the degP gene encoding the DegP/HtrA protease, abolished by a null mutation in the lpp gene encoding the murein-lipoprotein, and enhanced by a mutation in the pldA gene encoding the outer membrane phospholipase A. Transcription of the colicin A operon was blocked in cells exhibiting the Gbc phenotype as evidenced by rifampicin treatment of induced cells. This phenotype suggests that either a lipoprotein or a protein involved in lipoprotein metabolism might be involved in the regulation of the expression of the colicin operons and that the colicin A structural gene might play a role in the regulation of transcription of the colicin A operon. [ABSTRACT FROM AUTHOR]

Published

1998

12. Identification of Lipoproteins Using Globomycin and Radioactive Palmitate

Author

Nienke Buddelmeijer, Biologie et Génétique de la Paroi bactérienne - Biology and Genetics of Bacterial Cell Wall (BGPB), Institut Pasteur [Paris] (IP), Laure Journet et Eric Cascales, and Institut Pasteur [Paris]

Subjects

0301 basic medicine, chemistry.chemical_classification, Apolipoprotein B, biology, Tris-tricine gel electrophoresis, 3H-palmitate labeling, [SDV.MP.BAC]Life Sciences [q-bio]/Microbiology and Parasitology/Bacteriology, Globomycin, 3. Good health, Turn (biochemistry), 03 medical and health sciences, 030104 developmental biology, Enzyme, Membrane, chemistry, Biochemistry, Cytoplasm, Posttranslational modification, biology.protein, lipids (amino acids, peptides, and proteins), [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Fluorography, Lipoprotein

Abstract

International audience; Bacterial lipoproteins are characterized by fatty acids that are covalently attached to their amino terminus via posttranslational modification in the cytoplasmic membrane. Three enzymatic steps are involved in the synthesis of mature triacylated lipoprotein: prolipoprotein converts into diacylglyceryl-prolipoprotein that in turn converts into apolipoprotein, which is finally converted into mature triacylated lipoprotein. Here we describe the detection of one of these intermediate forms of lipoprotein, diacylglyceryl-prolipoprotein, using (3)H-palmitate labeling and inhibition by globomycin and detection by fluorography.

Published

2017

13. Optimization of globomycin analogs as novel gram-negative antibiotics.

Author

Garland, Keira, Pantua, Homer, Braun, Marie-Gabrielle, Burdick, Daniel J., Castanedo, Georgette M., Chen, Yi-Chen, Cheng, Yun-Xing, Cheong, Jonathan, Daniels, Blake, Deshmukh, Gauri, Fu, Yuhong, Gibbons, Paul, Gloor, Susan L., Hua, Rongbao, Labadie, Sharada, Liu, Xiongcai, Pastor, Richard, Stivala, Craig, Xu, Min, and Xu, Yiming

Subjects

*ANTIBIOTICS, *GRAM-negative bacteria, *PEPTIDASE, *NATURAL products, *DEPSIPEPTIDES, *BASIC needs, *TARGETED drug delivery

Abstract

Discovery of novel classes of Gram-negative antibiotics with activity against multi-drug resistant infections is a critical unmet need. As an essential member of the lipoprotein biosynthetic pathway, lipoprotein signal peptidase II (LspA) is an attractive target for antibacterial drug discovery, with the natural product inhibitor globomycin offering a modestly-active starting point. Informed by structure-based design, the globomycin depsipeptide was optimized to improve activity against E. coli. Backbone modifications, together with adjustment of physicochemical properties, afforded potent compounds with good in vivo pharmacokinetic profiles. Optimized compounds such as 51 (E. coli MIC 3.1 μM) and 61 (E. coli MIC 0.78 μM) demonstrate broad spectrum activity against gram-negative pathogens and may provide opportunities for future antibiotic discovery. [ABSTRACT FROM AUTHOR]

Published

2020

14. Unstable Mechanisms of Resistance to Inhibitors of Escherichia coli Lipoprotein Signal Peptidase.

Author

Pantua H, Skippington E, Braun MG, Noland CL, Diao J, Peng Y, Gloor SL, Yan D, Kang J, Katakam AK, Reeder J, Castanedo GM, Garland K, Komuves L, Sagolla M, Austin CD, Murray J, Xu Y, Modrusan Z, Xu M, Hanan EJ, and Kapadia SB

Subjects

Animals, Aspartic Acid Endopeptidases genetics, Bacterial Proteins genetics, Enterobacteriaceae classification, Enterobacteriaceae drug effects, Escherichia coli drug effects, Escherichia coli enzymology, Escherichia coli genetics, Escherichia coli Infections microbiology, Female, Humans, Mice, Mice, Inbred C57BL, Peptides chemistry, Peptides pharmacology, Uropathogenic Escherichia coli genetics, Uropathogenic Escherichia coli pathogenicity, Anti-Bacterial Agents pharmacology, Aspartic Acid Endopeptidases antagonists & inhibitors, Bacterial Proteins antagonists & inhibitors, Drug Resistance, Bacterial genetics, Lipoproteins metabolism, Uropathogenic Escherichia coli drug effects, Uropathogenic Escherichia coli enzymology

Abstract

Clinical development of antibiotics with novel mechanisms of action to kill pathogenic bacteria is challenging, in part, due to the inevitable emergence of resistance. A phenomenon of potential clinical importance that is broadly overlooked in preclinical development is heteroresistance, an often-unstable phenotype in which subpopulations of bacterial cells show decreased antibiotic susceptibility relative to the dominant population. Here, we describe a new globomycin analog, G0790, with potent activity against the Escherichia coli type II signal peptidase LspA and uncover two novel resistance mechanisms to G0790 in the clinical uropathogenic E. coli strain CFT073. Building on the previous finding that complete deletion of Lpp, the major Gram-negative outer membrane lipoprotein, leads to globomycin resistance, we also find that an unexpectedly modest decrease in Lpp levels mediated by insertion-based disruption of regulatory elements is sufficient to confer G0790 resistance and increase sensitivity to serum killing. In addition, we describe a heteroresistance phenotype mediated by genomic amplifications of lspA that result in increased LspA levels sufficient to overcome inhibition by G0790 in culture. These genomic amplifications are highly unstable and are lost after as few as two subcultures in the absence of G0790, which places amplification-containing resistant strains at high risk of being misclassified as susceptible by routine antimicrobial susceptibility testing. In summary, our study uncovers two vastly different mechanisms of resistance to LspA inhibitors in E. coli and emphasizes the importance of considering the potential impact of unstable and heterogenous phenotypes when developing antibiotics for clinical use. IMPORTANCE Despite increasing evidence suggesting that antibiotic heteroresistance can lead to treatment failure, the significance of this phenomena in the clinic is not well understood, because many clinical antibiotic susceptibility testing approaches lack the resolution needed to reliably classify heteroresistant strains. Here we present G0790, a new globomycin analog and potent inhibitor of the Escherichia coli type II signal peptidase LspA. We demonstrate that in addition to previously known mechanisms of resistance to LspA inhibitors, unstable genomic amplifications containing lspA can lead to modest yet biologically significant increases in LspA protein levels that confer a heteroresistance phenotype., (Copyright © 2020 Pantua et al.)

Published

2020

15. Bacterial Lipoprotein Biosynthetic Pathway as a Potential Target for Structure-based Design of Antibacterial Agents.

Author

Xia J, Feng B, Wen G, Xue W, Ma G, Zhang H, and Wu S

Subjects

Bacteria, Bacterial Proteins, Biosynthetic Pathways, Drug Design, Lipoproteins, Anti-Bacterial Agents therapeutic use

Abstract

Background: Antibiotic resistance is currently a serious problem for global public health. To this end, discovery of new antibacterial drugs that interact with novel targets is important. The biosynthesis of lipoproteins is vital to bacterial survival and its inhibitors have shown efficacy against a range of bacteria, thus bacterial lipoprotein biosynthetic pathway is a potential target., Methods: At first, the literature that covered the basic concept of bacterial lipoprotein biosynthetic pathway as well as biochemical characterization of three key enzymes was reviewed. Then, the recently resolved crystal structures of the three enzymes were retrieved from Protein Data Bank (PDB) and the essential residues in the active sites were analyzed. Lastly, all the available specific inhibitors targeting this pathway and their Structure-activity Relationship (SAR) were discussed., Results: We briefly introduce the bacterial lipoprotein biosynthetic pathway and describe the structures and functions of three key enzymes in detail. In addition, we present much knowledge on ligand recognition that may facilitate structure-based drug design. Moreover, we focus on the SAR of LspA inhibitors and discuss their potency and drug-likeness., Conclusion: This review presents a clear background of lipoprotein biosynthetic pathway and provides practical clues for structure-based drug design. In particular, the most up-to-date knowledge on the SAR of lead compounds targeting this pathway would be a good reference for discovery of a novel class of antibacterial agents., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2020

16. Countering Gram-Negative Antibiotic Resistance: Recent Progress in Disrupting the Outer Membrane with Novel Therapeutics.

Author

Lehman, Kelly M. and Grabowicz, Marcin

Subjects

DRUG resistance in bacteria, MULTIDRUG resistance, GRAM-negative bacteria, DRUG development, THERAPEUTICS

Abstract

Gram-negative bacteria shield themselves from antibiotics by producing an outer membrane (OM) that forms a formidable permeability barrier. Multidrug resistance among these organisms is a particularly acute problem that is exacerbated by the OM. The poor penetrance of many available antibiotics prevents their clinical use, and efforts to discover novel classes of antibiotics against Gram-negative bacteria have been unsuccessful for almost 50 years. Recent insights into how the OM is built offer new hope. Several essential multiprotein molecular machines (Bam, Lpt, and Lol) work in concert to assemble the barrier and offer a swathe of new targets for novel therapeutic development. Murepavadin has been at the vanguard of these efforts, but its recently reported phase III clinical trial toxicity has tempered the anticipation of imminent new clinical options. Nonetheless, the many concerted efforts aimed at breaking down the OM barrier provide a source of ongoing optimism for what may soon come through the development pipeline. We will review the current state of drug development against the OM assembly targets, highlighting insightful new discovery approaches and strategies. [ABSTRACT FROM AUTHOR]

Published

2019

17. Identification of Lipoproteins Using Globomycin and Radioactive Palmitate.

Author

Buddelmeijer N

Subjects

Electrophoresis, Polyacrylamide Gel, Escherichia coli Proteins chemistry, Escherichia coli Proteins metabolism, Immunoprecipitation, Isotope Labeling, Lipoproteins antagonists & inhibitors, Lipoproteins chemistry, Lipoproteins metabolism, Palmitates, Peptides chemistry, Peptides pharmacology, Radioactive Tracers

Abstract

Bacterial lipoproteins are characterized by fatty acids that are covalently attached to their amino terminus via posttranslational modification in the cytoplasmic membrane. Three enzymatic steps are involved in the synthesis of mature triacylated lipoprotein: prolipoprotein converts into diacylglyceryl-prolipoprotein that in turn converts into apolipoprotein, which is finally converted into mature triacylated lipoprotein. Here we describe the detection of one of these intermediate forms of lipoprotein, diacylglyceryl-prolipoprotein, using 3 H-palmitate labeling and inhibition by globomycin and detection by fluorography.

Published

2017

18. High-level expression of the colicin A lysis protein

Author

Cavard, Daniele, Howard, S. Peter, Lloubes, Roland, and Lazdunski, Claude

Published

1989

19. Translocation of colicin E1 through cytoplasmic membrane ofEscherichia coli

Author

Mamoru Yamada, Atsushi Nakazawa, and Toru Miki

Subjects

Colicin E1, Protein export, Maltose-binding protein, Biophysics, Colicins, Signal sequence, Chromosomal translocation, medicine.disease_cause, Biochemistry, Globomycin, Cell membrane, Fusion gene, Structural Biology, Escherichia coli, Genetics, medicine, Lipoprotein, Molecular Biology, ColE1, biology, Cell Membrane, Biological Transport, Cell Biology, medicine.anatomical_structure, Genes, Bacterial, Colicin, biology.protein, bacteria, lipids (amino acids, peptides, and proteins), Bacterial outer membrane

Abstract

The product of the malE—lacZ gene fusion was reported to compete with some proteins including outer membrane lipoprotein in the protein translocation across the Echerichia coli membrane. The fusion product also inhibited colicin E1 export. Furthermore, globomycin, which accumulated prolipoprotein in the membrane, inhibited the translocation of colicin E1 in the wild-type cells, but not in lipoprotein-negative mutant cells. Since colicin E1 contains the internal signal-like sequence [Proc. Natl. Acad. Sci. USA (1982) 79, 2827–2831], these results suggest that colicin E1 is exported by the aid of this sequence at a common site for maltose-binding protein and lipoprotein translocation.

Published

1982

20. Accumulation of glyceride-modified pre-penicillinase of Bacillus licheniformis in Escherichia coli treated with globomycin

Author

Musaddeq Hussain and J. Oliver Lampen

Subjects

Signal peptide, Chemical Phenomena, medicine.medical_treatment, Biophysics, Bacillus, Biology, medicine.disease_cause, Lipid modification, Biochemistry, beta-Lactamases, Globomycin, Microbiology, Glycerides, Structure-Activity Relationship, Structural Biology, Genetics, medicine, Escherichia coli, Bacillus licheniformis, Signal peptidase, Molecular Biology, Enzyme Precursors, Protease, Membrane Proteins, Pre-penicillinase, Cell Biology, Penicillinase, biology.organism_classification, Anti-Bacterial Agents, Chemistry, lipids (amino acids, peptides, and proteins), Bacterial outer membrane, Peptides, Cysteine

Abstract

The membrane penicillinase of Bacillus licheniformis is a glyceride-cysteine lipoprotein whose NH2 terminus is analogous to the major outer membrane lipoprotein of Escherichia coli. When E. coli cells producing B. licheniformis penicillinase were treated with the antibiotic, globomycin, a precursor of the penicillinase, pre-penicillinase, accumulated in the cell. It could be immunoprecipitated with anti-penicillinase antibodies; it contained palmitate; and one of its two cysteine residues was modified by glycerol. The action of globomycin, probably indirectly, also activates protease which acts differently on the pre-penicillinase than does the signal peptidase. The results strongly indicate that the pre-penicillinase is processed by the globomycin-sensitive signal peptidase in E. coli, and the modification of precursor by lipid precedes removal of the signal peptide as it does with the membrane lipoproteins of E. coli.

21. Lipoprotein Nature of Bacillus licheniformis Membrane Penicillinase

Author

Caulfield, Michael P. and Lampen, J. Oliver

Published

1981

22. Post-Translational Modification and Processing of Escherichia coli Prolipoprotein in vitro

Author

Tokunaga, Masao, Tokunaga, Hiroko, and Wu, Henry C.

Published

1982