Your search keyword '"Laurent, Chesnel"' showing total 39 results

1. ADS024, a single-strain live biotherapeutic product of Bacillus velezensis alleviates dextran sulfate-mediated colitis in mice, protects human colonic epithelial cells against apoptosis, and maintains epithelial barrier function

Author

Sophie Irwin, Andrea Chupina Estrada, Becca Nelson, Ashlen Bullock, Berkeley Limketkai, Wendy Ho, Susan Acton, Laurent Chesnel, and Hon Wai Koon

Subjects

inflammation, anti-inflammatory, inflammatory bowel disease (IBD), GI, biologic, therapy, Microbiology, QR1-502

Abstract

Epithelial cell apoptosis and compromised gut barrier function are features of inflammatory bowel disease. ADS024 is a single-strain live biotherapeutic product (LBP) of Bacillus velezensis under development for treating ulcerative colitis (UC). The cytoprotective effects of the sterile filtrate of ADS024’s secreted products on UC patient-derived colonic tissues, human primary colonic epithelial cells (HPEC), and human colonic epithelial T84 cells were evaluated. ADS024 filtrate significantly inhibited apoptosis and inflammation with reduced Bcl-2 Associated X-protein (BAX) and tumor necrosis factor (TNF) mRNA expression in fresh colonic explants from UC patients. Exposure to UC patient-derived serum exosomes (UCSE) induced apoptosis with increased cleaved caspase 3 protein expression in HPECs. ADS024 filtrate diminished the UCSE-mediated apoptosis by inhibiting cleaved caspase 3. TNFα and interferon-gamma (IFNγ) damaged epithelial barrier integrity with reduced transepithelial electrical resistance (TEER). ADS024 filtrate partially attenuated the TEER reduction and restored tight junction protein 1 (TJP1) expression. Oral live ADS024 treatment reduced weight loss, disease activity, colonic mucosal injury, and colonic expression of interleukin 6 (IL-6) and TNFα in dextran sodium sulfate (DSS)-treated mice with colitis. Thus, ADS024 may protect the colonic epithelial barrier in UC via anti-inflammatory, anti-apoptotic, and tight-junction protection mechanisms.

Published

2024

2. Identification of ADS024, a newly characterized strain of Bacillus velezensis with direct Clostridiodes difficile killing and toxin degradation bio-activities

Author

Michelle M. O’Donnell, James W. Hegarty, Brian Healy, Sarah Schulz, Calum J. Walsh, Colin Hill, R. Paul Ross, Mary C. Rea, Ronald Farquhar, and Laurent Chesnel

Subjects

Medicine, Science

Abstract

Abstract Clostridioides difficile infection (CDI) remains a significant health threat worldwide. C. difficile is an opportunistic, toxigenic pathogen that takes advantage of a disrupted gut microbiome to grow and produce signs and symptoms ranging from diarrhea to pseudomembranous colitis. Antibiotics used to treat C. difficile infection are usually broad spectrum and can further disrupt the commensal gut microbiota, leaving patients susceptible to recurrent C. difficile infection. There is a growing need for therapeutic options that can continue to inhibit the outgrowth of C. difficile after antibiotic treatment is completed. Treatments that degrade C. difficile toxins while having minimal collateral impact on gut bacteria are also needed to prevent recurrence. Therapeutic bacteria capable of producing a range of antimicrobial compounds, proteases, and other bioactive metabolites represent a potentially powerful tool for preventing CDI recurrence following resolution of symptoms. Here, we describe the identification and initial characterization of ADS024 (formerly ART24), a novel therapeutic bacterium that can kill C. difficile in vitro with limited impact on other commensal bacteria. In addition to directly killing C. difficile, ADS024 also produces proteases capable of degrading C. difficile toxins, the drivers of symptoms associated with most cases of CDI. ADS024 is in clinical development for the prevention of CDI recurrence as a single-strain live biotherapeutic product, and this initial data set supports further studies aimed at evaluating ADS024 in future human clinical trials.

Published

2022

3. ADS024, a Bacillus velezensis strain, protects human colonic epithelial cells against C. difficile toxin-mediated apoptosis

Author

Ying Xie, Andrea Chupina Estrada, Becca Nelson, Hanping Feng, Charalabos Pothoulakis, Laurent Chesnel, and Hon Wai Koon

Subjects

infection, biologic, therapy, single-strain live biotherapeutic product, apoptosis, C. difficile, Microbiology, QR1-502

Abstract

Clostridioides difficile infection (CDI) causes intestinal injury. Toxin A and toxin B cause intestinal injury by inducing colonic epithelial cell apoptosis. ADS024 is a Bacillus velezensis strain in development as a single-strain live biotherapeutic product (SS-LBP) to prevent the recurrence of CDI following the completion of standard antibiotic treatment. We evaluated the protective effects of the sterile filtrate and ethyl acetate extract of conditioned media from ADS024 and DSM7 (control strain) against mucosal epithelial injury in toxin-treated human colonic tissues and apoptosis in toxin-treated human colonic epithelial cells. Ethyl acetate extracts were generated from conditioned culture media from DSM7 and ADS024. Toxin A and toxin B exposure caused epithelial injury in fresh human colonic explants. The sterile filtrate of ADS024, but not DSM7, prevented toxin B-mediated epithelial injury in fresh human colonic explants. Both sterile filtrate and ethyl acetate extract of ADS024 prevented toxin-mediated apoptosis in human colonic epithelial cells. The anti-apoptotic effects of ADS024 filtrate and ethyl acetate extract were dependent on the inhibition of caspase 3 cleavage. The sterile filtrate, but not ethyl acetate extract, of ADS024 partially degraded toxin B. ADS024 inhibits toxin B-mediated apoptosis in human colonic epithelial cells and colonic explants.

Published

2023

4. Characterization of Clostridioides difficile isolates recovered from two Phase 3 surotomycin treatment trials by restriction endonuclease analysis, PCR ribotyping and antimicrobial susceptibilities

Author

Laurent Chesnel, Julia Nary, Adam Cheknis, Susan P Sambol, Richard V. Goering, Stuart Johnson, Dominique Devaris, Suzanne E. Dale, and Diane M. Citron

Subjects

Microbiology (medical), Canada, Veterinary medicine, Asia, Population, Microbial Sensitivity Tests, Peptides, Cyclic, Polymerase Chain Reaction, Ribotyping, Agar dilution, Lipopeptides, Anti-Infective Agents, Clostridioides, Moxifloxacin, Prohibitins, medicine, Humans, Pharmacology (medical), Israel, education, Pharmacology, education.field_of_study, Molecular epidemiology, Clostridioides difficile, business.industry, DNA Restriction Enzymes, South America, Clostridium difficile, Anti-Bacterial Agents, Europe, Metronidazole, Infectious Diseases, North America, Clostridium Infections, Vancomycin, business, medicine.drug

Abstract

Objectives To investigate the molecular epidemiology and antimicrobial susceptibility of Clostridioides difficile isolates from patients with C. difficile infection (CDI) from two Phase 3 clinical trials of surotomycin. Methods In both trials [Protocol MK-4261-005 (NCT01597505) conducted across Europe, North America and Israel; and Protocol MK-4261-006 (NCT01598311) conducted across North America, Asia-Pacific and South America], patients with CDI were randomized (1:1) to receive oral surotomycin (250 mg twice daily) or oral vancomycin (125 mg four times per day) for 10 days. Stool samples were collected at baseline and C. difficile isolates were characterized by restriction endonuclease analysis (REA) and PCR ribotyping. Susceptibility testing was performed by agar dilution, according to CLSI recommendations. Results In total, 1147 patients were included in the microbiological modified ITT population. Of 992 recovered isolates, 922 (92.9%) were typed. There was a high association between REA groups and their corresponding predominant PCR ribotype (RT) for BI, DH, G and CF strains. REA group A showed more diverse PCR RTs. Overall, the most common strain was BI/RT027 (20.3%) followed by Y/RT014/020 (15.0%) and DH/RT106 (7.2%). The BI/RT027 strain was particularly prevalent in Europe (29.9%) and Canada (23.6%), with lower prevalence in the USA (16.8%) and Australia/New Zealand (3.4%). Resistance was most prevalent in the BI/RT027 strain, particularly to metronidazole, vancomycin and moxifloxacin. Conclusions A wide variation in C. difficile strains, both within and across different geographical regions, was documented by both REA and ribotyping, which showed overall good correlation.

Published

2020

5. Identification of ADS024, a newly characterized strain of Bacillus velezensis with direct Clostridiodes difficile killing and toxin degradation bio-activities

Author

Michelle M, O'Donnell, James W, Hegarty, Brian, Healy, Sarah, Schulz, Calum J, Walsh, Colin, Hill, R Paul, Ross, Mary C, Rea, Ronald, Farquhar, and Laurent, Chesnel

Subjects

Clostridioides difficile, Clostridium Infections, Humans, Bacillus, Anti-Bacterial Agents, Peptide Hydrolases

Abstract

Clostridioides difficile infection (CDI) remains a significant health threat worldwide. C. difficile is an opportunistic, toxigenic pathogen that takes advantage of a disrupted gut microbiome to grow and produce signs and symptoms ranging from diarrhea to pseudomembranous colitis. Antibiotics used to treat C. difficile infection are usually broad spectrum and can further disrupt the commensal gut microbiota, leaving patients susceptible to recurrent C. difficile infection. There is a growing need for therapeutic options that can continue to inhibit the outgrowth of C. difficile after antibiotic treatment is completed. Treatments that degrade C. difficile toxins while having minimal collateral impact on gut bacteria are also needed to prevent recurrence. Therapeutic bacteria capable of producing a range of antimicrobial compounds, proteases, and other bioactive metabolites represent a potentially powerful tool for preventing CDI recurrence following resolution of symptoms. Here, we describe the identification and initial characterization of ADS024 (formerly ART24), a novel therapeutic bacterium that can kill C. difficile in vitro with limited impact on other commensal bacteria. In addition to directly killing C. difficile, ADS024 also produces proteases capable of degrading C. difficile toxins, the drivers of symptoms associated with most cases of CDI. ADS024 is in clinical development for the prevention of CDI recurrence as a single-strain live biotherapeutic product, and this initial data set supports further studies aimed at evaluating ADS024 in future human clinical trials.

Published

2021

6. LPAR3: a shared target for neurodegenerative diseases?

Author

Susan Acton and Laurent Chesnel

Subjects

Neurology. Diseases of the nervous system, RC346-429

Published

2025

7. S1065 ADS024, a Single Strain Live Biotherapeutic Product, Reduces Colonic Inflammation in DSS-Induced Colitis When Dosed Twice Daily

Author

Laurent Chesnel and Susan Acton

Subjects

Hepatology, Gastroenterology

Published

2022

8. 891: ART24, A BACILLUS VELEZENSIS STRAIN, PROTECTS HUMAN COLONIC EPITHELIAL CELLS AGAINST CLOSTRIDIOIDES DIFFICILE TOXINMEDIATED APOPTOSIS

Author

Ying Xie, Laurent Chesnel, Charalabos Pothoulakis, and Hon Wai Koon

Subjects

Hepatology, Gastroenterology

Published

2022

9. The capping domain in RalF regulates effector functions.

Author

Eric Alix, Laurent Chesnel, Brad J Bowzard, Aimee M Tucker, Anna Delprato, Jacqueline Cherfils, David O Wood, Richard A Kahn, and Craig R Roy

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

The Legionella pneumophila effector protein RalF functions as a guanine nucleotide exchange factor (GEF) that activates the host small GTPase protein ADP-ribosylation factor (Arf), and recruits this host protein to the vacuoles in which this pathogen resides. GEF activity is conferred by the Sec7 domain located in the N-terminal region of RalF. Structural studies indicate that the C-terminal region of RalF makes contacts with residues in the Sec7 domain important for Arf interactions. Theoretically, the C-terminal region of RalF could prevent nucleotide exchange activity by blocking the ability of Arf to interact with the Sec7 domain. For this reason, the C-terminal region of RalF has been termed a capping domain. Here, the role of the RalF capping domain was investigated by comparing biochemical and effector activities mediated by this domain in both the Legionella RalF protein (LpRalF) and in a RalF ortholog isolated from the unrelated intracellular pathogen Rickettsia prowazekii (RpRalF). These data indicate that both RalF proteins contain a functional Sec7 domain and that the capping domain regulates RalF GEF activity. The capping domain has intrinsic determinants that mediate localization of the RalF protein inside of host cells and confer distinct effector activities. Localization mediated by the capping domain of LpRalF enables the GEF to modulate membrane transport in the secretory pathway, whereas, the capping domain of RpRalF enables this bacterial GEF to modulate actin dynamics occurring near the plasma membrane. Thus, these data reveal that divergence in the function of the C-terminal capping domain alters the in vivo functions of the RalF proteins.

Published

2012

10. Analysis of Clostridium difficile biofilms: imaging and antimicrobial treatment

Author

Laura Boegli, Laurent Chesnel, Philip S. Stewart, Elinor deLancey Pulcini, Garth A. James, and Steve T. Fisher

Subjects

0301 basic medicine, Microbiology (medical), medicine.drug_class, 030106 microbiology, Antibiotics, Colony Count, Microbial, Surotomycin, Microbial Sensitivity Tests, Peptides, Cyclic, Microbiology, Lipopeptides, 03 medical and health sciences, chemistry.chemical_compound, Vancomycin, Metronidazole, medicine, Humans, Pharmacology (medical), Fidaxomicin, Spores, Bacterial, Pharmacology, Clostridioides difficile, Chemistry, Biofilm, Biological Transport, biochemical phenomena, metabolism, and nutrition, Clostridium difficile, Antimicrobial, Anti-Bacterial Agents, Aminoglycosides, Infectious Diseases, Biofilms, Microscopy, Electron, Scanning, medicine.drug

Abstract

Background Clostridium difficile, a spore-forming Gram-positive anaerobic bacillus, is the most common causative agent of healthcare-associated diarrhoea. Formation of biofilms may protect C. difficile against antibiotics, potentially leading to treatment failure. Furthermore, bacterial spores or vegetative cells may linger in biofilms in the gut causing C. difficile infection recurrence. Objectives In this study, we evaluated and compared the efficacy of four antibiotics (fidaxomicin, surotomycin, vancomycin and metronidazole) in penetrating C. difficile biofilms and killing vegetative cells. Methods C. difficile biofilms grown initially for 48 or 72 h using the colony biofilm model were then treated with antibiotics at a concentration of 25 × MIC for 24 h. Vegetative cells and spores were enumerated. The effect of treatment on biofilm structure was studied by scanning electron microscopy (SEM). The ability of fidaxomicin and surotomycin to penetrate biofilms was studied using fluorescently tagged antibiotics. Results Both surotomycin and fidaxomicin were significantly more effective than vancomycin or metronidazole (P

Published

2017

11. Surotomycin versus vancomycin in adults with Clostridium difficile infection: primary clinical outcomes from the second pivotal, randomized, double-blind, Phase 3 trial

Author

U Stoutenburgh, Dalya Guris, Yoshihiko Murata, Mandy Jin, Laurent Chesnel, Kajal B. Larson, P Daley, Sahil Khanna, Thomas J. Louie, J E Lutz, and Adedayo Adedoyin

Subjects

Adult, 0301 basic medicine, Microbiology (medical), medicine.medical_specialty, Adolescent, 030106 microbiology, Administration, Oral, Surotomycin, Placebo, Peptides, Cyclic, law.invention, Placebos, Lipopeptides, Young Adult, 03 medical and health sciences, chemistry.chemical_compound, Double-Blind Method, Randomized controlled trial, Vancomycin, law, Internal medicine, medicine, Humans, Pharmacology (medical), Young adult, Aged, Aged, 80 and over, Pharmacology, Response rate (survey), business.industry, Middle Aged, Clostridium difficile, Anti-Bacterial Agents, Surgery, Clinical trial, Treatment Outcome, Infectious Diseases, chemistry, Clostridium Infections, business, medicine.drug

Abstract

Background The available treatment options for Clostridium difficile infection (CDI) are limited by high recurrence rates. Surotomycin was a novel bactericidal cyclic lipopeptide in development to treat CDI that demonstrated non-inferiority to vancomycin in a Phase 2 trial. Objectives To assess surotomycin safety and clinical response (non-inferiority versus vancomycin) at the end of treatment (EOT) of CDI. Additionally, to assess surotomycin response over time and sustained response at 30-40 days post-EOT (superiority versus vancomycin). Patients and methods Patients with CDI were randomized (1:1) to receive twice-daily oral surotomycin 250 mg alternating with twice-daily placebo or four-times-daily oral vancomycin 125 mg for 10 days in this Phase 3, double-blind, multicentre, international trial. Clinical response over time and sustained clinical response were monitored until the end of the trial, through a follow-up period of 30-40 days. Clinical Trial Registration: NCT01598311. Results A total of 285 and 292 patients with confirmed CDI were randomized to receive surotomycin and vancomycin, respectively. Surotomycin-associated clinical response at EOT was non-inferior to vancomycin (surotomycin/vancomycin: 83.4%/82.1%; difference 1.4%, 95% CI - 4.9, 7.6). Following treatment with surotomycin, both clinical response over time (stratified log-rank test, P = 0.277) and sustained clinical response (63.3%/59.0%; difference 4.3%, 95% CI - 3.6, 12.2) did not demonstrate superiority versus vancomycin at end of trial. Both treatments were generally well tolerated. Conclusions Surotomycin demonstrated non-inferiority to vancomycin for CDI clinical response at EOT. Surotomycin did not demonstrate superiority to vancomycin for clinical response over time or sustained clinical response rate.

Published

2017

12. Comparison of Clostridium difficile minimum inhibitory concentrations obtained using agar dilution vs broth microdilution methods

Author

Darcie E. Roe-Carpenter, Laurent Chesnel, Julia Nary, Suzanne E. Dale, Diane M. Citron, Christine Hastey, and Jennifer H. Law

Subjects

0301 basic medicine, Clostridioides difficile, 030106 microbiology, Broth microdilution, Agar Dilution Method, Reproducibility of Results, Microbial Sensitivity Tests, Clostridium difficile, Biology, Antimicrobial, Microbiology, Anti-Bacterial Agents, Culture Media, Agar dilution, 03 medical and health sciences, Minimum inhibitory concentration, 0302 clinical medicine, Infectious Diseases, Antibiotic resistance, Humans, 030212 general & internal medicine, Anaerobic bacteria, Food science

Abstract

Due to increasing antibiotic resistance among anaerobic bacteria, routine antimicrobial susceptibility testing is recommended by the Clinical and Laboratory Standards Institute (CLSI). This study compared the minimum inhibitory concentrations (MICs) from 920 Clostridium difficile isolates tested against seven antimicrobial agents using the two current CLSI reference methodologies, agar dilution method, vs broth microdilution method. A subset of isolate testing was performed independently by two laboratories to evaluate reproducibility. A negative bias was noted for MICs generated from broth microdilution compared to agar dilution and the reproducibility was variable and drug dependent. Therefore, broth microdilution is not recommended as an alternative to agar dilution for C. difficile antimicrobial susceptibility testing.

Published

2017

13. Surotomycin versus vancomycin forClostridium difficileinfection: Phase 2, randomized, controlled, double-blind, non-inferiority, multicentre trial

Author

Shruta Rege, Thomas J. Louie, Hernando Patino, Chris Stevens, Laurent Chesnel, Christine H. Lee, and Kathleen M. Mullane

Subjects

Adult, Male, 0301 basic medicine, Microbiology (medical), medicine.medical_specialty, medicine.drug_class, 030106 microbiology, Antibiotics, Administration, Oral, Surotomycin, Peptides, Cyclic, law.invention, Lipopeptides, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Double-Blind Method, Randomized controlled trial, Recurrence, Vancomycin, law, Internal medicine, medicine, Humans, Pharmacology (medical), 030212 general & internal medicine, Adverse effect, Aged, Pharmacology, Clostridioides difficile, business.industry, Incidence (epidemiology), Middle Aged, Clostridium difficile, Anti-Bacterial Agents, Clinical trial, Treatment Outcome, Infectious Diseases, chemistry, Clostridium Infections, Female, business, medicine.drug

Abstract

Objectives Clostridium difficile infection (CDI) is a major public health concern. Treatment with commonly prescribed antibiotics is associated with high rates of recurrence after initial cure. Here, we present the efficacy and safety of surotomycin, an orally administered, minimally absorbed, selective bactericidal cyclic lipopeptide, compared with vancomycin, in patients with CDI. Methods In this Phase 2, randomized, controlled, double-blind, non-inferiority, multicentre trial, participants received surotomycin 125 mg twice daily, surotomycin 250 mg twice daily or vancomycin 125 mg four times daily for 10 days. The primary efficacy outcome was clinical response at end of treatment. The registration number of the study on clinicaltrials.gov is NCT01085591. Results Clinical cure rates were similar among treatment groups (92.4% for surotomycin 125 mg twice daily, 86.6% for surotomycin 250 mg twice daily and 89.4% for vancomycin). Recurrence rates were 27.9% for surotomycin 125 mg twice daily, 17.2% for surotomycin 250 mg twice daily and 35.6% for vancomycin. The lower recurrence rate with surotomycin 250 mg twice daily versus vancomycin was statistically significant (P = 0.035). Recurrence rates were statistically similar between the surotomycin dose groups (P = 0.193). Rates of sustained clinical response at end of study were 66.7% for surotomycin 125 mg twice daily, 70.1% for surotomycin 250 mg twice daily and 56.1% for vancomycin. Incidence of adverse events was similar among treatment arms. Conclusions Recurrence rates of CDI were lower with surotomycin with higher sustained clinical response rates compared with vancomycin, both of which may offer potential clinical benefits.

Published

2016

14. Effect of Fidaxomicin versus Vancomycin on Susceptibility to Intestinal Colonization with Vancomycin-Resistant Enterococci and Klebsiella pneumoniae in Mice

Author

Lihong Gao, Laurent Chesnel, Jennifer L. Cadnum, Curtis J. Donskey, Abhishek Deshpande, Sirisha Kundrapu, Alexander Polinkovsky, Luisa Chan, and Kelly Hurless

Subjects

0301 basic medicine, medicine.drug_class, 030106 microbiology, Population, Antibiotics, Firmicutes, Microbial Sensitivity Tests, Colonisation resistance, Real-Time Polymerase Chain Reaction, beta-Lactamases, Vancomycin-Resistant Enterococci, Microbiology, Feces, Mice, 03 medical and health sciences, 0302 clinical medicine, Vancomycin, medicine, Animals, Pharmacology (medical), Fidaxomicin, 030212 general & internal medicine, education, Clostridium, Pharmacology, Analytical Procedures, education.field_of_study, biology, business.industry, biochemical phenomena, metabolism, and nutrition, Bacteroides Infections, biology.organism_classification, Anti-Bacterial Agents, Intestines, Klebsiella pneumoniae, Metronidazole, Aminoglycosides, Infectious Diseases, Female, Anaerobic bacteria, Bacteroides, business, medicine.drug

Abstract

The use of oral vancomycin or metronidazole for treatment of Clostridium difficile infection (CDI) may promote colonization by health care-associated pathogens due to disruption of the intestinal microbiota. Because the macrocyclic antibiotic fidaxomicin causes less alteration of the intestinal microbiota than vancomycin, we hypothesized that it would not lead to a loss of colonization resistance to vancomycin-resistant enterococci (VRE) and extended-spectrum-β-lactamase-producing Klebsiella pneumoniae (ESBL-Kp). Mice (8 per group) received orogastric saline, vancomycin, or fidaxomicin daily for 5 days at doses resulting in stool concentrations in mice similar to those measured in humans. The mice were challenged with 10 5 CFU of orogastric VRE or ESBL-Kp on day 2 of treatment and concentrations of the pathogens in stool were monitored. The impact of drug exposure on the microbiome was measured by cultures, real-time PCR for selected anaerobic bacteria, and deep sequencing. In comparison to saline controls, oral vancomycin promoted establishment of high-density colonization by VRE and ESBL-Kp in stool (8 to 10 log 10 CFU/g; P < 0.001), whereas fidaxomicin did not (10 CFU; P > 0.5). Vancomycin treatment resulted in significant reductions in enterococci, Bacteroides spp., and Clostridium leptum , whereas the population of aerobic and facultative Gram-negative bacilli increased; deep-sequencing analysis demonstrated suppression of Firmicutes and expansion of Proteobacteria during vancomycin treatment. Fidaxomicin did not cause significant alteration of the microbiota. In summary, in contrast to vancomycin, fidaxomicin treatment caused minimal disruption of the intestinal microbiota and did not render the microbiota susceptible to VRE and ESBL-Kp colonization.

Published

2016

15. Impact of Surotomycin on the Gut Microbiota of Healthy Volunteers in a Phase 1 Clinical Trial

Author

Ellie J. C. Goldstein, Suzanne E. Dale, Laurent Chesnel, Diane M. Citron, and Kerin L. Tyrrell

Subjects

Adult, Male, 0301 basic medicine, 030106 microbiology, Prevotella, Physiology, Surotomycin, Microbial Sensitivity Tests, Gut flora, Placebo, Peptides, Cyclic, Bacteroides fragilis, Feces, Lipopeptides, 03 medical and health sciences, chemistry.chemical_compound, Double-Blind Method, Enterobacteriaceae, Lactobacillus, medicine, Humans, Pharmacology (medical), Pharmacology, biology, Middle Aged, biology.organism_classification, Healthy Volunteers, Anti-Bacterial Agents, Gastrointestinal Microbiome, Diarrhea, Infectious Diseases, chemistry, Enterococcus, Immunology, Female, medicine.symptom

Abstract

Clostridium difficile -associated diarrhea has been associated with disruption of the normal intestinal microbiota, particularly the Bacteroides fragilis group and Prevotella species. Surotomycin is a bactericidal cyclic lipopeptide in development for treatment of Clostridium difficile -associated diarrhea that has selective and potent activity against C. difficile and other Gram-positive bacteria and a minimal impact on intestinal Gram-negative organisms. The impacts of ascending doses of surotomycin on major organism groups in the gut microbiota of healthy volunteers were evaluated during a randomized, double-blind, placebo-controlled, multiple-dose phase 1 study. Thirty volunteers were randomized into 3 cohorts, using a 4:1 ratio, to receive 250 mg, 500 mg, or 1,000 mg of surotomycin, or placebo, twice daily for 14 days. Stool samples collected at baseline (days 0 and 1) and at the end of treatment (days 13 to 15) were cultured quantitatively. The B. fragilis group, the Bacteroides / Prevotella group, and Enterobacteriaceae were also quantified by quantitative real-time PCR. Baseline and end-of-treatment stool samples showed 1- to 2-log 10 CFU/g reductions in total bacterial counts for most volunteers. Various decreases in clostridial, Lactobacillus-Bifidobacterium group, and enterococcus-streptococcus group counts occurred while patients were receiving surotomycin, whereas the enterobacteria and the B. fragilis group persisted at the end of treatment. There was no change in enterococcus MICs of surotomycin, nor was vancomycin-resistant Enterococcus detected after exposure. Surotomycin at doses of up to 1,000 mg twice daily had only modest disruptive effects on the gut microbiota. The potential sparing of the gut microbiota by surotomycin may decrease the risk of disease recurrence.

Published

2016

16. Discovery and development of surotomycin for the treatment of Clostridium difficile

Author

Laurent Chesnel, Jared Silverman, Victoria Knight-Connoni, and Carmela Mascio

Subjects

0301 basic medicine, Streptomyces roseosporus, 030106 microbiology, Biological Availability, Bioengineering, Surotomycin, Microbial Sensitivity Tests, Peptides, Cyclic, Applied Microbiology and Biotechnology, Microbiology, Lipopeptides, 03 medical and health sciences, chemistry.chemical_compound, Minimum inhibitory concentration, Clinical Trials, Phase II as Topic, medicine, Animals, Humans, First episode, Gastrointestinal tract, biology, Clostridioides difficile, Clostridium difficile, biology.organism_classification, Anti-Bacterial Agents, Gastrointestinal Microbiome, Diarrhea, chemistry, Clostridium Infections, Vancomycin, medicine.symptom, Biotechnology, medicine.drug

Abstract

The primary challenge for treating Clostridium difficile infections (CDI) is maintenance of clinical response after the end of treatment (sustained clinical response). Disease recurrence following a positive clinical response occurs in approximately 6–25 % of patients after the first episode and in up to 65 % for subsequent recurrences. Surotomycin, a novel cyclic lipopeptide antibiotic with a core derived by Streptomyces roseosporus fermentation, disrupts C. difficile cellular membrane activity in both logarithmic and stationary phases and minimally disturbs normal gastrointestinal microbiota because of its lack of activity against Gram-negative anaerobes and facultative anaerobes. Preclinical and clinical evidence indicate that surotomycin has low oral bioavailability, allowing gastrointestinal tract concentrations to greatly exceed its minimum inhibitory concentration for C. difficile. Surotomycin is well tolerated and effective in hamster models of CDI. Phase 2 clinical evidence suggests that surotomycin (250 mg twice daily) is an effective CDI treatment, with statistically lower recurrence rates than vancomycin.

Published

2016

17. Impact of Variations in Test Method Parameters on In Vitro Activity of Surotomycin against Clostridium difficile and Surotomycin Quality Control Limits for Broth Microdilution and Agar Dilution Susceptibility Testing

Author

Daniel F. Sahm, Laurent Chesnel, Jennifer Deane, Maria M. Traczewski, and Steven D. Brown

Subjects

Quality Control, 0301 basic medicine, Microbiology (medical), food.ingredient, 030106 microbiology, Eggerthella lenta, Surotomycin, Microbial Sensitivity Tests, Peptides, Cyclic, Sensitivity and Specificity, Microbiology, Agar dilution, Lipopeptides, 03 medical and health sciences, chemistry.chemical_compound, food, Humans, Agar, Chromatography, Clostridioides difficile, Chemistry, Broth microdilution, Reproducibility of Results, Lipopeptide, Bacteriology, Test method, Clostridium difficile, Anti-Bacterial Agents

Abstract

Test parameter variations were evaluated for their effects on surotomycin MICs. Calcium concentration was the only variable that influenced MICs; therefore, 50 μg/ml (standard for lipopeptide testing) is recommended. Quality control ranges for Clostridium difficile (0.12 to 1 μg/ml) and Eggerthella lenta (broth, 1 to 4 μg/ml; agar, 1 to 8 μg/ml) were approved by the Clinical and Laboratory Standards Institute based on these data.

Published

2016

18. Impact of Oral Fidaxomicin Administration on the Intestinal Microbiota and Susceptibility to Clostridium difficile Colonization in Mice

Author

Julia L. Cope, Nadim J. Ajami, Laurent Chesnel, Joseph F. Petrosino, and Matthew C. Wong

Subjects

0301 basic medicine, medicine.drug_class, 030106 microbiology, Antibiotics, Colonisation resistance, Gut flora, Microbiology, 03 medical and health sciences, Feces, Mice, Vancomycin, RNA, Ribosomal, 16S, medicine, Animals, Pharmacology (medical), Fidaxomicin, Colonization, Pharmacology, Cross Infection, biology, business.industry, Clostridioides difficile, Clostridium difficile, biology.organism_classification, Anti-Bacterial Agents, Gastrointestinal Microbiome, Mice, Inbred C57BL, Diarrhea, Disease Models, Animal, Infectious Diseases, Susceptibility, Clostridium Infections, Female, medicine.symptom, business, medicine.drug

Abstract

Clostridium difficile infection (CDI), a common cause of hospital-acquired infections, typically occurs after disruption of the normal gut microbiome by broad-spectrum antibiotics. Fidaxomicin is a narrow-spectrum antibiotic that demonstrates a reduced impact on the normal gut microbiota and is approved for the treatment of CDI. To further explore the benefits of this property, we used a murine model to examine the effects of fidaxomicin versus vancomycin on gut microbiota and susceptibility to C. difficile colonization while tracking microbiota recovery over time. Mice were exposed to fidaxomicin or vancomycin by oral gavage for 3 days and subsequently challenged with C. difficile spores at predetermined time points up to 21 days postexposure to antibiotics. Fecal samples were subsequently collected for analysis. Twenty-four hours postchallenge, mice were euthanized and the colon contents harvested. The microbiota was characterized using 16S rRNA gene sequencing. All fidaxomicin-exposed mice (except for one at day 8) were resistant to C. difficile colonization. However, 9 of 15 vancomycin-exposed mice were susceptible to C. difficile colonization until day 12. All vancomycin-exposed mice recovered colonization resistance by day 16. Bacterial diversity was similar prior to antibiotic exposure in both arms and decreased substantially after exposure. A shift in taxonomic structure and composition occurred after both exposures; however, the shift was greater in vancomycin-exposed than in fidaxomicin-exposed mice. In summary, compared with vancomycin, fidaxomicin exposure had less impact on microbiota composition, promoted faster microbial recovery, and had less impact on the loss of C. difficile colonization resistance.

Published

2018

19. Molecular epidemiology of Clostridioides (Clostridium) difficile strains recovered from clinical trials in the US, Canada and Europe from 2006-2009 to 2012-2015

Author

Laurent Chesnel, Ellie J. C. Goldstein, Laurica A. Petrella, Stuart Johnson, Suzanne E. Dale, Diane M. Citron, Adam Cheknis, Susan P. Sambol, Julia Nary, Pamela Sears, and Dale N. Gerding

Subjects

0301 basic medicine, Canada, genetic structures, Genotype, 030106 microbiology, Microbial Sensitivity Tests, Microbiology, 03 medical and health sciences, Antibiotic resistance, Drug Resistance, Bacterial, Prohibitins, Prevalence, Medicine, Humans, Typing, Randomized Controlled Trials as Topic, Molecular Epidemiology, Molecular epidemiology, business.industry, Clostridioides difficile, Strain (biology), Clostridium difficile, Antimicrobial, United States, Clinical trial, Europe, Molecular Typing, Restriction enzyme, Infectious Diseases, Clostridium Infections, business

Abstract

The prevalence of C. difficile infection (CDI) and severe CDI are influenced by the prevalence of specific C. difficile strains, which are themselves influenced by antimicrobial susceptibility determinants as well as antimicrobial usage patterns. Restriction endonuclease analysis (REA) typing and antimicrobial susceptibility testing were used to characterize 1808 C. difficile isolates obtained from patients enrolled in four multicenter, multi-country, randomized CDI treatment trials conducted between 2006 and 2009 and between 2012 and 2015. By 2015, the epidemic REA group BI strain (RT027) had decreased in prevalence in North America (US: 43%-18%, Canada: 39%-24%, P 0.001), but rates of moxifloxacin resistance remained high. In contrast, REA group Y (RT014/020) and DH (RT106) strains, both of which had low rates of moxifloxacin resistance, increased in prevalence (Y strain - US: 6%-17%, Canada: 11%-23%, P 0.001; DH strain - US: 1%-11%, Canada: 0%-8%, P 0.0001). In Europe, the BI strain (RT027) was highly prevalent in Eastern European countries in 2015, but was unchanged in other parts of Europe. As in North America, the Y strain (RT014/020) was prevalent in both time periods, but the DH strain was rarely identified. Continued international molecular surveillance of C. difficile will be important to track prevalence of known epidemic strains and detect emergence of new strains of potential epidemiologic significance.

Published

2018

20. Effects of Surotomycin on Clostridium difficile Viability and Toxin Production In Vitro

Author

Shonna M. McBride, Jose M. Suárez, Laurent Chesnel, Laurent Bouillaut, Saul Tzipori, Abraham L. Sonenshein, Joseph A. Sorg, Carmela Mascio, and Diane J. Schmidt

Subjects

Virulence Factors, medicine.drug_class, Bacterial Toxins, Antibiotics, Virulence, Surotomycin, Microbial Sensitivity Tests, Biology, medicine.disease_cause, Peptides, Cyclic, Microbiology, Enterotoxins, Lipopeptides, chemistry.chemical_compound, Cell Wall, Vancomycin, Metronidazole, medicine, Experimental Therapeutics, Pharmacology (medical), Spores, Bacterial, Pharmacology, Clostridioides difficile, Toxin, Gene Expression Regulation, Bacterial, Clostridium difficile, Antimicrobial, Anti-Bacterial Agents, Infectious Diseases, chemistry, Mutation, medicine.drug

Abstract

The increasing incidence and severity of infection by Clostridium difficile have stimulated attempts to develop new antimicrobial therapies. We report here the relative abilities of two antibiotics (metronidazole and vancomycin) in current use for treating C. difficile infection and of a third antimicrobial, surotomycin, to kill C. difficile cells at various stages of development and to inhibit the production of the toxin proteins that are the major virulence factors. The results indicate that none of the drugs affects the viability of spores at 8× MIC or 80× MIC and that all of the drugs kill exponential-phase cells when provided at 8× MIC. In contrast, none of the drugs killed stationary-phase cells or inhibited toxin production when provided at 8× MIC and neither vancomycin nor metronidazole killed stationary-phase cells when provided at 80× MIC. Surotomycin, on the other hand, did kill stationary-phase cells when provided at 80× MIC but did so without inducing lysis.

Published

2015

21. Enteric microbiome profiles during a randomized Phase 2 clinical trial of surotomycin versus vancomycin for the treatment of Clostridium difficile infection

Author

Laurent Chesnel, Thomas J. Louie, Jennifer Happe, Brendan Byrne, Kristine Cannon, Linda R. Ward, and Kaiyu Wu

Subjects

0301 basic medicine, Male, Time Factors, Phases of clinical research, Administration, Oral, Gastroenterology, law.invention, chemistry.chemical_compound, Feces, 0302 clinical medicine, Randomized controlled trial, law, Prevotella, Pharmacology (medical), 030212 general & internal medicine, Aged, 80 and over, biology, Clostridium difficile, Middle Aged, Anti-Bacterial Agents, Infectious Diseases, Vancomycin, Female, medicine.drug, Microbiology (medical), Adult, medicine.medical_specialty, Adolescent, 030106 microbiology, Surotomycin, Real-Time Polymerase Chain Reaction, Peptides, Cyclic, Microbiology, 03 medical and health sciences, Lipopeptides, Young Adult, Double-Blind Method, Internal medicine, medicine, Humans, Aged, Pharmacology, Bacteriological Techniques, Bacteria, business.industry, biology.organism_classification, Bacterial Load, Gastrointestinal Microbiome, Clinical trial, chemistry, Clostridium Infections, Dysbiosis, Metagenomics, business

Abstract

Objectives The effects of surotomycin (CB-183,315, MK-4261), a bactericidal cyclic lipopeptide, and vancomycin, the current standard-of-care for Clostridium difficile infection (CDI), on intestinal pathogens and microbiota were evaluated parallel to a Phase 2 randomized, double-blind clinical trial. Methods The single-centre cohort included 26 patients receiving surotomycin [125 or 250 mg twice daily (n = 9 each)] or oral vancomycin [125 mg four times daily (n = 8)] for 10 days. Faecal samples were collected at days 0-42 to quantify both C. difficile by conventional culture and the major components of the microbiome by quantitative PCR. Results Surotomycin 250 mg twice daily or vancomycin 125 mg four times daily reduced faecal C. difficile counts from ∼105-107 log10 cfu/g at baseline to ≤ 102 cfu/g by days 4-10 of treatment. Day 10 counts of C. difficile in 3/9 patients receiving surotomycin 125 mg twice daily remained detectable, including one patient who failed to achieve clinical cure. Bacteroidetes and Prevotella mean counts increased 0.7 log10 or remained unchanged with surotomycin 125 and 250 mg twice daily, respectively, whereas vancomycin reduced counts by 2.5-3.2 log10 (P

Published

2017

22. Surotomycin Demonstrates Low In Vitro Frequency of Resistance and Rapid Bactericidal Activity in Clostridium difficile, Enterococcus faecalis, and Enterococcus faecium

Author

Grace M. Thorne, Jared Silverman, Laurent Chesnel, and Carmela Mascio

Subjects

Enterococcus faecium, Surotomycin, Microbial Sensitivity Tests, Peptides, Cyclic, Enterococcus faecalis, Microbiology, Bacteria, Anaerobic, Lipopeptides, chemistry.chemical_compound, Ampicillin, Drug Resistance, Bacterial, medicine, Experimental Therapeutics, Pharmacology (medical), Pharmacology, biology, Clostridioides difficile, business.industry, Vancomycin Resistance, biochemical phenomena, metabolism, and nutrition, Clostridium difficile, biology.organism_classification, Anti-Bacterial Agents, Metronidazole, Infectious Diseases, Enterococcus, chemistry, Vancomycin, business, medicine.drug

Abstract

Surotomycin (CB-183,315) is an orally administered, minimally absorbed, selective bactericidal cyclic lipopeptide in phase 3 development for the treatment of Clostridium difficile -associated diarrhea. The aim of this study was to evaluate the emergence of resistance in C. difficile (ATCC 700057 and three recent clinical isolates from the restriction endonuclease analysis groups BI, BK, and K), vancomycin-susceptible (VS) Enterococcus faecalis (ATCC 49452), vancomycin-resistant (VR) E. faecalis (ATCC 700802), VS Enterococcus faecium (ATCC 6569), and VR E. faecium (ATCC 51559) under anaerobic conditions. The rate of spontaneous resistance was below the limit of detection (−8 to −9 ) for surotomycin at 16 and 32× the MIC for all isolates tested. Under selective pressure by serial passage, C. difficile grew in a maximum of 4 μg/ml surotomycin (final MICs of 2 to 8 μg/ml [4- to 16-fold higher than those of the naive control]) at day 15, with the exception of the C. difficile BK strain, which grew in 16 to 32 μg/ml (final MICs of 8 to 32 μg/ml [16- to 64-fold higher than those of the naive control]). Enterococci remained relatively unchanged over 15 days, growing in a maximum of 8 μg/ml surotomycin (final MICs of 2 to 16 μg/ml [8- to 64-fold higher than those of the naive control]). Of the isolates tested, no cross-resistance to vancomycin, rifampin, ampicillin, metronidazole, or moxifloxacin was observed. Surotomycin at 20× MIC demonstrated equally rapid bactericidal activity (≥3-log-unit reduction in CFU/ml in ≤8 h) against naive and reduced-susceptibility isolates of C. difficile , VS Enterococcus (VSE), and VR Enterococcus (VRE), except for C. difficile BK (2.6-log-unit reductions for both). These results suggest that emergence of resistance to surotomycin against C. difficile , E. faecalis , and E. faecium is likely to be rare.

Published

2014

23. In vitro activity of ceftolozane/tazobactam in combination with other classes of antibacterial agents

Author

Karen Howland, Laurent Chesnel, and Cédric Jacqueline

Subjects

0301 basic medicine, Microbiology (medical), Tazobactam, medicine.drug_class, 030106 microbiology, Immunology, Antibiotics, Aztreonam, Tigecycline, Microbial Sensitivity Tests, Pharmacology, Microbiology, Meropenem, 03 medical and health sciences, chemistry.chemical_compound, Gram-Negative Bacteria, polycyclic compounds, Immunology and Allergy, Medicine, Humans, Amikacin, Antibacterial agent, business.industry, Drug Synergism, biochemical phenomena, metabolism, and nutrition, bacterial infections and mycoses, Cephalosporins, chemistry, bacteria, Ceftolozane, Drug Therapy, Combination, business, Drug Antagonism, medicine.drug

Abstract

Objectives Combination antibiotic therapy has been used successfully to treat some patients with bacterial infections. However, although certain combinations may result in beneficial synergistic activity, others may produce antagonistic effects resulting in poor treatment outcomes. Ceftolozane/tazobactam is an antibacterial agent with potent activity against Pseudomonas aeruginosa and many other Gram-negative pathogens, including extended-spectrum β-lactamase (ESBL)-producing Enterobacteriaceae. This study aimed to evaluate potential synergistic or antagonistic interactions between ceftolozane/tazobactam and a selection of antibacterial agents. Methods Chequerboard analyses were conducted with Escherichia coli, Klebsiella pneumoniae and P. aeruginosa isolates. Results Combinations of ceftolozane/tazobactam with aztreonam, amikacin, tigecycline and meropenem resulted in synergistic effects in some of the bacterial strains tested. The potency of ceftolozane/tazobactam against common Gram-negative pathogens was not compromised in the presence of other commonly prescribed antibacterial agents, and ceftolozane/tazobactam did not antagonise the activity of these other antibacterials. Conclusions The synergy observed for some antibacterial combinations in this study supplements the currently available information for combination therapy and may suggest new directions for treating challenging cases. Some synergistic effects may be attributed, at least in part, to the ESBL-inhibitory activity of tazobactam, although this remains to be proven. The mechanisms of the other synergistic interactions observed also require further elucidation. Ceftolozane/tazobactam did not adversely affect the activity of, and was not affected by, other antibacterial agents given concurrently. In vivo studies will be needed to substantiate these results and to determine their clinical relevance.

Published

2017

24. Primary Outcomes From a Phase 3, Randomized, Double-Blind, Active-Controlled Trial of Surotomycin in Subjects With Clostridium difficile Infection

Author

Adedayo Adedoyin, Dalya Guris, Vicente Boix, Uschi Stoutenburgh, Laurent Chesnel, Yoshihiko Murata, Richard N. Fedorak, Kajal B. Larson, Kathleen M. Mullane, Mandy Jin, and Yves Pesant

Subjects

0301 basic medicine, medicine.medical_specialty, 030106 microbiology, Population, vancomycin, Surotomycin, surotomycin, law.invention, 03 medical and health sciences, chemistry.chemical_compound, Randomized controlled trial, law, Internal medicine, antibiotic, Clostridium difficile infection, medicine, Major Article, education, education.field_of_study, Intention-to-treat analysis, Surrogate endpoint, business.industry, Clostridium difficile, Log-rank test, Infectious Diseases, Oncology, chemistry, Immunology, Vancomycin, business, medicine.drug

Abstract

Background Although the incidence of Clostridium difficile infection (CDI) is increasing, available CDI treatment options are limited in terms of sustained response after treatment. This phase 3 trial assessed the efficacy and safety of surotomycin, a novel bactericidal cyclic lipopeptide, versus oral vancomycin in subjects with CDI. Methods In this randomized, double-blind, active-controlled, multicenter, international trial, subjects with CDI confirmed by a positive toxin result were randomized to receive surotomycin (250 mg twice daily) or vancomycin (125 mg 4 times daily) orally for 10 days. The primary endpoints were clinical response at end of treatment and evaluation of surotomycin safety. The key secondary endpoints were clinical response over time and sustained clinical response through a 30- to 40-day follow-up period. Clostridium difficile infection recurrence during follow-up and time to diarrhea resolution were also analyzed. Results In total, 570 subjects were randomized and had confirmed CDI; 290 subjects received surotomycin and 280 subjects received vancomycin. Surotomycin clinical cure rates at end of treatment (surotomycin/vancomycin: 79.0%/83.6%; difference of −4.6%; 95% confidence interval, −11.0 to 1.9]), clinical response over time (stratified log-rank test, P = .832), and sustained clinical response at end of trial (Day 40–50) (60.6%/61.4%; difference of −0.8%; 95% CI, −8.8 to 7.1) in the microbiological modified intent to treat population did not meet noninferiority or superiority criteria versus vancomycin. Both treatments were generally well tolerated. Conclusions Surotomycin failed to meet the criteria for noninferiority versus vancomycin for the primary and key secondary endpoints in this trial.

Published

2017

25. New Antimicrobial Agents … but No Susceptibility Tests!

Author

Ian A. Critchley, Alisa W Serio, Kevin M. Krause, Sandra P. McCurdy, Joseph P. Iaconis, Nicole E. Scangarella-Oman, Sachin Bhagwat, Laurent Chesnel, Patricia A. Bradford, Trudy Grossman, Jeff Alder, George A. Williams, Gregory G. Stone, Mary Motyl, Nicole M. Mahoney, Linda A. Miller, Jane E. Ambler, Roger Echols, Luigi Xerri, David Van Veenhuyzen, and Judith N. Steenbergen

Subjects

0301 basic medicine, Microbiology (medical), Traditional medicine, business.industry, 030106 microbiology, MEDLINE, Microbial Sensitivity Tests, Antimicrobial, Anti-Bacterial Agents, 03 medical and health sciences, 0302 clinical medicine, Infectious Diseases, Anti-Infective Agents, Medicine, 030212 general & internal medicine, business

Published

2016

26. Evaluating the Effects of Surotomycin Treatment on Clostridium difficile Toxin A and B Production, Immune Response, and Morphological Changes

Author

Mohammed Khaleduzzaman, Eugénie Bassères, Laurent Chesnel, Kevin W. Garey, Bradley T. Endres, and M. Jahangir Alam

Subjects

0301 basic medicine, 030106 microbiology, Bacterial Toxins, Clostridium difficile toxin A, Surotomycin, Clostridium difficile toxin B, Microbial Sensitivity Tests, medicine.disease_cause, Peptides, Cyclic, Microbiology, 03 medical and health sciences, chemistry.chemical_compound, Enterotoxins, Lipopeptides, Clostridium, Immune system, Bacterial Proteins, Vancomycin, Cell Line, Tumor, Metronidazole, medicine, Humans, Pharmacology (medical), Pharmacology, biology, Toxin, Clostridioides difficile, Interleukin-8, Clostridium difficile, biology.organism_classification, Anti-Bacterial Agents, 030104 developmental biology, Infectious Diseases, chemistry, Microscopy, Electron, Scanning, Caco-2 Cells, medicine.drug

Abstract

Surotomycin is a cyclic lipopeptide in development for Clostridium difficile -associated diarrhea. This study aimed to assess the impact of surotomycin exposure on C. difficile toxin A and B concentrations and the associated changes in immune response in comparison to vancomycin and metronidazole. Time-kill curve assays were performed using strain R20291 (BI/NAP1/027) at supra-MICs (4× and 40×) and sub-MICs (0.5×) of surotomycin and comparators. Following treatment, CFU counts, toxin A and B concentrations, and cellular morphological changes using scanning electron microscopy were examined. Inflammatory response was determined by measuring interleukin-8 (IL-8) concentrations from polarized Caco-2 cells exposed to antibiotic-treated C. difficile growth media. Supra-MICs (4× and 40×) of surotomycin resulted in a reduction of vegetative cells over 72 h (4-log difference, P < 0.01) compared to controls. These results correlated with decreases of 77% and 68% in toxin A and B production at 48 h, respectively ( P < 0.005, each), which resulted in a significant reduction in IL-8 concentration compared to controls. Similar results were observed with comparator antibiotics. Bacterial cell morphology showed that the cell wall was broken apart by surotomycin treatment at supra-MICs while sub-MIC studies showed a “deflated” phenotype plus a rippling effect. These results suggest that surotomycin has potent killing effects on C. difficile that results in reduced toxin production and attenuates the immune response similar to comparator antibiotics. The morphological data also confirm observations that surotomycin is a membrane-active antibiotic.

Published

2016

27. Effect of Surotomycin, a Novel Cyclic Lipopeptide Antibiotic, on Intestinal Colonization with Vancomycin-Resistant Enterococci and Klebsiella pneumoniae in Mice

Author

Laurent Chesnel, Kelly Hurless, Jennifer L. Cadnum, Lihong Gao, Alexander Polinkovsky, Luisa Chan, Sirisha Kundrapu, Curtis J. Donskey, and Abhishek Deshpande

Subjects

0301 basic medicine, medicine.drug_class, Klebsiella pneumoniae, 030106 microbiology, Antibiotics, Surotomycin, Peptides, Cyclic, Microbiology, Vancomycin-Resistant Enterococci, 03 medical and health sciences, chemistry.chemical_compound, Lipopeptides, Mice, Vancomycin, Metronidazole, Gram-Negative Bacteria, medicine, Animals, Pharmacology (medical), Colonization, Experimental Therapeutics, Pharmacology, biology, business.industry, Vancomycin Resistance, Clostridium difficile, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, bacterial infections and mycoses, Anti-Bacterial Agents, Infectious Diseases, chemistry, Female, Bacteroides, business, medicine.drug

Abstract

Surotomycin (formerly called CB-183,315) is a novel, orally administered cyclic lipopeptide antibacterial in development for the treatment of Clostridium difficile infection (CDI) that has potent activity against vancomycin-resistant enterococci (VRE) but limited activity against Gram-negative bacilli, including Bacteroides spp. We used a mouse model to investigate the impact of surotomycin exposure on the microbiome, and to test the consequences of the disruption on colonization by vancomycin-resistant enterococci (VRE) and extended-spectrum β-lactamase-producing Klebsiella pneumoniae (ESBL-KP), in comparison with the effects of oral vancomycin and metronidazole. Mice (8 per group) received saline, vancomycin, metronidazole, or surotomycin through an orogastric tube daily for 5 days and were challenged with 10 5 CFU of VRE or ESBL-KP administered through an orogastric tube on day 2 of treatment. The concentrations of the pathogens in stool were determined during and after treatment by plating on selective media. A second experiment was conducted to determine if the antibiotics would inhibit established VRE colonization. In comparison to controls, oral vancomycin promoted VRE and ESBL-KP overgrowth in stool (8 log 10 to 10 log 10 CFU/g; P < 0.001), whereas metronidazole did not (10 CFU/g; P > 0.5). Surotomycin promoted ESBL-KP overgrowth (>8 log 10 CFU/g; P

Published

2015

28. Mode of action and bactericidal properties of surotomycin against growing and nongrowing Clostridium difficile

Author

Carmela T. M. Mascio, Xiaoqian Wu, Mohammed Zahidul Alam, Laurent Chesnel, and Julian G. Hurdle

Subjects

Pharmacology, medicine.drug_class, Clostridioides difficile, Antibiotics, RNA, Surotomycin, Microbial Sensitivity Tests, Clostridium difficile, Biology, Peptides, Cyclic, In vitro, Microbiology, Anti-Bacterial Agents, Cell wall, chemistry.chemical_compound, Lipopeptides, Infectious Diseases, chemistry, medicine, Pharmacology (medical), Propidium iodide, Mode of action, Mechanisms of Action: Physiological Effects

Abstract

Surotomycin (CB-183,315), a cyclic lipopeptide, is in phase 3 clinical development for the treatment of Clostridium difficile infection. We report here the further characterization of the in vitro mode of action of surotomycin, including its activity against growing and nongrowing C. difficile . This was assessed through time-kill kinetics, allowing a determination of the effects on the membrane potential and permeability and macromolecular synthesis in C. difficile . Against representative strains of C. difficile , surotomycin displayed concentration-dependent killing of both logarithmic-phase and stationary-phase cultures at a concentration that was ≤16× the MIC. Exposure resulted in the inhibition of macromolecular synthesis (in DNA, RNA, proteins, and cell wall). At bactericidal concentrations, surotomycin dissipated the membrane potential of C. difficile without changes to the permeability of propidium iodide. These observations are consistent with surotomycin acting as a membrane-active antibiotic, exhibiting rapid bactericidal activities against growing and nongrowing C. difficile .

Published

2015

29. A yeast genetic system for the identification and characterization of substrate proteins transferred into host cells by the Legionella pneumophila Dot/Icm system

Author

Laurent Chesnel, Craig R. Roy, and Eva M. Campodonico

Subjects

biology, Endoplasmic reticulum, Saccharomyces cerevisiae, Vacuole, biology.organism_classification, Microbiology, Legionella pneumophila, Molecular biology, Yeast, Cell biology, Vesicular transport protein, Protein structure, Secretion, Molecular Biology

Abstract

The Dot/Icm system is a type IVb secretion system used by Legionella pneumophila to modulate vesicular transport in both protozoan and mammalian host cells. It has been shown that proteins and processes that are highly conserved in all eukaryotic cells are targets for some of the proteins injected by the Dot/Icm system. For example, the Legionella protein RalF was shown previously to be a Dot/Icm substrate that functions as a guanine nucleotide exchange factor (GEF) for the Arf family of eukaryotic small GTP-binding proteins. Here we show that ectopic production of the RalF protein in Saccharomyces cerevisiae interferes with yeast growth. Inhibition of yeast growth was found to be dependent on the ability of RalF to function as an Arf-GEF in vivo. The possibility that other Dot/Icm substrate proteins would have the capacity to interfere with yeast growth was used as a rationale to screen plasmid libraries containing random fragments of Legionella chromosomal DNA positioned downstream of a galactose-inducible promoter. This screen identified Legionella proteins that conferred a conditional growth defect when overproduced by yeast cultured in the presence of galactose. Most of the Legionella proteins identified were determined to be substrates of the Dot/Icm system. This screen led to the identification of a new Dot/Icm substrate protein that was called YlfA, for yeast lethal factor A. A paralogue of YlfA was identified on an unlinked region of the Legionella chromosome and this protein was also translocated by the Dot/Icm system. It was determined that a hydrophobic region near the N-terminus of the YlfA protein and an adjacent region predicted to form a coiled-coil domain were necessary for a biological activity that interfered with yeast growth. The YlfA protein did not decorate the Legionella-containing vacuole during the first 7 h of infection but could be observed on the endoplasmic reticulum (ER)-derived replicative vacuole and on punctate structures throughout the host cell at later stages. Ectopic production of YlfA in mammalian cells revealed that the N-terminal hydrophobic domain in YlfA was able to localize the protein to early secretory organelles, including endoplasmic reticulum. These studies show that yeast genetics can be exploited to identify and characterize proteins that are injected into host cells by bacterial pathogens that utilize type IV secretion systems for pathogenesis.

Published

2005

30. Biochemical Characterization of Streptococcus pneumoniae Penicillin-Binding Protein 2b and Its Implication in β-Lactam Resistance

Author

Thierry Vernet, Laurent Chesnel, Julie Hopkins, Jacques Croize, Estelle Pagliero, Anne Marie Di Guilmi, and Otto Dideberg

Subjects

DNA, Bacterial, Penicillin binding proteins, Molecular Sequence Data, Penicillins, Muramoylpentapeptide Carboxypeptidase, Biology, medicine.disease_cause, Pneumococcal Infections, beta-Lactam Resistance, law.invention, Microbiology, chemistry.chemical_compound, Bacterial Proteins, Mechanisms of Resistance, law, Streptococcus pneumoniae, polycyclic compounds, medicine, Humans, Penicillin-Binding Proteins, Pharmacology (medical), Amino Acid Sequence, Cloning, Molecular, Serotyping, Peptide sequence, Pharmacology, Mutation, Strain (chemistry), Penicillin G, Aminoacyltransferases, Penicillin, Infectious Diseases, Hexosyltransferases, chemistry, Peptidyl Transferases, Recombinant DNA, Peptidoglycan, Carrier Proteins, medicine.drug

Abstract

Extensive use of β-lactam antibiotics has led to the selection of pathogenic streptococci resistant to β-lactams due to modifications of the penicillin-binding proteins (PBPs). PBP2b from Streptococcus pneumoniae is a monofunctional (class B) high-molecular-weight PBP catalyzing the transpeptidation between adjacent stem peptides of peptidoglycan. The transpeptidase domain of PBP2b isolated from seven clinical resistant (CR) strains contains 7 to 44 amino acid changes over the sequence of PBP2b from the R6 β-lactam-sensitive strain. We show that the extracellular soluble domains of recombinant PBP2b proteins (PBP2b*) originating from these CR strains have an in vitro affinity for penicillin G that is reduced by up to 99% from that of the R6 strain. The Thr446Ala mutation is always observed in CR strains and is close to the key conserved motif (S 443 SN). The Thr446Ala mutation in R6 PBP2b* displays a 60% reduction in penicillin G affinity in vitro compared to that for the wild-type protein. A recombinant R6 strain expressing the R6 PBP2b Thr446Ala mutation is twofold less sensitive to piperacillin than the parental S. pneumoniae strain. Analysis of the Thr446Ala mutation in the context of the PBP2b CR sequences revealed that its influence depends upon the presence of other unidentified mutations.

Published

2004

31. The Structural Modifications Induced by the M339F Substitution in PBP2x from Streptococcus pneumoniae Further Decreases the Susceptibility to β-Lactams of Resistant Strains

Author

Otto Dideberg, André Zapun, Lucile Pernot, Jacques Croize, David Lemaire, Thierry Vernet, Laurent Chesnel, and Dominique Champelovier

Subjects

Models, Molecular, medicine.drug_class, Acylation, Molecular Sequence Data, Antibiotics, Cefotaxime, beta-Lactams, medicine.disease_cause, Biochemistry, beta-Lactam Resistance, In vivo, Streptococcus pneumoniae, β lactams, Serine, medicine, Penicillin-Binding Proteins, Point Mutation, Single amino acid, Molecular Biology, Genetics, Binding Sites, Molecular Structure, biology, Double mutant, Active site, Penicillin G, Cell Biology, Hydrogen-Ion Concentration, In vitro, Kinetics, Phenotype, Mutagenesis, Site-Directed, biology.protein, Carrier Proteins, Crystallization

Abstract

PBP2x is a primary determinant of beta-lactams resistance in Streptococcus pneumoniae. Altered PBP2x with multiple mutations have a reduced "affinity" for the antibiotics. An important polymorphism is found in PBP2x sequences from clinical resistant strains. To understand the mechanism of resistance, it is necessary to identify and characterize the relevant substitutions. Many similar PBP2x sequences from resistant isolates have the previously studied T338A mutation, adjacent to the active site Ser337. We report here the structural and functional analysis of the M339F substitution that is found in a subset of these sequences, originating from highly resistant strains. The M339F mutation causes a 4-10-fold reduction of the reaction rate with beta-lactams, depending on the molecular context. In addition, release of the inactivated antibiotic from the active site is up to 3-fold faster as a result from the M339F mutation. These effects measured in vitro are correlated with the level of beta-lactam resistance in vivo conferred by several PBP2x variants. Thus, a single amino acid difference between similar PBP2x from clinical isolates can strongly modulate the degree of beta-lactam resistance. The crystal structure of the double mutant T338A/M339F solved to a resolution of 2.4 A shows a distortion of the active site and a reorientation of the hydroxyl group of the active site Ser337, which can explain the kinetic effects of the mutations.

Published

2003

32. Increase of the deacylation rate of PBP2x fromStreptococcus pneumoniaeby single point mutations mimicking the class A β-lactamases

Author

Otto Dideberg, André Zapun, Laurent Chesnel, Nicolas Mouz, and Thierry Vernet

Subjects

chemistry.chemical_classification, Penicillin binding proteins, medicine.drug_class, Point mutation, Cephalosporin, Biology, medicine.disease_cause, Biochemistry, Acylation, Hydrolysis, Enzyme, chemistry, Streptococcus pneumoniae, polycyclic compounds, medicine, Escherichia coli

Abstract

The class A beta-lactamases and the transpeptidase domain of the penicillin-binding proteins (PBPs) share the same topology and conserved active-site residues. They both react with beta-lactams to form acylenzymes. The stability of the PBP acylenzymes results in the inhibition of the transpeptidase function and the antibiotic activity of the beta-lactams. In contrast, the deacylation of the beta-lactamases is extremely fast, resulting in a high turnover of beta-lactam hydrolysis, which confers resistance to these antibiotics. In TEM-1 beta-lactamase from Escherichia coli, Glu166 is required for the fast deacylation and occupies the same spatial location as Phe450 in PBP2x from Streptococcus pneumoniae. To gain insight into the deacylation mechanism of both enzymes, Phe450 of PBP2x was replaced by various residues. The introduction of ionizable side chains increased the deacylation rate, in a pH-dependent manner, for the acidic residues. The aspartic acid-containing variant had a 110-fold faster deacylation at pH 8. The magnitude of this effect is similar to that observed in a naturally occurring variant of PBP2x, which confers increased resistance to cephalosporins.

Published

2002

33. Efficacy of surotomycin in an in vitro gut model of Clostridium difficile infection

Author

Laurent Chesnel, Mark H. Wilcox, Scott Nicholson, Sharie L. Todhunter, Jane Freeman, Caroline H. Chilton, and Grace S. Crowther

Subjects

Microbiology (medical), Surotomycin, medicine.disease_cause, Peptides, Cyclic, Microbiology, chemistry.chemical_compound, Lipopeptides, Clostridium, medicine, Humans, Pharmacology (medical), Feces, Pharmacology, biology, Toxin, Clostridioides difficile, Clindamycin, Clostridium difficile, Models, Theoretical, biology.organism_classification, Anti-Bacterial Agents, Gastrointestinal Tract, Infectious Diseases, Treatment Outcome, Enterococcus, chemistry, Clostridium Infections, Bacteroides fragilis, medicine.drug

Abstract

OBJECTIVES: We investigated the efficacy of the cyclic lipopeptide surotomycin in treating clindamycin-induced Clostridium difficile infection (CDI) using an in vitro gut model. METHODS: Two three-stage chemostat gut models were inoculated with human faeces, spiked with C. difficile spores (∼10(7) cfu/mL, PCR ribotype 027 or 001). Clindamycin (33.9 mg/L, four times daily for 7 days) was dosed to induce CDI. Following high-level toxin production, surotomycin (250 mg/L, twice daily for 7 days) was instilled. Microflora populations, C. difficile vegetative cells and spores, cytotoxin titres and antimicrobial levels (LC-MS/MS and bioassay) were determined. The emergence of C. difficile and enterococci with reduced susceptibility to surotomycin was monitored on breakpoint agar (4 × MIC). RESULTS: Counts of viable C. difficile were reduced to near the limit of detection on Days 1 and 3 of surotomycin instillation, and cytotoxin was undetectable on Days 3 and 4 of surotomycin instillation in the 027 and 001 models, respectively. Recurrence of vegetative growth and toxin production occurred 11 days (001 model) and 15 days (027 model) after surotomycin instillation had ceased, and remained for the duration of the experiment. Surotomycin instillation decreased populations of bifidobacteria, clostridia, enterococci and lactobacilli, but was sparing of Bacteroides fragilis group populations. All enumerated organisms had recovered to steady-state levels by 3 weeks post-surotomycin instillation. No evidence of the emergence of reduced susceptibility to surotomycin was observed. CONCLUSIONS: Surotomycin successfully reduced C. difficile vegetative cell counts and toxin levels in the gut model and was sparing of B. fragilis group populations. There was no evidence of decreased susceptibility to surotomycin during exposure or post-exposure.

Published

2014

34. Mo1844 Effect of Fidaxomicin on Susceptibility to Intestinal Colonization With Vancomycin-Resistant Enterococci and Klebsiella pneumoniae in Mice

Author

Jennifer L. Cadnum, Sirisha Kundrapu, Abhishek Deshpande, Kelly Hurless, Laurent Chesnel, Curtis J. Donskey, and Luisa Chan

Subjects

Hepatology, biology, business.industry, Klebsiella pneumoniae, Gastroenterology, Medicine, Fidaxomicin, Vancomycin-Resistant Enterococci, business, biology.organism_classification, Intestinal colonization, Microbiology, medicine.drug

Published

2015

35. Pneumococcal beta-lactam resistance due to a conformational change in penicillin-binding protein 2x

Author

Raphaël Carapito, Laurent Chesnel, André Zapun, Thierry Vernet, Laboratoire d'Ingénierie des Macromolécules (LIM), Institut de biologie structurale (IBS - UMR 5075 ), Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Centre National de la Recherche Scientifique (CNRS)-Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Centre National de la Recherche Scientifique (CNRS), Biotechnologie des interactions macromoléculaires (BIM), Université Louis Pasteur - Strasbourg I-Centre National de la Recherche Scientifique (CNRS), Centre National de la Recherche Scientifique (CNRS)-Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA), Institut de biologie structurale (IBS - UMR 5075), Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Grenoble Alpes (UGA)-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Grenoble Alpes (UGA)-Centre National de la Recherche Scientifique (CNRS), Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), and Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche Interdisciplinaire de Grenoble (IRIG)

Subjects

Models, Molecular, Conformational change, Penicillin binding proteins, MESH: Sequence Homology, Amino Acid, MESH: Protein Structure, Secondary, MESH: Amino Acid Sequence, Cefotaxime, medicine.disease_cause, Biochemistry, Protein Structure, Secondary, Protein structure, Peptide sequence, Genetics, chemistry.chemical_classification, 0303 health sciences, Mutation, MESH: Microbial Sensitivity Tests, MESH: Penicillin-Binding Proteins, MESH: Polymorphism, Single Nucleotide, MESH: Cefotaxime, MESH: Amino Acid Substitution, 3. Good health, Amino acid, [SDV.BBM.BC]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biomolecules [q-bio.BM], Streptococcus pneumoniae, MESH: Streptococcus pneumoniae, MESH: Models, Molecular, MESH: Mutation, Molecular Sequence Data, MESH: Sequence Alignment, Sequence alignment, Microbial Sensitivity Tests, Sciences du Vivant [q-bio]/Médecine humaine et pathologie, Biology, Polymorphism, Single Nucleotide, beta-Lactam Resistance, 03 medical and health sciences, medicine, Penicillin-Binding Proteins, Amino Acid Sequence, [SDV.BBM.BC]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biochemistry [q-bio.BM], Molecular Biology, 030304 developmental biology, MESH: Molecular Sequence Data, Sequence Homology, Amino Acid, 030306 microbiology, Cell Biology, MESH: beta-Lactam Resistance, chemistry, Amino Acid Substitution, Sequence Alignment

Abstract

Streptococcus pneumoniae is a life-threatening human pathogen that is increasingly resistant to a wide array of drugs. Resistance to beta-lactams, the most widely used antibiotics, is correlated with tens of amino acid substitutions in their targets; that is, the penicillin-binding proteins (PBPs), resulting from multiple events of recombination. To discriminate relevant substitutions from those that are incidental to the recombination process, we report the exhaustive characterization of all the mutations in the transpeptidase domain of PBP2x from the highly resistant strain 5204. A semi-automated method combining biochemical and microbiological approaches singled out 6 mutations of 41 (15%) that are essential for high level resistance. The hitherto uncharacterized I371T, R384G, M400T, and N605T together with the previously studied T338M and M339F account for nearly all the loss of affinity of PBP2x for beta-lactams. Most interestingly, I371T and R384G cause the conformational change of a loop that borders the entrance of the active site cavity, hampering antibiotic binding. For the first time all the mutations of a PBP relevant to beta-lactam resistance have been identified, providing new mechanistic insights. Most notable is the relationship between the decreased susceptibility to beta-lactams and the dynamic behavior of a loop.

Published

2005

36. Identical penicillin-binding domains in penicillin-binding proteins of Streptococcus pneumoniae clinical isolates with different levels of beta-lactam resistance

Author

André Zapun, Laurent Chesnel, Jacques Croize, Raphael Carapito, Otto Dideberg, Thierry Vernet, Laboratoire d'Ingénierie des Macromolécules (LIM), Institut de biologie structurale (IBS - UMR 5075 ), Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Centre National de la Recherche Scientifique (CNRS)-Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Centre National de la Recherche Scientifique (CNRS), Biotechnologie des interactions macromoléculaires (BIM), Université Louis Pasteur - Strasbourg I-Centre National de la Recherche Scientifique (CNRS), Centre National de la Recherche Scientifique (CNRS)-Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA), Institut de biologie structurale (IBS - UMR 5075), Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Grenoble Alpes (UGA)-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Grenoble Alpes (UGA)-Centre National de la Recherche Scientifique (CNRS), Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), and Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche Interdisciplinaire de Grenoble (IRIG)

Subjects

MESH: Sequence Analysis, DNA, Penicillin binding proteins, Sequence analysis, Molecular Sequence Data, Microbial Sensitivity Tests, Penicillins, Biology, medicine.disease_cause, beta-Lactam Resistance, Microbiology, 03 medical and health sciences, Bacterial Proteins, MESH: Penicillins, Mechanisms of Resistance, Streptococcus pneumoniae, Genotype, medicine, polycyclic compounds, Humans, Penicillin-Binding Proteins, Pharmacology (medical), Peptide Synthases, MESH: Bacterial Proteins, 030304 developmental biology, Antibacterial agent, Pharmacology, 0303 health sciences, MESH: Microbial Sensitivity Tests, MESH: Penicillin-Binding Proteins, MESH: Humans, MESH: Molecular Sequence Data, 030306 microbiology, Sequence Analysis, DNA, biochemical phenomena, metabolism, and nutrition, Streptococcaceae, biology.organism_classification, MESH: Peptide Synthases, MESH: beta-Lactam Resistance, 3. Good health, Penicillin, Infectious Diseases, [SDV.MP]Life Sciences [q-bio]/Microbiology and Parasitology, bacteria, Penicillin binding, Transformation, Bacterial, MESH: Transformation, Bacterial, MESH: Streptococcus pneumoniae, medicine.drug

Abstract

We have sequenced the penicillin-binding domains of the complete repertoire of penicillin-binding proteins and MurM from 22 clinical isolates of Streptococcus pneumoniae that span a wide range of β-lactam resistance levels. Evidence of mosaicism was found in the genes encoding PBP 1a, PBP 2b, PBP 2x, MurM, and, possibly, PBP 2a. Five isolates were found to have identical PBP and MurM sequences, even though the MICs for penicillin G ranged from 0.25 to 2.0 mg/liter. When the sequences encoding PBP 1a, PBP 2b, and PBP 2x from one of these isolates were used to transform laboratory strain R6, the resulting strain had a resistance level higher than that of the less resistant isolates carrying that PBP set but lower than that of the most resistant isolates carrying that PBP set. This result demonstrates that if the R6 strain is arbitrarily defined as the standard genotype, some wild genetic backgrounds can either increase or decrease the PBP-based resistance phenotype.

Published

2005

37. A PBP2x from a clinical isolate of Streptococcus pneumoniae exhibits an alternative mechanism for reduction of susceptibility to beta-lactam antibiotics

Author

Andréa Dessen, Otto Dideberg, Laurent Chesnel, Audrey Le Gouellec, Jacques Croize, Thierry Vernet, Lucile Pernot, Centre de Mathématiques Appliquées - Ecole Polytechnique (CMAP), École polytechnique (X)-Centre National de la Recherche Scientifique (CNRS), Shape reconstruction and identification (DeFI ), École polytechnique (X)-Centre National de la Recherche Scientifique (CNRS)-École polytechnique (X)-Centre National de la Recherche Scientifique (CNRS)-Inria Saclay - Ile de France, Institut National de Recherche en Informatique et en Automatique (Inria)-Institut National de Recherche en Informatique et en Automatique (Inria), Laboratoire des sciences et techniques de l'information, de la communication et de la connaissance (Lab-STICC), Université européenne de Bretagne - European University of Brittany (UEB)-École Nationale d'Ingénieurs de Brest (ENIB)-Université de Bretagne Sud (UBS)-Université de Brest (UBO)-Télécom Bretagne-Institut Brestois du Numérique et des Mathématiques (IBNM), Université de Brest (UBO)-École Nationale Supérieure de Techniques Avancées Bretagne (ENSTA Bretagne)-Institut Mines-Télécom [Paris] (IMT)-Centre National de la Recherche Scientifique (CNRS), Service de Bactériologie, Virologie, Hygiène [CHU Limoges], CHU Limoges, Institut de biologie structurale (IBS - UMR 5075 ), Centre National de la Recherche Scientifique (CNRS)-Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA), Inria Saclay - Ile de France, Institut National de Recherche en Informatique et en Automatique (Inria)-Institut National de Recherche en Informatique et en Automatique (Inria)-Centre de Mathématiques Appliquées - Ecole Polytechnique (CMAP), École polytechnique (X)-Centre National de la Recherche Scientifique (CNRS)-École polytechnique (X)-Centre National de la Recherche Scientifique (CNRS), École Nationale d'Ingénieurs de Brest (ENIB)-Université de Bretagne Sud (UBS)-Université de Brest (UBO)-Télécom Bretagne-Institut Brestois du Numérique et des Mathématiques (IBNM), Université de Brest (UBO)-Université européenne de Bretagne - European University of Brittany (UEB)-École Nationale Supérieure de Techniques Avancées Bretagne (ENSTA Bretagne)-Institut Mines-Télécom [Paris] (IMT)-Centre National de la Recherche Scientifique (CNRS), Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), and Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Models, Molecular, Penicillin binding proteins, MESH: Mutation, Protein Conformation, medicine.drug_class, [SDV]Life Sciences [q-bio], Molecular Sequence Data, Antibiotics, MESH: Carrier Proteins, Drug resistance, medicine.disease_cause, Biochemistry, beta-Lactam Resistance, Microbiology, 03 medical and health sciences, Antibiotic resistance, Protein structure, MESH: Protein Conformation, Streptococcus pneumoniae, medicine, Humans, Penicillin-Binding Proteins, Binding site, Molecular Biology, 030304 developmental biology, 0303 health sciences, MESH: Penicillin-Binding Proteins, Binding Sites, MESH: Humans, MESH: Molecular Sequence Data, biology, 030306 microbiology, Active site, Cell Biology, MESH: beta-Lactam Resistance, 3. Good health, MESH: Ribonucleoproteins, Ribonucleoproteins, MESH: Binding Sites, Mutation, biology.protein, Carrier Proteins, MESH: Models, Molecular, MESH: Streptococcus pneumoniae

Abstract

International audience; The human pathogen Streptococcus pneumoniae is one of the main causative agents of respiratory tract infections. At present, clinical isolates of S. pneumoniae often exhibit decreased susceptibility toward beta-lactams, a phenomenon linked to multiple mutations within the penicillin-binding proteins (PBPs). PBP2x, one of the six PBPs of S. pneumoniae, is the first target to be modified under antibiotic pressure. By comparing 89 S. pneumoniae PBP2x sequences from clinical and public data bases, we have identified one major group of sequences from drug-sensitive strains as well as two distinct groups from drug-resistant strains. The first group includes proteins that display high similarity to PBP2x from the well characterized resistant strain Sp328. The second group includes sequences in which a signature mutation, Q552E, is found adjacent to the third catalytic motif. In this work, a PBP2x from a representative strain from the latter group (S. pneumoniae 5259) was biochemically and structurally characterized. Phenotypical analyses of transformed pneumococci show that the Q552E substitution is responsible for most of the reduction of strain susceptibility toward beta-lactams. The crystal structure of 5259-PBP2x reveals a change in polarity and charge distribution around the active site cavity, as well as rearrangement of strand beta3, emulating structural changes observed for other PBPs that confer drug resistance to Gram-positive pathogens. Interestingly, the active site of 5259-PBP2x is in closed conformation, whereas that of Sp328-PBP2x is open. Consequently, S. pneumoniae has evolved to employ the same protein in two distinct mechanisms of antibiotic resistance.

Published

2004

38. Increase of the deacylation rate of PBP2x from Streptococcus pneumoniae by single point mutations mimicking the class A beta-lactamases

Author

Laurent, Chesnel, André, Zapun, Nicolas, Mouz, Otto, Dideberg, and Thierry, Vernet

Subjects

Kinetics, Streptococcus pneumoniae, Acylation, Hydrolysis, Penicillin-Binding Proteins, Point Mutation, Carrier Proteins, beta-Lactamases

Abstract

The class A beta-lactamases and the transpeptidase domain of the penicillin-binding proteins (PBPs) share the same topology and conserved active-site residues. They both react with beta-lactams to form acylenzymes. The stability of the PBP acylenzymes results in the inhibition of the transpeptidase function and the antibiotic activity of the beta-lactams. In contrast, the deacylation of the beta-lactamases is extremely fast, resulting in a high turnover of beta-lactam hydrolysis, which confers resistance to these antibiotics. In TEM-1 beta-lactamase from Escherichia coli, Glu166 is required for the fast deacylation and occupies the same spatial location as Phe450 in PBP2x from Streptococcus pneumoniae. To gain insight into the deacylation mechanism of both enzymes, Phe450 of PBP2x was replaced by various residues. The introduction of ionizable side chains increased the deacylation rate, in a pH-dependent manner, for the acidic residues. The aspartic acid-containing variant had a 110-fold faster deacylation at pH 8. The magnitude of this effect is similar to that observed in a naturally occurring variant of PBP2x, which confers increased resistance to cephalosporins.

Published

2002

39. The Capping Domain in RalF Regulates Effector Functions

Author

Laurent Chesnel, David O. Wood, Brad J. Bowzard, Craig R. Roy, Richard A. Kahn, Anna Delprato, Jacqueline Cherfils, Eric Alix, and Aimee M. Tucker

Subjects

Plasma protein binding, Biochemistry, Protein structure, Cricetinae, Molecular Cell Biology, Guanine Nucleotide Exchange Factors, Gram Negative, Small GTPase, Rickettsia prowazekii, lcsh:QH301-705.5, Cytoskeleton, 0303 health sciences, Effector, Cellular Structures, Enzymes, Bacterial Pathogens, Cell biology, Host-Pathogen Interaction, Membranes and Sorting, Guanine nucleotide exchange factor, Protein Binding, Research Article, lcsh:Immunologic diseases. Allergy, Immunology, Protein domain, CHO Cells, Biology, Microbiology, Legionella pneumophila, Enzyme Regulation, 03 medical and health sciences, Cricetulus, Bacterial Proteins, Virology, Genetics, Animals, Humans, Molecular Biology, Secretory pathway, 030304 developmental biology, 030306 microbiology, Cell Membrane, Protein Structure, Tertiary, lcsh:Biology (General), Membrane protein, Enzyme Structure, Parasitology, lcsh:RC581-607, HeLa Cells

Abstract

The Legionella pneumophila effector protein RalF functions as a guanine nucleotide exchange factor (GEF) that activates the host small GTPase protein ADP-ribosylation factor (Arf), and recruits this host protein to the vacuoles in which this pathogen resides. GEF activity is conferred by the Sec7 domain located in the N-terminal region of RalF. Structural studies indicate that the C-terminal region of RalF makes contacts with residues in the Sec7 domain important for Arf interactions. Theoretically, the C-terminal region of RalF could prevent nucleotide exchange activity by blocking the ability of Arf to interact with the Sec7 domain. For this reason, the C-terminal region of RalF has been termed a capping domain. Here, the role of the RalF capping domain was investigated by comparing biochemical and effector activities mediated by this domain in both the Legionella RalF protein (LpRalF) and in a RalF ortholog isolated from the unrelated intracellular pathogen Rickettsia prowazekii (RpRalF). These data indicate that both RalF proteins contain a functional Sec7 domain and that the capping domain regulates RalF GEF activity. The capping domain has intrinsic determinants that mediate localization of the RalF protein inside of host cells and confer distinct effector activities. Localization mediated by the capping domain of LpRalF enables the GEF to modulate membrane transport in the secretory pathway, whereas, the capping domain of RpRalF enables this bacterial GEF to modulate actin dynamics occurring near the plasma membrane. Thus, these data reveal that divergence in the function of the C-terminal capping domain alters the in vivo functions of the RalF proteins., Author Summary Legionella pneumophila and Rickettsia prowazekii are two pathogenic intracellular bacteria, phylogenetically distant and presenting different intracellular lifestyles. Interestingly, both organisms encode a protein called RalF, which in Legionella has been shown to be an effector protein that functions as a guanine nucleotide exchange factor (GEF) for the Arf family of eukaryotic GTPases. We show that the Sec7 domains in both proteins have a similar enzymatic ability to activate Arf1, however, the two proteins differ in their effector functions inside mammalian cells. The Legionella RalF protein targets secretory transport functions, whereas, the Rickettsia RalF protein modulates actin dynamics at the plasma membrane. These differences in RalF effector activities are mediated by a C-terminal domain that directs localization and interaction with host cell determinants. These data reveal important properties of the RalF protein that provide insight into differential roles for Arf during infection by Legionella and Rickettsia, and also provide a model for investigating how intracellular localization of structurally similar Arf GEFs enables a protein to regulate functionally distinct host cell processes.

Published

2012