Your search keyword '"Darren A. N. Cook"' showing total 19 results

1. Short-Course, High-Dose Rifampicin Achieves Wolbachia Depletion Predictive of Curative Outcomes in Preclinical Models of Lymphatic Filariasis and Onchocerciasis

Author

Ghaith Aljayyoussi, Hayley E. Tyrer, Louise Ford, Hanna Sjoberg, Nicolas Pionnier, David Waterhouse, Jill Davies, Joanne Gamble, Haelly Metuge, Darren A. N. Cook, Andrew Steven, Raman Sharma, Ana F. Guimaraes, Rachel H. Clare, Andrew Cassidy, Kelly L. Johnston, Laura Myhill, Laura Hayward, Samuel Wanji, Joseph D. Turner, Mark J. Taylor, and Stephen A. Ward

Subjects

Medicine, Science

Abstract

Abstract Lymphatic filariasis (LF) and onchocerciasis are priority neglected tropical diseases targeted for elimination. The only safe drug treatment with substantial curative activity against the filarial nematodes responsible for LF (Brugia malayi, Wuchereria bancrofti) or onchocerciasis (Onchocerca volvulus) is doxycycline. The target of doxycycline is the essential endosymbiont, Wolbachia. Four to six weeks doxycycline therapy achieves >90% depletion of Wolbachia in worm tissues leading to blockade of embryogenesis, adult sterility and premature death 18–24 months post-treatment. Long treatment length and contraindications in children and pregnancy are obstacles to implementing doxycycline as a public health strategy. Here we determine, via preclinical infection models of Brugia malayi or Onchocerca ochengi that elevated exposures of orally-administered rifampicin can lead to Wolbachia depletions from filariae more rapidly than those achieved by doxycycline. Dose escalation of rifampicin achieves >90% Wolbachia depletion in time periods of 7 days in B. malayi and 14 days in O. ochengi. Using pharmacokinetic-pharmacodynamic modelling and mouse-human bridging analysis, we conclude that clinically relevant dose elevations of rifampicin, which have recently been determined as safe in humans, could be administered as short courses to filariasis target populations with potential to reduce anti-Wolbachia curative therapy times to between one and two weeks.

Published

2017

2. Author Correction: Short-Course, High-Dose Rifampicin Achieves Wolbachia Depletion Predictive of Curative Outcomes in Preclinical Models of Lymphatic Filariasis and Onchocerciasis

Author

Ghaith Aljayyoussi, Hayley E. Tyrer, Louise Ford, Hanna Sjoberg, Nicolas Pionnier, David Waterhouse, Jill Davies, Joanne Gamble, Haelly Metuge, Darren A. N. Cook, Andrew Steven, Raman Sharma, Ana F. Guimaraes, Rachel H. Clare, Andrew Cassidy, Kelly L. Johnston, Laura Myhill, Laura Hayward, Samuel Wanji, Joseph D. Turner, Mark J. Taylor, and Stephen A. Ward

Subjects

Medicine, Science

Abstract

A correction to this article has been published and is linked from the HTML version of this paper. The error has been fixed in the paper.

Published

2018

3. Development of Pyrazolopyrimidine Anti-Wolbachia Agents for the Treatment of Filariasis

Author

Peter J. H. Webborn, Stefan Kavanagh, Andrew Cassidy, Paul M. O'Neill, Rachel H. Clare, Mark J. Taylor, Mark C. Wenlock, Neil G. Berry, W. David Hong, Darren A. N. Cook, Gemma L. Nixon, Stephen A. Ward, Paul McGillan, Suet C. Leung, Kelly L. Johnston, and Louise Ford

Subjects

wc_880, biology, Phenotypic screening, Organic Chemistry, qv_38, Pharmacology, biology.organism_classification, medicine.disease, Biochemistry, Pyrazolopyrimidine, In vitro, Filariasis, chemistry.chemical_compound, chemistry, In vivo, Pharmacodynamics, Drug Discovery, medicine, Wolbachia, Lead compound

Abstract

Anti-Wolbachia therapy has been identified as a viable treatment for combating filarial diseases. Phenotypic screening revealed a series of pyrazolopyrimidine hits with potent anti-Wolbachia activity. This paper focuses on the exploration of the SAR for this chemotype, with improvement of metabolic stability and solubility profiles using medicinal chemistry approaches. Organic synthesis has enabled functionalization of the pyrazolopyrimidine core at multiple positions, generating a library of compounds of which many analogues possess nanomolar activity against Wolbachia in vitro with improved DMPK parameters. A lead compound, 15f, was selected for in vivo pharmacokinetics (PK) profiling in mice. The combination of potent anti-Wolbachia activity in two in vitro assessments plus the exceptional oral PK profiles in mice puts this lead compound in a strong position for in vivo proof-of-concept pharmacodynamics studies and demonstrates the strong potential for further optimization and development of this series for treatment of filariasis in the future.

Published

2021

4. Preclinical development of an oral anti-Wolbachia macrolide drug for the treatment of lymphatic filariasis and onchocerciasis

Author

Sabine Specht, Thomas W. von Geldern, Kelly L. Johnston, Franziska Lenz, Samuel Wanji, Joseph D. Turner, Nicolas Pionnier, Abdel Jelil Njouendou, Dominique Bloemker, Darren A. N. Cook, Robert A. Carr, Louise Ford, Stephen A. Ward, Mark J. Taylor, Kennan C. Marsh, Marianne Koschel, Hanna T. Sjoberg, Howard E. Morton, Dale J. Kempf, John Archer, Hayley E. Tyrer, Haelly M. Metuge, Fanny Fri Fombad, Ghaith Aljayyoussi, Valerinne C. Chunda, Patrick W. N. Chounna, Rachel H. Clare, Marc P. Hübner, Alexandra Ehrens, Achim Hoerauf, Andrew Steven, and Emma A Murphy

Subjects

0301 basic medicine, Doxycycline, biology, business.industry, 030231 tropical medicine, General Medicine, Minocycline, Pharmacology, biology.organism_classification, medicine.disease, Brugia malayi, 03 medical and health sciences, Macrofilaricide, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, chemistry, parasitic diseases, medicine, Neglected tropical diseases, Wolbachia, Onchocerciasis, business, Lymphatic filariasis, medicine.drug

Abstract

There is an urgent global need for a safe macrofilaricide drug to accelerate elimination of the neglected tropical diseases onchocerciasis and lymphatic filariasis. From an anti-infective compound library, the macrolide veterinary antibiotic, tylosin A, was identified as a hit against Wolbachia. This bacterial endosymbiont is required for filarial worm viability and fertility and is a validated target for macrofilaricidal drugs. Medicinal chemistry was undertaken to develop tylosin A analogs with improved oral bioavailability. Two analogs, A-1535469 and A-1574083, were selected. Their efficacy was tested against the gold-standard second-generation tetracycline antibiotics, doxycycline and minocycline, in mouse and gerbil infection models of lymphatic filariasis (Brugia malayi and Litomosoides sigmodontis) and onchocerciasis (Onchocerca ochengi). A 1- or 2-week course of oral A-1535469 or A-1574083 provided >90% Wolbachia depletion from nematodes in infected animals, resulting in a block in embryogenesis and depletion of microfilarial worm loads. The two analogs delivered comparative or superior efficacy compared to a 3- to 4-week course of doxycycline or minocycline. A-1574083 (now called ABBV-4083) was selected for further preclinical testing. Cardiovascular studies in dogs and toxicology studies in rats and dogs revealed no adverse effects at doses (50 mg/kg) that achieved plasma concentrations >10-fold above the efficacious concentration. A-1574083 (ABBV-4083) shows potential as an anti-Wolbachia macrolide with an efficacy, pharmacology, and safety profile that is compatible with a short-term oral drug course for treating lymphatic filariasis and onchocerciasis.

Published

2019

5. AWZ1066S, a highly specific anti-Wolbachia drug candidate for a short-course treatment of filariasis

Author

Paul M. O'Neill, Edward W. Tate, W. David Hong, Adam P. Roberts, Marc P. Hübner, Peter J. H. Webborn, Mark J. Taylor, Alexandra Ehrens, Stefan J. Frohberger, Dominique Struever, John Archer, Farid Benayoud, Joseph D. Turner, Rachel H. Clare, Achim Hoerauf, Stefan Kavanagh, Fabian Gusovsky, Andrew Steven, Neil G. Berry, Kelly L. Johnston, Ghaith Aljayyoussi, Andrew Cassidy, Remigiusz A. Serwa, Suet C. Leung, Janet Hemingway, Alasdair T. M. Hubbard, Gemma L. Nixon, Amy Siu, Stephen A. Ward, Emma A Murphy, Louise Ford, Li Qie, Motohiro Shiotani, and Darren A. N. Cook

Subjects

0301 basic medicine, Drug, MACROFILARICIDAL ACTIVITY, Phenotypic screening, media_common.quotation_subject, 030231 tropical medicine, WUCHERERIA-BANCROFTI, medicine.disease_cause, Bioinformatics, drug discovery, Filariasis, DOUBLE-BLIND, 03 medical and health sciences, Macrofilaricide, chemistry.chemical_compound, 0302 clinical medicine, MD Multidisciplinary, medicine, BACTERIAL ENDOSYMBIONTS, macrofilaricide, lymphatic filariasis, ELIMINATION, Lymphatic filariasis, media_common, Science & Technology, LITOMOSOIDES-SIGMODONTIS, Multidisciplinary, biology, business.industry, onchocerciasis, ENDOBACTERIA, anti-Wolbachia, biology.organism_classification, medicine.disease, DOXYCYCLINE, Multidisciplinary Sciences, 030104 developmental biology, Wuchereria bancrofti, chemistry, Neglected tropical diseases, Science & Technology - Other Topics, Wolbachia, ALBENDAZOLE, business

Abstract

Onchocerciasis and lymphatic filariasis are two neglected tropical diseases that together affect ∼157 million people and inflict severe disability. Both diseases are caused by parasitic filarial nematodes with elimination efforts constrained by the lack of a safe drug that can kill the adult filaria (macrofilaricide). Previous proof-of-concept human trials have demonstrated that depleting >90% of the essential nematode endosymbiont bacterium, Wolbachia, using antibiotics, can lead to permanent sterilization of adult female parasites and a safe macrofilaricidal outcome. AWZ1066S is a highly specific anti-Wolbachia candidate selected through a lead optimization program focused on balancing efficacy, safety and drug metabolism/pharmacokinetic (DMPK) features of a thienopyrimidine/quinazoline scaffold derived from phenotypic screening. AWZ1066S shows superior efficacy to existing anti-Wolbachia therapies in validated preclinical models of infection and has DMPK characteristics that are compatible with a short therapeutic regimen of 7 days or less. This candidate molecule is well-positioned for onward development and has the potential to make a significant impact on communities affected by filariasis.

Published

2019

6. Laboratory evaluation of molecular xenomonitoring using mosquito excreta/feces to amplify Plasmodium, Brugia, and Trypanosoma DNA

Author

Michael F. Zulch, Darren A. N. Cook, Lisa J. Reimer, Steven A. Williams, Corrado Minetti, Joseph Pryce, and Nils Pilotte

Subjects

biology, Health Policy, 030231 tropical medicine, Public Health, Environmental and Occupational Health, Medicine (miscellaneous), Plasmodium falciparum, Computational biology, Trypanosoma brucei, biology.organism_classification, medicine.disease, Biochemistry, Genetics and Molecular Biology (miscellaneous), Brugia malayi, 03 medical and health sciences, 0302 clinical medicine, Immunology and Microbiology (miscellaneous), Trypanosoma, medicine, Digital polymerase chain reaction, 030212 general & internal medicine, Pathogen, Feces, Malaria

Abstract

Background: Results from an increasing number of studies suggest that mosquito excreta/feces (E/F) testing has considerable potential to serve as a supplement for traditional molecular xenomonitoring techniques. However, as the catalogue of possible use-cases for this methodology expands, and the list of amenable pathogens grows, a number of fundamental methods-based questions remain. Answering these questions is critical to maximizing the utility of this approach and to facilitating its successful implementation as an effective tool for molecular xenomonitoring.Methods: Utilizing E/F produced by mosquitoes or tsetse flies experimentally exposed toBrugia malayi,Plasmodium falciparum, orTrypanosoma brucei brucei, factors such as limits of detection, throughput of testing, adaptability to use with competent- and incompetent-vector species, and effects of additional blood feedings post parasite-exposure were evaluated. Two platforms for the detection of pathogen signal (quantitative real-time PCR and digital PCR [dPCR]) were also compared, with strengths and weaknesses examined for each. Results: Experimental results indicated that high throughput testing is possible when evaluating mosquito E/F for the presence of eitherB. malayiorP. falciparumfrom both competent- and incompetent-vector mosquito species. Furthermore, following exposure to pathogen, providing mosquitoes with a second, uninfected bloodmeal did not expand the temporal window for E/F collection during which pathogen detection was possible. However, this collection window did appear longer in E/F collected from tsetse flies following exposure toT. b. brucei. Testing also suggested that dPCR may facilitate detection through its increased sensitivity. Unfortunately, logistical obstacles will likely make the large-scale use of dPCR impractical for this purpose.Conclusions: By examining many E/F testing variables, expansion of this technology to a field-ready platform has become increasingly feasible. However, translation of this methodology from the lab to the field will first require the completion of field-based pilot studies aimed at assessing the efficacy of E/F screening.

Published

2019

7. Author Correction: Short-Course, High-Dose Rifampicin Achieves Wolbachia Depletion Predictive of Curative Outcomes in Preclinical Models of Lymphatic Filariasis and Onchocerciasis

Author

David Waterhouse, Laura Hayward, Samuel Wanji, Hayley E. Tyrer, Laura Myhill, Andrew Steven, Andrew Cassidy, Stephen A. Ward, Nicolas Pionnier, Hanna T. Sjoberg, Kelly L. Johnston, Joseph D. Turner, Mark J. Taylor, Rachel H. Clare, Jill Davies, Raman Sharma, Ghaith Aljayyoussi, Louise Ford, Ana F. Guimaraes, Haelly M. Metuge, Darren A. N. Cook, and Joanne Gamble

Subjects

DNA, Bacterial, 0301 basic medicine, Science, 030231 tropical medicine, Administration, Oral, Embryonic Development, Onchocerciasis, Bioinformatics, Article, Mice, 03 medical and health sciences, Elephantiasis, Filarial, 0302 clinical medicine, parasitic diseases, medicine, Animals, Humans, Wuchereria bancrofti, Short course, Author Correction, Brugia malayi, Filarioidea, Lymphatic filariasis, Multidisciplinary, biology, business.industry, qs_4, medicine.disease, biology.organism_classification, Anti-Bacterial Agents, Disease Models, Animal, Onchocerca volvulus, Treatment Outcome, 030104 developmental biology, Medicine, Wolbachia, Rifampin, business, Rifampicin, medicine.drug

Abstract

Lymphatic filariasis (LF) and onchocerciasis are priority neglected tropical diseases targeted for elimination. The only safe drug treatment with substantial curative activity against the filarial nematodes responsible for LF (Brugia malayi, Wuchereria bancrofti) or onchocerciasis (Onchocerca volvulus) is doxycycline. The target of doxycycline is the essential endosymbiont, Wolbachia. Four to six weeks doxycycline therapy achieves >90% depletion of Wolbachia in worm tissues leading to blockade of embryogenesis, adult sterility and premature death 18–24 months post-treatment. Long treatment length and contraindications in children and pregnancy are obstacles to implementing doxycycline as a public health strategy. Here we determine, via preclinical infection models of Brugia malayi or Onchocerca ochengi that elevated exposures of orally-administered rifampicin can lead to Wolbachia depletions from filariae more rapidly than those achieved by doxycycline. Dose escalation of rifampicin achieves >90% Wolbachia depletion in time periods of 7 days in B. malayi and 14 days in O. ochengi. Using pharmacokinetic-pharmacodynamic modelling and mouse-human bridging analysis, we conclude that clinically relevant dose elevations of rifampicin, which have recently been determined as safe in humans, could be administered as short courses to filariasis target populations with potential to reduce anti-Wolbachia curative therapy times to between one and two weeks.

Published

2018

8. Development and Validation of a High-Throughput Anti-Wolbachia Whole-Cell Screen: A Route to Macrofilaricidal Drugs against Onchocerciasis and Lymphatic Filariasis

Author

Darren A. N. Cook, Louise Ford, Mark J. Taylor, Kelly L. Johnston, Stephen A. Ward, and Rachel H. Clare

Subjects

Computational biology, Biology, Onchocerciasis, Biochemistry, Cell Line, Analytical Chemistry, Elephantiasis, Filarial, Drug Discovery, medicine, Animals, Humans, Throughput (business), Lymphatic filariasis, Dose-Response Relationship, Drug, Drug discovery, Antinematodal Agents, Neglected Diseases, Reproducibility of Results, medicine.disease, biology.organism_classification, Anti-Bacterial Agents, High-Throughput Screening Assays, High-content screening, Immunology, Molecular Medicine, Wolbachia, Classical pharmacology, Onchocerca, Whole cell, Biotechnology

Abstract

There is an urgent need to develop new, safe, and affordable macrofilaricidal drugs for onchocerciasis and lymphatic filariasis treatment and control. The Anti-Wolbachia Consortium (A·WOL) aims to provide a novel treatment with macrofilaricidal activity by targeting the essential bacterial symbiont Wolbachia. The consortium is currently screening a diverse range of compounds to find new chemical space to drive this drug discovery initiative and address this unmet demand. To increase the throughput and capacity of the A·WOL cell-based screen, we have developed a 384-well format assay using a high-content imaging system (Operetta) in conjunction with optimized Wolbachia growth dynamics in the C6/36 Aedes albopictus mosquito cell line. This assay uses texture analysis of cells stained with SYTO 11 as a direct measure of bacterial load. This validated assay has dramatically increased the capacity and throughput of the A·WOL compound library screening program 25-fold, enriching the number of new anti-Wolbachia hits identified for further development as potential macrofilaricides for onchocerciasis and lymphatic filariasis.

Published

2015

9. Albendazole and antibiotics synergize to deliver short-course anti- Wolbachia curative treatments in preclinical models of filariasis

Author

Mark J. Taylor, Rachel H. Clare, Louise Ford, Andrew Steven, Richard S. Priestley, Emma A Murphy, Joseph D. Turner, Janet Hemingway, Jill Davies, John McCall, David Waterhouse, Stephen A. Ward, Andrew Cassidy, Hayley E. Tyrer, Kelly L. Johnston, Raman Sharma, Darren A. N. Cook, Laura Hayward, Joanne Gamble, and Ghaith Al Jayoussi

Subjects

0301 basic medicine, Combination therapy, medicine.drug_class, 030231 tropical medicine, Antibiotics, Pharmacology, Biology, Albendazole, Filariasis, 03 medical and health sciences, Macrofilaricide, chemistry.chemical_compound, 0302 clinical medicine, parasitic diseases, medicine, Anthelmintic, Multidisciplinary, A100, biochemical phenomena, metabolism, and nutrition, medicine.disease, biology.organism_classification, 3. Good health, 030104 developmental biology, Synergy, chemistry, Immunology, bacteria, Wolbachia, medicine.drug

Abstract

Significance Filarial nematode infections, caused by Wuchereria bancrofti , Brugia malayi (elephantiasis), and Onchocerca volvulus (river blindness) infect 150 million of the world’s poorest populations and cause profound disability. Standard treatments require repetitive, long-term, mass drug administrations and have failed to interrupted transmission in certain sub-Saharan African regions. A drug cure using doxycycline, which targets the essential filarial endosymbiont Wolbachia , is clinically effective but programmatically challenging to implement due to long treatment durations and contraindications. Here we provide proof-of-concept of a radical improvement of targeting Wolbachia via identification of drug synergy between the anthelmintic albendazole and antibiotics. This synergy enables the shortening of treatment duration of macrofilaricidal anti- Wolbachia based treatments from 4 wk to 7 d with registered drugs ready for clinical testing.

Published

2017

10. Short-Course, High-Dose Rifampicin Achieves Wolbachia Depletion Predictive of Curative Outcomes in Preclinical Models of Lymphatic Filariasis and Onchocerciasis

Author

Jill Davies, Nicolas Pionnier, Hanna T. Sjoberg, Laura Hayward, Samuel Wanji, Ana F. Guimaraes, David Waterhouse, Hayley E. Tyrer, Joanne Gamble, Joseph D. Turner, Andrew Steven, Rachel H. Clare, Louise Ford, Laura Myhill, Mark J. Taylor, Stephen A. Ward, Ghaith Aljayyoussi, Darren A. N. Cook, Andrew Cassidy, Raman Sharma, Haelly M. Metuge, and Kelly L. Johnston

Subjects

0301 basic medicine, Science, C111, 030231 tropical medicine, medicine.disease_cause, Brugia malayi, Filariasis, 03 medical and health sciences, 0302 clinical medicine, parasitic diseases, medicine, Lymphatic filariasis, Doxycycline, Multidisciplinary, biology, biology.organism_classification, medicine.disease, Onchocerca volvulus, 3. Good health, 030104 developmental biology, Wuchereria bancrofti, Immunology, Medicine, Wolbachia, Onchocerciasis, medicine.drug

Abstract

Lymphatic filariasis (LF) and onchocerciasis are priority neglected tropical diseases targeted for elimination. The only safe drug treatment with substantial curative activity against the filarial nematodes responsible for LF (Brugia malayi, Wuchereria bancrofti) or onchocerciasis (Onchocerca volvulus) is doxycycline. The target of doxycycline is the essential endosymbiont, Wolbachia. Four to six weeks doxycycline therapy achieves >90% depletion of Wolbachia in worm tissues leading to blockade of embryogenesis, adult sterility and premature death 18–24 months post-treatment. Long treatment length and contraindications in children and pregnancy are obstacles to implementing doxycycline as a public health strategy. Here we determine, via preclinical infection models of Brugia malayi or Onchocerca ochengi that elevated exposures of orally-administered rifampicin can lead to Wolbachia depletions from filariae more rapidly than those achieved by doxycycline. Dose escalation of rifampicin achieves >90% Wolbachia depletion in time periods of 7 days in B. malayi and 14 days in O. ochengi. Using pharmacokinetic-pharmacodynamic modelling and mouse-human bridging analysis, we conclude that clinically relevant dose elevations of rifampicin, which have recently been determined as safe in humans, could be administered as short courses to filariasis target populations with potential to reduce anti-Wolbachia curative therapy times to between one and two weeks.

Published

2017

11. Filarial infection influences mosquito behaviour and fecundity

Author

Mark J. Taylor, Lisa J. Reimer, Darren A. N. Cook, and Katherine Gleave

Subjects

0301 basic medicine, Mosquito Control, 030231 tropical medicine, Aedes aegypti, Article, Brugia malayi, Filariasis, 03 medical and health sciences, Elephantiasis, Filarial, 0302 clinical medicine, Aedes, parasitic diseases, medicine, Animals, Humans, Lymphatic filariasis, Multidisciplinary, Behavior, Animal, biology, Host (biology), fungi, biology.organism_classification, Fecundity, medicine.disease, Virology, Insect Vectors, Mosquito control, 030104 developmental biology, Larva, Female

Abstract

Understanding vector-parasite interactions is increasingly important as we move towards the endpoint goals set by the Global Programme for the Elimination of Lymphatic Filariasis (GPELF), as interaction dynamics may change with reduced transmission pressure. Elimination models used to predict programmatic endpoints include parameters for vector-specific transmission dynamics, despite the fact that our knowledge of the host-seeking behaviour of filariasis infected mosquitoes is lacking. We observed a dynamic, stage-specific and density dependent change in Aedes aegypti behaviour towards host cues when exposed to Brugia malayi filarial parasites. Infected mosquitoes exhibited reduced activation and flight towards a host during the period of larval development (L1/L2), transitioning to a 5 fold increase in activation and flight towards a host when infective stage larvae (L3) were present (p

Published

2016

12. Minocycline as a re-purposed anti-Wolbachia macrofilaricide: superiority compared with doxycycline regimens in a murine infection model of human lymphatic filariasis

Author

Joanne Gamble, David Waterhouse, Laura Myhill, Jill Davies, Rachel H. Clare, Hayley E. Tyrer, Andrew Cassidy, Stephen A. Ward, Laura Hayward, Darren A. N. Cook, Ana F. Guimaraes, Louise Ford, Ghaith Al Jayoussi, Andrew Steven, Raman Sharma, Kelly L. Johnston, Mark J. Taylor, and Joseph D. Turner

Subjects

0301 basic medicine, 030231 tropical medicine, C111, Pharmacology, Article, Brugia malayi, Filariasis, 03 medical and health sciences, Macrofilaricide, chemistry.chemical_compound, 0302 clinical medicine, parasitic diseases, medicine, Lymphatic filariasis, Doxycycline, Multidisciplinary, biology, business.industry, Minocycline, biology.organism_classification, medicine.disease, 3. Good health, Regimen, 030104 developmental biology, chemistry, Pharmacodynamics, Immunology, business, medicine.drug

Abstract

Lymphatic filariasis and onchocerciasis are parasitic helminth diseases, which cause severe morbidities such as elephantiasis, skin disease and blindness, presenting a major public health burden in endemic communities. The anti-Wolbachia consortium (A·WOL: http://www.a-wol.com/) has identified a number of registered antibiotics that target the endosymbiotic bacterium, Wolbachia, delivering macrofilaricidal activity. Here we use pharmacokinetics/pharmacodynamics (PK/PD) analysis to rationally develop an anti-Wolbachia chemotherapy by linking drug exposure to pharmacological effect. We compare the pharmacokinetics and anti-Wolbachia efficacy in a murine Brugia malayi model of minocycline versus doxycycline. Doxycycline exhibits superior PK in comparison to minocycline resulting in a 3-fold greater exposure in SCID mice. Monte-Carlo simulations confirmed that a bi-daily 25–40 mg/Kg regimen is bioequivalent to a clinically effective 100–200 mg/day dose for these tetracyclines. Pharmacodynamic studies showed that minocycline depletes Wolbachia more effectively than doxycycline (99.51% vs. 90.35%) after 28 day 25 mg/Kg bid regimens with a more potent block in microfilarial production. PK/PD analysis predicts that minocycline would be expected to be 1.7 fold more effective than doxycycline in man despite lower exposure in our infection models. Our findings warrant onward clinical investigations to examine the clinical efficacy of minocycline treatment regimens against lymphatic filariasis and onchocerciasis.

Published

2016

13. Research strategies to improve snakebite treatment: Challenges and progress

Author

Robert A. Harrison, Darren A. N. Cook, Nicholas R. Casewell, Rachel B. Currier, Simon C. Wagstaff, and Camila Renjifo

Subjects

Organizations, medicine.medical_specialty, Antivenins, business.industry, International Cooperation, Research, Biophysics, Snake Bites, Biochemistry, Disadvantaged, Research strategies, Research community, Intervention (counseling), medicine, Humans, Effective treatment, Preventable death, Intensive care medicine, business, Delivery of Health Care

Abstract

Antivenom is an effective treatment of snakebite but, because of the complex interplay of fiscal, epidemiological, therapeutic efficacy and safety issues, the mortality of snakebite remains unacceptably high. Efficiently combating this high level of preventable death amongst the world's most disadvantaged communities requires the globally-coordinated action of multiple intervention programmes. This is the overall objective of the Global Snakebite Initiative. This paper describes the challenges facing the research community to develop snakebite treatments that are more efficacious, safe and affordable than current therapy.

Published

2011

14. Brugia malayi microfilariae adhere to human vascular endothelial cells in a C3-dependent manner

Author

Jan Hendrik Schroeder, Alister Craig, Charlotte Lawson, Rachel A. Lawrence, David McCarthy, Tadge Szestak, Mark J. Taylor, and Darren A. N. Cook

Subjects

0301 basic medicine, Nematoda, Physiology, Pathogenesis, Pathology and Laboratory Medicine, Biochemistry, Epithelium, Brugia malayi, 0302 clinical medicine, Animal Cells, Medicine and Health Sciences, Brugia Malayi, Lymphatic filariasis, Melatonin, Flow Rate, biology, lcsh:Public aspects of medicine, Physics, Classical Mechanics, Complement C3, qs_532, Body Fluids, Cell biology, Chemistry, Blood, Infectious Diseases, medicine.anatomical_structure, qx_510, Host-Pathogen Interactions, Physical Sciences, 293T cells, Cell lines, Anatomy, Cellular Types, medicine.symptom, Biological cultures, Research Article, Chemical Elements, medicine.drug, wc_880, lcsh:Arctic medicine. Tropical medicine, lcsh:RC955-962, 030231 tropical medicine, Fluid Mechanics, Continuum Mechanics, 03 medical and health sciences, parasitic diseases, Brugia, Cell Adhesion, Human Umbilical Vein Endothelial Cells, medicine, Animals, Humans, Cell adhesion, Lung, HEK 293 cells, Organisms, Public Health, Environmental and Occupational Health, Biology and Life Sciences, Endothelial Cells, lcsh:RA1-1270, Epithelial Cells, Fluid Dynamics, Cell Biology, Hypoxia (medical), biology.organism_classification, medicine.disease, Invertebrates, Hormones, Oxygen, Research and analysis methods, Biological Tissue, 030104 developmental biology, Nematode, Immunology, qu_350

Abstract

Brugia malayi causes the human tropical disease, lymphatic filariasis. Microfilariae (Mf) of this nematode live in the bloodstream and are ingested by a feeding mosquito vector. Interestingly, in a remarkable co-evolutionary adaptation, Mf appearance in the peripheral blood follows a circadian periodicity and reaches a peak when the mosquito is most likely to feed. For the remaining hours, the majority of Mf sequester in the lung capillaries. This circadian phenomenon has been widely reported and is likely to maximise parasite fitness and optimise transmission potential. However, the mechanism of Mf sequestration in the lungs remains largely unresolved. In this study, we demonstrate that B. malayi Mf can, directly adhere to vascular endothelial cells under static conditions and under flow conditions, they can bind at high (but not low) flow rates. High flow rates are more likely to be experienced diurnally. Furthermore, a non-periodic nematode adheres less efficiently to endothelial cells. Strikingly C3, the central component of complement, plays a crucial role in the adherence interaction. These novel results show that microfilariae have the ability to bind to endothelial cells, which may explain their sequestration in the lungs, and this binding is increased in the presence of inflammatory mediators.

Published

2017

15. A murine macrofilaricide pre-clinical screening model for onchocerciasis and lymphatic filariasis

Author

Samuel Wanji, Hayley E. Tyrer, Haelly M. Metuge, Peter Enyong, Chounna N.dongmo Winston Patrick, Joseph D. Turner, Kengne Ouafo J.onas Arnaud, Mark J. Taylor, Tayong Dizzle Bita Kwenti, Andrew Steven, Darren A. N. Cook, George Forsbrook, Alice Halliday, and Ana F. Guimaraes

Subjects

Male, wc_880, Anti-filarial, Menotropins, Mycology & Parasitology, Mice, SCID, Elephantiasis, Onchocerciasis, wc_885, Brugia malayi, Mice, Macrofilaricide, chemistry.chemical_compound, Elephantiasis, Filarial, 1108 Medical Microbiology, qv_771, parasitic diseases, Brugia, medicine, Animals, Onchocerca, Lymphatic filariasis, Mice, Inbred BALB C, biology, business.industry, Research, A100, medicine.disease, biology.organism_classification, Filaricides, Infectious Diseases, 1117 Public Health And Health Services, chemistry, Drug development, Immunology, Female, Parasitology, Gerbillinae, business, Wolbachia

Abstract

Background: New drugs effective against adult filariae (macrofilaricides) would accelerate the elimination of lymphatic filariasis and onchocerciasis. Anti-Onchocerca drug development is hampered by the lack of a facile model. We postulated that SCID mice could be developed as a fmacrofilaricide screening model.\ud \ud Methods: The filaricides: albendazole (ABZ), diethylcarbamazine (DEC), flubendazole (FBZ), ivermectin (IVM) and the\ud anti-Wolbachia macrofilaricide, minocycline (MIN) were tested in Brugia malayi (Bm)-parasitized BALB/c SCID mice vs\ud vehicle control (VC). Responses were compared to BALB/c wild type (WT). Onchocerca ochengi male worms or\ud onchocercomata were surgically implanted into BALB/c SCID, CB.17 SCID, BALB/c WT mice or Meriones gerbils. Survival\ud was evaluated at 7–15 days. BALB/c SCID were tested to evaluate the responsiveness of pre-clinical macrofilaricides FBZ\ud and rifapentine (RIFAP) against male Onchocerca.\ud \ud Results: WT and SCID responded with >95% efficacy following ABZ or DEC treatments against Bm larvae (P < 0.0001).\ud IVM was partially filaricidal against Bm larvae in WT and SCID (WT; 39.8%, P = 0.0356 and SCID; 56.7%, P = 0.026). SCID\ud responded similarly to WT following IVM treatment of microfilaraemias (WT; 79%, P = 0.0194. SCID; 76%, P = 0.0473). FBZ\ud induced a total macrofilaricidal response against adult Bm in WT and SCID (WT; P = 0.0067, SCID; P = 0.0071). MIN\ud induced a >90% reduction in Bm Wolbachia burdens (P < 0.0001) and a blockade of microfilarial release (P = 0.0215) in\ud SCID. Male Onchocerca survival was significantly higher in SCID vs WT mice, but not gerbils, after +15 days (60% vs 22% vs\ud 39% P = 0.0475). Onchocercoma implants had engrafted into host tissues, with evidence of neovascularisation, after +7\ud days and yielded viable macro/microfilariae ex vivo. FBZ induced a macrofilaricidal effect in Onchocerca male implanted\ud SCID at +5 weeks (FBZ; 1.67% vs VC; 43.81%, P = 0.0089). Wolbachia loads within male Onchocerca were reduced by 99%\ud in implanted SCID receiving RIFAP for +2 weeks.\ud \ud Conclusions: We have developed a ‘pan-filarial’ small animal research model that is sufficiently robust, with adequate\ud capacity and throughput, to screen existing and future pre-clinical candidate macrofilaricides. Pilot data suggests a murine\ud onchocercoma xenograft model is achievable.

Published

2014

16. Medically important differences in snake venom composition are dictated by distinct postgenomic mechanisms

Author

Wolfgang Wüster, Libia Sanz, Simon C. Wagstaff, Davinia Pla, Juan J. Calvete, Sarah I. King, Nicholas R. Casewell, Fiona M.S. Bolton, Robert A. Harrison, and Darren A. N. Cook

Subjects

Proteome, Transcription, Genetic, Snake Bites, Venom, Bioinformatics, complex mixtures, Evolution, Molecular, Species Specificity, Viperidae, biology.animal, Crotalid Venoms, medicine, Gene family, Animals, Gene, Regulation of gene expression, Multidisciplinary, biology, Neglected Diseases, Venom Protein, Biological Sciences, medicine.disease, Snake bites, Gene Expression Regulation, Snake venom, Evolutionary biology, Protein Biosynthesis, Protein Processing, Post-Translational

Abstract

6 páginas, 4 figuras. Este artículo contiene información suplementaria online en: www.pnas.org/lookup/suppl/doi:10.1073/pnas.1405484111/-/DCSupplemental, Variation in venom composition is a ubiquitous phenomenon in snakes and occurs both interspecifically and intraspecifically. Venom variation can have severe outcomes for snakebite victims by rendering the specific antibodies found in antivenoms ineffective against heterologous toxins found in different venoms. The rapid evolutionary expansion of different toxin-encoding gene families in different snake lineages is widely perceived as the main cause of venom variation. However, this view is simplistic and disregards the understudied influence that processes acting on gene transcription and translation may have on the production of the venom proteome. Here, we assess the venom composition of six related viperid snakes and compare interspecific changes in the number of toxin genes, their transcription in the venom gland, and their translation into proteins secreted in venom. Our results reveal that multiple levels of regulation are responsible for generating variation in venom composition between related snake species. We demonstrate that differential levels of toxin transcription, translation, and their posttranslational modification have a substantial impact upon the resulting venom protein mixture. Notably, these processes act to varying extents on different toxin paralogs found in different snakes and are therefore likely to be as important as ancestral gene duplication events for generating compositionally distinct venom proteomes. Our results suggest that these processes may also contribute to altering the toxicity of snake venoms, and we demonstrate how this variability can undermine the treatment of a neglected tropical disease, snakebite., This work was funded by NERC UK Research Studentship NER/S/A/2006/14086 and Postdoctoral Research Fellowship NE/J018678/1 (to N.R.C.), access to the NERC Molecular Genetics Facility at the University of Edinburgh from Grant MGF150 (to W.W.), a Leverhulme Trust Grant F/00174/I (to W.W. and R.A.H.), a National Centre for the Replacement, Refinement and Reduction of Animals in Research Studentship NC/K500288/1 (to R.A.H.), Ministerio de Ciencia é Innovación (currently Ministerio de Economía y Competitividad), Madrid Grant BFU2010-17373 and the Generalitat Valenciana Grant PROMETEO/2010/005 (to J.J.C.).

Published

2014

17. Analysis of camelid IgG for antivenom development: Serological responses of venom-immunised camels to prepare either monospecific or polyspecific antivenoms for West Africa

Author

Robert A. Harrison, Simon C. Wagstaff, Darren A. N. Cook, Ulrich Wernery, Joerg Kinne, and Timothy Owen

Subjects

Echis ocellatus, Camelus, biology, Antivenins, Antivenom, Enzyme-Linked Immunosorbent Assay, Toxicology, medicine.disease, biology.organism_classification, complex mixtures, Snake bites, Bitis, Africa, Western, Immunoglobulin G, Immunology, medicine, Animals, Avidity, Snake antivenom, Envenomation, Camelid, Snake Venoms

Abstract

Snake envenoming is a significant cause of mortality and morbidity in sub-Saharan Africa. The only effective treatment, antivenom, has been in short supply since the 1990s. Whilst the humanitarian response by some antivenom producers has significantly improved the situation, strategies to ensure the long term stability of antivenom supply are still necessary. We are investigating whether the potential safety and logistic advantages of camel IgG antivenom can be exploited to improve antivenom provision in many countries where snakebite is endemic. This study assessed the IgG titre, specificity and avidity of camels immunised with either individual venom or a mixture of venoms from the three most medically important snakes of West Africa, the saw-scale viper (Echis ocellatus), the puff adder (Bitis arietans) and the spitting cobra (Naja nigricollis). Seven of the eight immunised camels generated IgG titres and avidities comparable to, or exceeding, that of commercial equine and ovine antivenoms that are highly effective in envenomed patients. In this, the first of a series of reports on the potential utility of camelid IgG antivenom, we describe an immunisation protocol that induced potent, sustained serological response of very high antibody avidity. These attributes suggest, from an immunological perspective, that camel IgG antivenoms should be as efficacious as current equine and ovine antivenoms.

Published

2010

18. Reply to Professor Ratanabanangkoon’s letter entitled ‘D.A.N. Cook et al.’s account of the immunization of camels is at variance with the ‘low dose, low volume multi-site’ immunization protocol’

Author

Ulrich Wernery, Simon C. Wagstaff, Robert A. Harrison, Joerg Kinne, and Darren A. N. Cook

Subjects

Low volume, Protocol (science), Pediatrics, medicine.medical_specialty, Immunization, business.industry, Immunology, Low dose, medicine, Multi site, Variance (accounting), Toxicology, business

Published

2010

19. Pre-Clinical Assays Predict Pan-African Echis Viper Efficacy for a Species-Specific Antivenom

Author

Darren A. N. Cook, Wolfgang Wüster, Nandul Durfa, Nicholas R. Casewell, Abdulsalami Nasidi, Robert A. Harrison, and Simon C. Wagstaff

Subjects

Veterinary medicine, lcsh:Arctic medicine. Tropical medicine, VIPeR, lcsh:RC955-962, Immunoblotting, 030231 tropical medicine, Antivenom, Drug Evaluation, Preclinical, Snake Bites, Zoology, Enzyme-Linked Immunosorbent Assay, Venom, Viper Venoms, complex mixtures, Mice, 03 medical and health sciences, 0302 clinical medicine, Echis, Neutralization Tests, Viperidae, biology.animal, medicine, Animals, Humans, Envenomation, Africa South of the Sahara, 030304 developmental biology, 0303 health sciences, biology, Antivenins, business.industry, lcsh:Public aspects of medicine, Public Health, Environmental and Occupational Health, lcsh:RA1-1270, Venom Protein, medicine.disease, biology.organism_classification, Antibodies, Neutralizing, Survival Analysis, Snake bites, 3. Good health, Disease Models, Animal, Infectious Diseases, Infectious Diseases/Neglected Tropical Diseases, Electrophoresis, Polyacrylamide Gel, business, Research Article

Abstract

Background Snakebite is a significant cause of death and disability in subsistent farming populations of sub-Saharan Africa. Antivenom is the most effective treatment of envenoming and is manufactured from IgG of venom-immunised horses/sheep but, because of complex fiscal reasons, there is a paucity of antivenom in sub-Saharan Africa. To address the plight of thousands of snakebite victims in savannah Nigeria, the EchiTAb Study Group organised the production, testing and delivery of antivenoms designed to treat envenoming by the most medically-important snakes in the region. The Echis saw-scaled vipers have a wide African distribution and medical importance. In an effort to maximise the clinical utility of scarce antivenom resources in Africa, we aimed to ascertain, at the pre-clinical level, to what extent the E. ocellatus-specific EchiTAbG antivenom, which was designed specifically for Nigeria, neutralised the lethal activity of venom from two other African species, E. pyramidum leakeyi and E. coloratus. Methodology/Principal Findings Despite apparently quite distinctive venom protein profiles, we observed extensive cross-species similarity in the immuno-reactivity profiles of Echis species-specific antisera. Using WHO standard pre-clinical in vivo tests, we determined that the monospecific EchiTAbG antivenom was as effective at neutralising the venom-induced lethal effects of E. pyramidum leakeyi and E. coloratus as it was against E. ocellatus venom. Under the restricted conditions of this assay, the antivenom was ineffective against the lethal effects of venom from the non-African Echis species, E. carinatus sochureki. Conclusions/Significance Using WHO-recommended pre-clinical tests we have demonstrated that the new anti-E. ocellatus monospecific antivenom EchiTAbG, developed in response to the considerable snakebite-induced mortality and morbidity in Nigeria, neutralised the lethal effects of venoms from Echis species representing each taxonomic group of this genus in Africa. This suggests that this monospecific antivenom has potential to treat envenoming by most, perhaps all, African Echis species., Author Summary Snakebite is principally a health concern of rural poor communities. The high snakebite risk of subsistence farming and paucity of effective antivenoms in sub-Saharan Africa means that many communities remain unacceptably vulnerable to snakebite mortality and morbidity. There is therefore a compelling need to maximise the utility of the snakebite therapies that are available. To address Nigeria's severe snakebite problem, the government funded a collaboration of ministry officials, antivenom manufacturers and academics (the EchiTAb Study Group) to produce, test and deliver antivenom. Accordingly, we prepared EchiTAbG, an antivenom specific for envenoming by the saw-scaled viper (E. ocellatus) which is responsible for 80% of snakebite deaths in Nigeria. Since E. ocellatus is widely distributed across the West African savannah, EchiTAbG offers considerable therapeutic promise in many countries in the region. Since other Echis species represent public health concerns elsewhere in Africa, the objective of this study was to examine the pre-clinical intra-generic venom-neutralising efficacy of EchiTAbG. Our results suggest that EchiTAbG (Nigeria registration: A6-0078) has pan-African efficacy against Echis envenoming indicating that costly investment in region-specific antivenoms therefore may not be required. This represents an important progression to minimise development costs and maximise the delivery of snakebite therapy for the continent.

Published

2010