Your search keyword '"Nolder, D"' showing total 40 results

1. Diagnosis and Clinical Management of Chagas Disease: An Increasing Challenge in Non-Endemic Areas

Author

Suárez C, Nolder D, García-Mingo A, Moore DAJ, and Chiodini PL

Subjects

trypanosoma cruzi, antenatal, transplant, migrant, screening, prevention, Arctic medicine. Tropical medicine, RC955-962

Abstract

Cristina Suárez,1,2 Debbie Nolder,1,3 Ana García-Mingo,1,4 David AJ Moore,1,5,6 Peter L Chiodini1,5,7 1UK Chagas Hub, London, UK; 2Department of Infection, Barts Health NHS Trust, London, UK; 3Diagnostic Parasitology Laboratory, London School of Hygiene & Tropical Medicine, London, UK; 4Microbiology Department, Whittington Health NHS Trust, London, UK; 5Hospital for Tropical Diseases, University College London Hospitals NHS Trust;, London, UK; 6Department of Clinical Research, Faculty of Infectious and Tropical Diseases, London School of Hygiene and Tropical Medicine, London, UK; 7London School of Hygiene and Tropical Medicine, London, UKCorrespondence: Cristina Suárez, Barts Health NHS Trust, Royal London Hospital, Department of Infection, Pharmacy & Pathology Building – 3rd floor, 80 Newark Street, London, E1 2ES, UK, Tel +44 20 3246 0302, Email cristina.suarez@nhs.netAbstract: Chagas disease (CD) is caused by the parasite Trypanosoma cruzi, and it is endemic in Central, South America, Mexico and the South of the United States. It is an important cause of early mortality and morbidity, and it is associated with poverty and stigma. A third of the cases evolve into chronic cardiomyopathy and gastrointestinal disease. The infection is transmitted vertically and by blood/organ donation and can reactivate with immunosuppression. Case identification requires awareness and screening programmes targeting the population at risk (women in reproductive age, donors, immunocompromised patients). Treatment with benznidazole or nifurtimox is most effective in the acute phase and prevents progression to chronic phase when given to children. Treating women antenatally reduces but does not eliminate vertical transmission. Treatment is poorly tolerated, contraindicated during pregnancy, and has little effect modifying the disease in the chronic phase. Screening is easily performed with serology. Migration has brought the disease outside of the endemic countries, where the transmission continues vertically and via blood and tissue/organ donations. There are more than 32 million migrants from Latin America living in non-endemic countries. However, the infection is massively underdiagnosed in this setting due to the lack of awareness by patients, health authorities and professionals. Blood and tissue donation screening policies have significantly reduced transmission in endemic countries but are not universally established in the non-endemic setting. Antenatal screening is not commonly done. Other challenges include difficulties accessing and retaining patients in the healthcare system and lack of specific funding for the interventions. Any strategy must be accompanied by education and awareness campaigns directed to patients, professionals and policy makers. The involvement of patients and their communities is central and key for success and must be sought early and actively. This review proposes strategies to address challenges faced by non-endemic countries.Keywords: Trypanosoma cruzi, antenatal, transplant, migrant, screening, prevention

Published

2022

2. Rapid profiling of Plasmodium parasites from genome sequences to assist malaria control.

Author

Phelan, J.E., Turkiewicz, A., Manko, E., Thorpe, J., Vanheer, L.N., Vegte-Bolmer, M. van de, Ngoc, N.T.H., Binh, N.T.H., Thieu, N.Q., Gitaka, J., Nolder, D., Beshir, K.B., Dombrowski, J.G., Santi, S.M. Di, Bousema, T., Sutherland, C.J., Campino, S., Clark, T.G., Phelan, J.E., Turkiewicz, A., Manko, E., Thorpe, J., Vanheer, L.N., Vegte-Bolmer, M. van de, Ngoc, N.T.H., Binh, N.T.H., Thieu, N.Q., Gitaka, J., Nolder, D., Beshir, K.B., Dombrowski, J.G., Santi, S.M. Di, Bousema, T., Sutherland, C.J., Campino, S., and Clark, T.G.

Abstract

Item does not contain fulltext, BACKGROUND: Malaria continues to be a major threat to global public health. Whole genome sequencing (WGS) of the underlying Plasmodium parasites has provided insights into the genomic epidemiology of malaria. Genome sequencing is rapidly gaining traction as a diagnostic and surveillance tool for clinical settings, where the profiling of co-infections, identification of imported malaria parasites, and detection of drug resistance are crucial for infection control and disease elimination. To support this informatically, we have developed the Malaria-Profiler tool, which rapidly (within minutes) predicts Plasmodium species, geographical source, and resistance to antimalarial drugs directly from WGS data. RESULTS: The online and command line versions of Malaria-Profiler detect ~ 250 markers from genome sequences covering Plasmodium speciation, likely geographical source, and resistance to chloroquine, sulfadoxine-pyrimethamine (SP), and other anti-malarial drugs for P. falciparum, but also providing mutations for orthologous resistance genes in other species. The predictive performance of the mutation library was assessed using 9321 clinical isolates with WGS and geographical data, with most being single-species infections (P. falciparum 7152/7462, P. vivax 1502/1661, P. knowlesi 143/151, P. malariae 18/18, P. ovale ssp. 5/5), but co-infections were identified (456/9321; 4.8%). The accuracy of the predicted geographical profiles was high to both continental (96.1%) and regional levels (94.6%). For P. falciparum, markers were identified for resistance to chloroquine (49.2%; regional range: 24.5% to 100%), sulfadoxine (83.3%; 35.4- 90.5%), pyrimethamine (85.4%; 80.0-100%) and combined SP (77.4%). Markers associated with the partial resistance of artemisinin were found in WGS from isolates sourced from Southeast Asia (30.6%). CONCLUSIONS: Malaria-Profiler is a user-friendly tool that can rapidly and accurately predict the geographical regional source and anti-malarial drug

Published

2023

3. Population-based genomic study of Plasmodium vivax malaria in seven Brazilian states and across South America

Author

Ibrahim, A, Manko, E, Dombrowski, JG, Campos, M, Benavente, ED, Nolder, D, Sutherland, CJ, Nosten, F, Fernandez, D, Vélez-Tobón, G, Castaño, AT, Aguiar, ACC, Pereira, DB, da Silva Santos, S, Suarez-Mutis, M, Di Santi, SM, Regina de Souza Baptista, A, Dantas Machado, RL, Marinho, CRF, Clark, TG, and Campino, S

Subjects

Health Policy, Public Health, Environmental and Occupational Health, Internal Medicine, GENÉTICA DE POPULAÇÕES

Abstract

Background Brazil is a unique and understudied setting for malaria, with complex foci of transmission associated with human and environmental conditions. An understanding of the population genomic diversity of P. vivax parasites across Brazil can support malaria control strategies. Methods Through whole genome sequencing of P. vivax isolates across 7 Brazilian states, we use population genomic approaches to compare genetic diversity within country (n = 123), continent (6 countries, n = 315) and globally (26 countries, n = 885). Findings We confirm that South American isolates are distinct, have more ancestral populations than the other global regions, with differentiating mutations in genes under selective pressure linked to antimalarial drugs (pvmdr1, pvdhfr-ts) and mosquito vectors (pvcrmp3, pvP45/48, pvP47). We demonstrate Brazil as a distinct parasite population, with signals of selection including ABC transporter (PvABCI3) and PHIST exported proteins. Interpretation Brazil has a complex population structure, with evidence of P. simium infections and Amazonian parasites separating into multiple clusters. Overall, our work provides the first Brazil-wide analysis of P. vivax population structure and identifies important mutations, which can inform future research and control measures.

Published

2023

4. Investigation of molecular diagnostic assays for the detection of Trypanosoma cruzi DNA in blood: O42

Author

Alvarez-Martinez, M. J., Nolder, D., and Chiodini, P.

Published

2010

5. Selective Whole-Genome Amplification Is a Robust Method That Enables Scalable Whole-Genome Sequencing of Plasmodium vivax from Unprocessed Clinical Samples.

Author

Miller, LH, Cowell, AN, Loy, DE, Sundararaman, SA, Valdivia, H, Fisch, K, Lescano, AG, Baldeviano, GC, Durand, S, Gerbasi, V, Sutherland, CJ, Nolder, D, Vinetz, JM, Hahn, BH, Winzeler, EA, Miller, LH, Cowell, AN, Loy, DE, Sundararaman, SA, Valdivia, H, Fisch, K, Lescano, AG, Baldeviano, GC, Durand, S, Gerbasi, V, Sutherland, CJ, Nolder, D, Vinetz, JM, Hahn, BH, and Winzeler, EA

Abstract

UNLABELLED: Whole-genome sequencing (WGS) of microbial pathogens from clinical samples is a highly sensitive tool used to gain a deeper understanding of the biology, epidemiology, and drug resistance mechanisms of many infections. However, WGS of organisms which exhibit low densities in their hosts is challenging due to high levels of host genomic DNA (gDNA), which leads to very low coverage of the microbial genome. WGS of Plasmodium vivax, the most widely distributed form of malaria, is especially difficult because of low parasite densities and the lack of an ex vivo culture system. Current techniques used to enrich P. vivax DNA from clinical samples require significant resources or are not consistently effective. Here, we demonstrate that selective whole-genome amplification (SWGA) can enrich P. vivax gDNA from unprocessed human blood samples and dried blood spots for high-quality WGS, allowing genetic characterization of isolates that would otherwise have been prohibitively expensive or impossible to sequence. We achieved an average genome coverage of 24×, with up to 95% of the P. vivax core genome covered by ≥5 reads. The single-nucleotide polymorphism (SNP) characteristics and drug resistance mutations seen were consistent with those of other P. vivax sequences from a similar region in Peru, demonstrating that SWGA produces high-quality sequences for downstream analysis. SWGA is a robust tool that will enable efficient, cost-effective WGS of P. vivax isolates from clinical samples that can be applied to other neglected microbial pathogens. IMPORTANCE: Malaria is a disease caused by Plasmodium parasites that caused 214 million symptomatic cases and 438,000 deaths in 2015. Plasmodium vivax is the most widely distributed species, causing the majority of malaria infections outside sub-Saharan Africa. Whole-genome sequencing (WGS) of Plasmodium parasites from clinical samples has revealed important insights into the epidemiology and mechanisms of drug resistance of

Published

2017

6. International study to evaluate PCR methods for detection of Trypanosoma cruzi DNA in blood samples from Chagas disease patients.

Author

Schijman,AG, Bisio,M, Orellana,L, Sued,M, Duffy,T, Mejia Jaramillo,AM, Cura,C, Auter,F, Veron,V, Qvarnstrom,Y, Deborggraeve,S, Hijar,G, Zulantay,I, Lucero,RH, Velazquez,E, Tellez,T, Sanchez Leon,Z, Galvão,L, Nolder,D, Monje Rumi,M, Levi,JE, Ramirez,JD, Zorrilla,P, Flores,M, Jercic,MI, Crisante,G, Añez,N, De Castro,AM, Gonzalez,CI, Acosta Viana,K, Yachelini,P, Torrico,F, Robello,C, Diosque,P, Triana Chavez,O, Aznar,C, Russomando,G, Büscher,P, Assal,A, Guhl,F, Sosa Estani,S, DaSilva,A, Britto,C, Luquetti,A, Ladzins,J, Schijman,AG, Bisio,M, Orellana,L, Sued,M, Duffy,T, Mejia Jaramillo,AM, Cura,C, Auter,F, Veron,V, Qvarnstrom,Y, Deborggraeve,S, Hijar,G, Zulantay,I, Lucero,RH, Velazquez,E, Tellez,T, Sanchez Leon,Z, Galvão,L, Nolder,D, Monje Rumi,M, Levi,JE, Ramirez,JD, Zorrilla,P, Flores,M, Jercic,MI, Crisante,G, Añez,N, De Castro,AM, Gonzalez,CI, Acosta Viana,K, Yachelini,P, Torrico,F, Robello,C, Diosque,P, Triana Chavez,O, Aznar,C, Russomando,G, Büscher,P, Assal,A, Guhl,F, Sosa Estani,S, DaSilva,A, Britto,C, Luquetti,A, and Ladzins,J

Abstract

A century after its discovery, Chagas disease still represents a major neglected tropical threat. Accurate diagnostics tools as well as surrogate markers of parasitological response to treatment are research priorities in the field. The purpose of this study was to evaluate the performance of PCR methods in detection of Trypanosoma cruzi DNA by an external quality evaluation.

Published

2011

7. Recrudescence of imported falciparum malaria after quinine therapy: potential drug interaction with phenytoin

Author

Fabre, C., primary, Criddle, J., additional, Nolder, D., additional, and Klein, J.L., additional

Published

2005

8. Molecular diversity in the Leishmania subgenus Viannia

Author

Nolder, D and Miles, M

Abstract

The aim of this work was to provide further insight into the relationships between species of the Leishmania subgenus Viannia by examining inter- and intra-specific genetic diversity.\ud Diversity among Viannia strains and stocks was investigated using biochemical and molecular techniques. Isoenzyme and microsatellite analyses were found to be the most discriminatory and generated results which could be interpreted genotypically. These techniques were used to study diversity in Viannia populations consisting of i) Brazilian L V. braziliensis stocks, ii) Nicaraguan stocks belonging to different Viannia species complexes, including putative species-complex hybrids, and iii) uncharacterized stocks from a new epidemic focus in Huanuco, Peru.\ud LEA identified all stocks to at least the species level. Microsatellite analyses using Genescan® / Genotyper® and direct sequencing were found to be more discriminatory than EEA for all populations. The application of Genescan® / Genotyper® to the identification of alleles at these microsatellite loci has not been described previously. Phylogenetic analysis was carried out for each population using enzyme and microsatellite sequence data: phylogenies constructed from multilocus enzyme data were most accurate.\ud Putative species heterozygotes between/,. V. braziliensis/L. V. panamensis and/,. V. braziliensis / L. V. peruviana were identified in the Nicaraguan and Huanuco populations, respectively, using IEA. Microsatellite analysis identified heterozygous stocks in all 3 populations. This approach also supported the hybrid status of the Nicaraguan and Huanuco stocks. Population genetic analysis of stocks from Huanuco provided statistical evidence for a limited degree of genetic recombination between stocks in this population. Results indicated, however, that clonal expansion was the predominant mode of replication. To explore the possibility of the occurrence of genetic recombination between species, genetic transformation experiments were initiated using putative parental stocks from the Nicaraguan population

9. A Pan Plasmodium lateral flow recombinase polymerase amplification assay for monitoring malaria parasites in vectors and human populations.

Author

Higgins M, Kristan M, Collins EL, Messenger LA, Dombrowski JG, Vanheer LN, Nolder D, Drakeley CJ, Stone W, Mahamar A, Bousema T, Delves M, Bandibabone J, N'Do S, Bantuzeko C, Zawadi B, Walker T, Sutherland CJ, Marinho CRF, Cameron MM, Clark TG, and Campino S

Subjects

Humans, Animals, Recombinases metabolism, Recombinases genetics, Plasmodium falciparum genetics, Plasmodium falciparum isolation & purification, Anopheles parasitology, Plasmodium genetics, Plasmodium isolation & purification, Nucleic Acid Amplification Techniques methods, Malaria diagnosis, Malaria parasitology, Mosquito Vectors parasitology

Abstract

Robust diagnostic tools and surveillance are crucial for malaria control and elimination efforts. Malaria caused by neglected Plasmodium parasites is often underestimated due to the lack of rapid diagnostic tools that can accurately detect these species. While nucleic-acid amplification technologies stand out as the most sensitive methods for detecting and confirming Plasmodium species, their implementation in resource-constrained settings poses significant challenges. Here, we present a Pan Plasmodium recombinase polymerase amplification lateral flow (RPA-LF) assay, capable of detecting all six human infecting Plasmodium species in low resource settings. The Pan Plasmodium RPA-LF assay successfully detected low density clinical infections with a preliminary limit of detection between 10-100 fg/µl for P. falciparum. When combined with crude nucleic acid extraction, the assay can serve as a point-of-need tool for molecular xenomonitoring. This utility was demonstrated by screening laboratory-reared Anopheles stephensi mosquitoes fed with Plasmodium-infected blood, as well as field samples of An. funestus s.l. and An. gambiae s.l. collected from central Africa. Overall, our proof-of-concept Pan Plasmodium diagnostic tool has the potential to be applied for clinical and xenomonitoring field surveillance, and after further evaluation, could become an essential tool to assist malaria control and elimination., (© 2024. The Author(s).)

Published

2024

10. Treatment Failure in a UK Malaria Patient Harboring Genetically Variant Plasmodium falciparum From Uganda With Reduced In Vitro Susceptibility to Artemisinin and Lumefantrine.

Author

van Schalkwyk DA, Pratt S, Nolder D, Stewart LB, Liddy H, Muwanguzi-Karugaba J, Beshir KB, Britten D, Victory E, Rogers C, Millard J, Brown M, Nabarro LE, Taylor A, Young BC, Chiodini PL, and Sutherland CJ

Subjects

Humans, Lumefantrine pharmacology, Lumefantrine therapeutic use, Plasmodium falciparum, Artemether, Lumefantrine Drug Combination pharmacology, Artemether, Lumefantrine Drug Combination therapeutic use, Uganda, Drug Resistance, Artemether pharmacology, Artemether therapeutic use, Treatment Failure, United Kingdom, Protozoan Proteins genetics, Antimalarials pharmacology, Antimalarials therapeutic use, Artemisinins pharmacology, Artemisinins therapeutic use, Malaria drug therapy, Malaria, Falciparum drug therapy, Malaria, Falciparum parasitology

Abstract

Background: Recent cases of clinical failure in malaria patients in the United Kingdom (UK) treated with artemether-lumefantrine have implications for malaria chemotherapy worldwide., Methods: Parasites were isolated from an index case of confirmed Plasmodium falciparum treatment failure after standard treatment, and from comparable travel-acquired UK malaria cases. Drug susceptibility in vitro and genotypes at 6 resistance-associated loci were determined for all parasite isolates and compared with clinical outcomes for each parasite donor., Results: A traveler, who returned to the UK from Uganda in 2022 with Plasmodium falciparum malaria, twice failed treatment with full courses of artemether-lumefantrine. Parasites from the patient exhibited significantly reduced susceptibility to artemisinin (ring-stage survival, 17.3% [95% confidence interval {CI}, 13.6%-21.1%]; P < .0001) and lumefantrine (effective concentration preventing 50% of growth = 259.4 nM [95% CI, 130.6-388.2 nM]; P = .001). Parasite genotyping identified an allele of pfk13 encoding both the A675V variant in the Pfk13 propeller domain and a novel L145V nonpropeller variant. In vitro susceptibility testing of 6 other P. falciparum lines of Ugandan origin identified reduced susceptibility to artemisinin and lumefantrine in 1 additional line, also from a 2022 treatment failure case. These parasites did not harbor a pfk13 propeller domain variant but rather the novel nonpropeller variant T349I. Variant alleles of pfubp1, pfap2mu, and pfcoronin were also identified among the 7 parasite lines., Conclusions: We confirm, in a documented case of artemether-lumefantrine treatment failure imported from Uganda, the presence of pfk13 mutations encoding L145V and A675V. Parasites with reduced susceptibility to both artemisinin and lumefantrine may be emerging in Uganda., Competing Interests: Potential conflicts of interest. B. C. Y. reports a clinical lecturer starter grant paid via institution from Academy of Medical Sciences and funding to institution from the Oxford University National Institute for Health and Care Research Biomedical Research Centre grant. P. L. C. reports grants or contracts from the World Health Organization for the Molecular External Quality Assessment Scheme. J. M. reports grant to institution 203919/Z/16/Z from Wellcome Trust Clinical PhD and grant to institution from UCL Global Challenges, and participation as chair of a data and safety monitoring board for Triage Test for All Oral DR-TB Regimen (TRiAD Study). L. E. N. reports royalties or licenses paid to author from Peter’s Atlas of Tropical Medicine and Parasitology (Elsevier, author). All other authors report no potential conflicts. All authors have submitted the ICMJE Form for Disclosure of Potential Conflicts of Interest. Conflicts that the editors consider relevant to the content of the manuscript have been disclosed., (© The Author(s) 2023. Published by Oxford University Press on behalf of Infectious Diseases Society of America.)

Published

2024

11. New reference genomes to distinguish the sympatric malaria parasites, Plasmodium ovale curtisi and Plasmodium ovale wallikeri.

Author

Higgins M, Manko E, Ward D, Phelan JE, Nolder D, Sutherland CJ, Clark TG, and Campino S

Subjects

Animals, Humans, Sequence Analysis, DNA, Nigeria, Plasmodium ovale, Parasites genetics, Malaria parasitology

Abstract

Despite Plasmodium ovale curtisi (Poc) and wallikeri (Pow) being important human-infecting malaria parasites that are widespread across Africa and Asia, little is known about their genome diversity. Morphologically identical, Poc and Pow are indistinguishable and commonly misidentified. Recent rises in the incidence of Poc/Pow infections have renewed efforts to address fundamental knowledge gaps in their biology, and to develop diagnostic tools to understand their epidemiological dynamics and malaria burden. A major roadblock has been the incompleteness of available reference assemblies (PocGH01, PowCR01; ~ 33.5 Mbp). Here, we applied multiple sequencing platforms and advanced bioinformatics tools to generate new reference genomes, Poc221 (South Sudan; 36.0 Mbp) and Pow222 (Nigeria; 34.3 Mbp), with improved nuclear genome contiguity (> 4.2 Mbp), annotation and completeness (> 99% Plasmodium spp., single copy orthologs). Subsequent sequencing of 6 Poc and 15 Pow isolates from Africa revealed a total of 22,517 and 43,855 high-quality core genome SNPs, respectively. Genome-wide levels of nucleotide diversity were determined to be 2.98 × 10 -4 (Poc) and 3.43 × 10 -4 (Pow), comparable to estimates for other Plasmodium species. Overall, the new reference genomes provide a robust foundation for dissecting the biology of Poc/Pow, their population structure and evolution, and will contribute to uncovering the recombination barrier separating these species., (© 2024. The Author(s).)

Published

2024

12. Rapid profiling of Plasmodium parasites from genome sequences to assist malaria control.

Author

Phelan JE, Turkiewicz A, Manko E, Thorpe J, Vanheer LN, van de Vegte-Bolmer M, Ngoc NTH, Binh NTH, Thieu NQ, Gitaka J, Nolder D, Beshir KB, Dombrowski JG, Di Santi SM, Bousema T, Sutherland CJ, Campino S, and Clark TG

Subjects

Humans, Animals, Chloroquine therapeutic use, Drug Resistance genetics, Plasmodium falciparum genetics, Antimalarials pharmacology, Antimalarials therapeutic use, Parasites, Coinfection drug therapy, Malaria drug therapy, Malaria parasitology, Plasmodium genetics, Malaria, Falciparum drug therapy, Malaria, Vivax

Abstract

Background: Malaria continues to be a major threat to global public health. Whole genome sequencing (WGS) of the underlying Plasmodium parasites has provided insights into the genomic epidemiology of malaria. Genome sequencing is rapidly gaining traction as a diagnostic and surveillance tool for clinical settings, where the profiling of co-infections, identification of imported malaria parasites, and detection of drug resistance are crucial for infection control and disease elimination. To support this informatically, we have developed the Malaria-Profiler tool, which rapidly (within minutes) predicts Plasmodium species, geographical source, and resistance to antimalarial drugs directly from WGS data., Results: The online and command line versions of Malaria-Profiler detect ~ 250 markers from genome sequences covering Plasmodium speciation, likely geographical source, and resistance to chloroquine, sulfadoxine-pyrimethamine (SP), and other anti-malarial drugs for P. falciparum, but also providing mutations for orthologous resistance genes in other species. The predictive performance of the mutation library was assessed using 9321 clinical isolates with WGS and geographical data, with most being single-species infections (P. falciparum 7152/7462, P. vivax 1502/1661, P. knowlesi 143/151, P. malariae 18/18, P. ovale ssp. 5/5), but co-infections were identified (456/9321; 4.8%). The accuracy of the predicted geographical profiles was high to both continental (96.1%) and regional levels (94.6%). For P. falciparum, markers were identified for resistance to chloroquine (49.2%; regional range: 24.5% to 100%), sulfadoxine (83.3%; 35.4- 90.5%), pyrimethamine (85.4%; 80.0-100%) and combined SP (77.4%). Markers associated with the partial resistance of artemisinin were found in WGS from isolates sourced from Southeast Asia (30.6%)., Conclusions: Malaria-Profiler is a user-friendly tool that can rapidly and accurately predict the geographical regional source and anti-malarial drug resistance profiles across large numbers of samples with WGS data. The software is flexible with modifiable bioinformatic pipelines. For example, it is possible to select the sequencing platform, display specific variants, and customise the format of outputs. With the increasing application of next-generation sequencing platforms on Plasmodium DNA, Malaria-Profiler has the potential to be integrated into point-of-care and surveillance settings, thereby assisting malaria control. Malaria-Profiler is available online (bioinformatics.lshtm.ac.uk/malaria-profiler) and as standalone software ( https://github.com/jodyphelan/malaria-profiler )., (© 2023. The Author(s).)

Published

2023

13. Population genetic analysis of Plasmodium knowlesi reveals differential selection and exchange events between Borneo and Peninsular sub-populations.

Author

Turkiewicz A, Manko E, Oresegun DR, Nolder D, Spadar A, Sutherland CJ, Cox-Singh J, Moon RW, Lau YL, Campino S, and Clark TG

Subjects

Animals, Humans, Genetic Variation, Macaca fascicularis parasitology, Malaysia epidemiology, Genetics, Population, Selection, Genetic, Plasmodium knowlesi genetics, Malaria parasitology, Malaria, Vivax, Malaria, Falciparum

Abstract

The zoonotic Plasmodium knowlesi parasite is a growing public health concern in Southeast Asia, especially in Malaysia, where elimination of P. falciparum and P. vivax malaria has been the focus of control efforts. Understanding of the genetic diversity of P. knowlesi parasites can provide insights into its evolution, population structure, diagnostics, transmission dynamics, and the emergence of drug resistance. Previous work has revealed that P. knowlesi fall into three main sub-populations distinguished by a combination of geographical location and macaque host (Macaca fascicularis and M. nemestrina). It has been shown that Malaysian Borneo groups display profound heterogeneity with long regions of high or low divergence resulting in mosaic patterns between sub-populations, with some evidence of chromosomal-segment exchanges. However, the genetic structure of non-Borneo sub-populations is less clear. By gathering one of the largest collections of P. knowlesi whole-genome sequencing data, we studied structural genomic changes across sub-populations, with the analysis revealing differences in Borneo clusters linked to mosquito-related stages of the parasite cycle, in contrast to differences in host-related stages for the Peninsular group. Our work identifies new genetic exchange events, including introgressions between Malaysian Peninsular and M. nemestrina-associated clusters on various chromosomes, including in parasite invasion genes (DBP[Formula: see text], NBPX[Formula: see text] and NBPX[Formula: see text]), and important proteins expressed in the vertebrate parasite stages. Recombination events appear to have occurred between the Peninsular and M. fascicularis-associated groups, including in the DBP[Formula: see text] and DBP[Formula: see text] invasion associated genes. Overall, our work finds that genetic exchange events have occurred among the recognised contemporary groups of P. knowlesi parasites during their evolutionary history, leading to apparent mosaicism between these sub-populations. These findings generate new hypotheses relevant to parasite evolutionary biology and P. knowlesi epidemiology, which can inform malaria control approaches to containing the impact of zoonotic malaria on human communities., (© 2023. The Author(s).)

Published

2023

14. Population-based genomic study of Plasmodium vivax malaria in seven Brazilian states and across South America.

Author

Ibrahim A, Manko E, Dombrowski JG, Campos M, Benavente ED, Nolder D, Sutherland CJ, Nosten F, Fernandez D, Vélez-Tobón G, Castaño AT, Aguiar ACC, Pereira DB, da Silva Santos S, Suarez-Mutis M, Di Santi SM, Regina de Souza Baptista A, Dantas Machado RL, Marinho CRF, Clark TG, and Campino S

Abstract

Background: Brazil is a unique and understudied setting for malaria, with complex foci of transmission associated with human and environmental conditions. An understanding of the population genomic diversity of P. vivax parasites across Brazil can support malaria control strategies., Methods: Through whole genome sequencing of P. vivax isolates across 7 Brazilian states, we use population genomic approaches to compare genetic diversity within country (n = 123), continent (6 countries, n = 315) and globally (26 countries, n = 885)., Findings: We confirm that South American isolates are distinct, have more ancestral populations than the other global regions, with differentiating mutations in genes under selective pressure linked to antimalarial drugs ( pvmdr1 , pvdhfr-ts ) and mosquito vectors ( pvcrmp3, pvP45/48, pvP47 ). We demonstrate Brazil as a distinct parasite population, with signals of selection including ABC transporter ( PvABCI3 ) and PHIST exported proteins., Interpretation: Brazil has a complex population structure, with evidence of P. simium infections and Amazonian parasites separating into multiple clusters. Overall, our work provides the first Brazil-wide analysis of P. vivax population structure and identifies important mutations, which can inform future research and control measures., Funding: AI is funded by an MRC LiD PhD studentship. TGC is funded by the Medical Research Council (Grant no. MR/M01360X/1, MR/N010469/1, MR/R025576/1, MR/R020973/1 and MR/X005895/1). SC is funded by Medical Research Council UK grants (MR/M01360X/1, MR/R025576/1, MR/R020973/1 and MR/X005895/1) and Bloomsbury SET (ref. CCF17-7779). FN is funded by The Shloklo Malaria Research Unit - part of the Mahidol Oxford Research Unit, supported by the Wellcome Trust (Grant no. 220211). ARSB is funded by São Paulo Research Foundation - FAPESP (Grant no. 2002/09546-1). RLDM is funded by Brazilian National Council for Scientific and Technological Development - CNPq (Grant no. 302353/2003-8 and 471605/2011-5); CRFM is funded by FAPESP (Grant no. 2020/06747-4) and CNPq (Grant no. 302917/2019-5 and 408636/2018-1); JGD is funded by FAPESP fellowships (2016/13465-0 and 2019/12068-5) and CNPq (Grant no. 409216/2018-6)., Competing Interests: The authors have declared that no competing interests exist., (© 2022 The Author(s).)

Published

2023

15. Emergence of Congenital Chagas Disease in Ireland.

Author

Stone RG, Gavin P, Chiodini P, Nolder D, McGettrick P, Keogh A, Mc Entagart N, Drew R, Lambert J, and Ferguson W

Subjects

Female, Humans, Infant, Ireland epidemiology, Chagas Disease congenital, Chagas Disease epidemiology

Abstract

Chagas disease (CD) is an under-diagnosed tropical disease that is increasingly being observed outside of Latin America. We describe the first 2 infants with congenital Chagas Disease (cCD) in Ireland. Clinicians in nonendemic countries need to be aware of the potential for cCD due to the migration of women from countries of high prevalence., Competing Interests: The authors have no funding or conflicts of interest to disclose., (Copyright © 2022 Wolters Kluwer Health, Inc. All rights reserved.)

Published

2022

16. Vertical Transmission of Trypanosoma Cruzi in a Non-Endemic Country: Histology of the Infected Placenta.

Author

Keogh A, Ferguson W, Nolder D, Doyle E, and McEntagart N

Subjects

Female, Fetus, Humans, Infectious Disease Transmission, Vertical, Placenta, Pregnancy, Chagas Disease diagnosis, Trypanosoma cruzi

Abstract

Chagas disease, once confined to rural Latin America is an increasing public health concern in non-endemic countries due to population movements. Here we present an unexpected finding of a placenta infected with T. cruzi from a Brazilian woman residing in Ireland. Histology of the placenta showed a lymphocytic chorioamnionitis with multinucleated giant cells (MNGCs) as well as cord vasculitis and funisitis. Amastigotes of trypanosomiasis were found in both cord and membranes. The placenta parenchyma, however, had no villitis or amastigotes and maturation was appropriate for gestation. To date, there have been few reported cases of vertical transmission in non-endemic countries. We discuss the histological findings and review the literature on potential modes of transmission from mother to fetus.

Published

2021

17. Failure of rapid diagnostic tests in Plasmodium falciparum malaria cases among travelers to the UK and Ireland: Identification and characterisation of the parasites.

Author

Nolder D, Stewart L, Tucker J, Ibrahim A, Gray A, Corrah T, Gallagher C, John L, O'Brien E, Aggarwal D, Benavente ED, van Schalkwyk D, Henriques G, Sepúlveda N, Campino S, Chiodini P, Sutherland C, and Beshir KB

Subjects

Animals, Antigens, Protozoan genetics, Diagnostic Tests, Routine, Gene Deletion, Humans, Ireland epidemiology, Plasmodium falciparum genetics, Protozoan Proteins genetics, United Kingdom epidemiology, Malaria, Falciparum diagnosis, Malaria, Falciparum epidemiology, Parasites

Abstract

Objectives: Our objective was to systematically investigate false-negative histidine-rich protein 2 rapid diagnostic tests (HRP2-RDT) in imported Plasmodium falciparum malaria cases from travelers to the UK and the Republic of Ireland (RoI)., Methods: Five imported malaria cases in travellers returning to the UK and RoI from East Africa were reported to the PHE Malaria Reference Laboratory as negative according to histidine-rich protein (HRP2)-RDT. The cases were systematically investigated using microscopic, RDT, molecular, genomic, and in in vitro approaches., Results: In each case, HRP2-RDT was negative, whereas microscopy confirmed the presence of P. falciparum. Further analysis revealed that the genes encoding HRP2 and HRP3 were deleted in three of the five cases. Whole-genome sequencing in one of these isolates confirmed deletions in P. falciparum chromosomes 8 and 13. Our study produced evidence that the fourth case, which had high parasitemia at clinical presentation, was a rare example of antigen saturation ('prozone-like effect'), leading to a false negative in the HRP2-RDT, while the fifth case was due to low parasitemia., Conclusions: False-negative HRP2-RDT results with P. falciparum are concerning. Our findings emphasise the necessity of supporting the interpretation of RDT results with microscopy, in conjunction with clinical observations, and sets out a systematic approach to identifying parasites carrying pfhrp2 and pfhrp3 deletions., (Copyright © 2021 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published

2021

18. Distinctive genetic structure and selection patterns in Plasmodium vivax from South Asia and East Africa.

Author

Benavente ED, Manko E, Phelan J, Campos M, Nolder D, Fernandez D, Velez-Tobon G, Castaño AT, Dombrowski JG, Marinho CRF, Aguiar ACC, Pereira DB, Sriprawat K, Nosten F, Moon R, Sutherland CJ, Campino S, and Clark TG

Subjects

Africa, Eastern, Antimalarials pharmacology, Antimalarials therapeutic use, Asia, Drug Resistance genetics, Duffy Blood-Group System, Genetic Loci, Humans, Malaria, Vivax blood, Malaria, Vivax drug therapy, Phylogeny, Phylogeography, Plasmodium vivax drug effects, Plasmodium vivax pathogenicity, Polymorphism, Single Nucleotide, Protozoan Proteins genetics, Reticulocytes parasitology, Genes, Protozoan, Malaria, Vivax parasitology, Plasmodium vivax genetics, Selection, Genetic

Abstract

Despite the high burden of Plasmodium vivax malaria in South Asian countries, the genetic diversity of circulating parasite populations is not well described. Determinants of antimalarial drug susceptibility for P. vivax in the region have not been characterised. Our genomic analysis of global P. vivax (n = 558) establishes South Asian isolates (n = 92) as a distinct subpopulation, which shares ancestry with some East African and South East Asian parasites. Signals of positive selection are linked to drug resistance-associated loci including pvkelch10, pvmrp1, pvdhfr and pvdhps, and two loci linked to P. vivax invasion of reticulocytes, pvrbp1a and pvrbp1b. Significant identity-by-descent was found in extended chromosome regions common to P. vivax from India and Ethiopia, including the pvdbp gene associated with Duffy blood group binding. Our investigation provides new understanding of global P. vivax population structure and genomic diversity, and genetic evidence of recent directional selection in this important human pathogen.

Published

2021

19. Corrigendum to 'A novel multiplex qPCR assay for detection of Plasmodium falciparum with histidine-rich protein 2 and 3 (pfhrp2 and pfhrp3) deletions in polyclonal infections'.

Author

Grignard L, Nolder D, Sepulveda N, Berhane A, Mihreteab S, Kaaya R, Phelan J, Moser K, van Schalkwyk DA, Campino S, Parr JB, Juliano JJ, Chiodini P, Cunningham J, Sutherland CJ, Drakeley C, and Beshir KB

Published

2021

20. Selective whole genome amplification of Plasmodium malariae DNA from clinical samples reveals insights into population structure.

Author

Ibrahim A, Diez Benavente E, Nolder D, Proux S, Higgins M, Muwanguzi J, Gomez Gonzalez PJ, Fuehrer HP, Roper C, Nosten F, Sutherland C, Clark TG, and Campino S

Subjects

Animals, DNA, Protozoan isolation & purification, Drug Resistance genetics, Humans, Malaria parasitology, Malaria prevention & control, Polymorphism, Single Nucleotide, DNA, Protozoan genetics, Genetics, Population methods, Nucleic Acid Amplification Techniques methods, Plasmodium malariae genetics, Whole Genome Sequencing methods

Abstract

The genomic diversity of Plasmodium malariae malaria parasites is understudied, partly because infected individuals tend to present with low parasite densities, leading to difficulties in obtaining sufficient parasite DNA for genome analysis. Selective whole genome amplification (SWGA) increases the relative levels of pathogen DNA in a clinical sample, but has not been adapted for P. malariae parasites. Here we design customized SWGA primers which successfully amplify P. malariae DNA extracted directly from unprocessed clinical blood samples obtained from patients with P. malariae-mono-infections from six countries, and further test the efficacy of SWGA on mixed infections with other Plasmodium spp. SWGA enables the successful whole genome sequencing of samples with low parasite density (i.e. one sample with a parasitaemia of 0.0064% resulted in 44% of the genome covered by ≥ 5 reads), leading to an average 14-fold increase in genome coverage when compared to unamplified samples. We identify a total of 868,476 genome-wide SNPs, of which 194,709 are unique across 18 high-quality isolates. After exclusion of the hypervariable subtelomeric regions, a high-quality core subset of 29,899 unique SNPs is defined. Population genetic analysis suggests that P. malariae parasites display clear geographical separation by continent. Further, SWGA successfully amplifies genetic regions of interest such as orthologs of P. falciparum drug resistance-associated loci (Pfdhfr, Pfdhps, Pfcrt, Pfk13 and Pfmdr1), and several non-synonymous SNPs were detected in these genes. In conclusion, we have established a robust SWGA approach that can assist whole genome sequencing of P. malariae, and thereby facilitate the implementation of much-needed large-scale multi-population genomic studies of this neglected malaria parasite. As demonstrated in other Plasmodia, such genetic diversity studies can provide insights into the biology underlying the disease and inform malaria surveillance and control measures.

Published

2020

21. Chagas disease in the United Kingdom: A review of cases at the Hospital for Tropical Diseases London 1995-2018. The current state of detection of Chagas disease in the UK.

Author

González Sanz M, De Sario V, García-Mingo A, Nolder D, Dawood N, Álvarez-Martínez MJ, Daly R, Lowe P, Yacoub S, Moore DA, and Chiodini PL

Subjects

Bolivia, Female, Hospitals, Humans, Infant, Newborn, Latin America, London, Pregnancy, United Kingdom epidemiology, Chagas Disease

Abstract

Background: Chagas disease (CD), is a parasitic disease endemic in Latin America. Presentation in non-endemic areas is either in the asymptomatic indeterminate phase or the chronic phase with cardiac and/or gastrointestinal complications., Methods: The Hospital for Tropical Diseases (HTD) based in central London, provides tertiary care for the management of CD. We reviewed all cases managed at this centre between 1995 and 2018., Results: Sixty patients with serologically proven CD were identified. Most were female (70%), with a median age at diagnosis of 41 years. Three quarters of the patients were originally from Bolivia. 62% of all patients were referred to the HTD by their GP. Nearly half of the patients were asymptomatic (47%). Twelve patients had signs of cardiac involvement secondary to CD. Evidence of gastrointestinal damage was established in three patients. Treatment was provided at HTD for 31 patients (47%). Most patients (29) received benznidazole, five of them did not tolerate the course and were switched to nifurtimox. Of the seven patients receiving this second line drug, five completed treatment, whilst two interrupted it due to side effects., Conclusions: Despite the UK health system having all the resources required to diagnose, treat and follow up cases, there is lack of awareness of CD, such that the vast majority of cases remain undiagnosed and therefore do not receive treatment. We propose key interventions to improve the detection and management of this condition in the UK, especially in pregnant women and neonates., (Copyright © 2020 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2020

22. A novel multiplex qPCR assay for detection of Plasmodium falciparum with histidine-rich protein 2 and 3 (pfhrp2 and pfhrp3) deletions in polyclonal infections.

Author

Grignard L, Nolder D, Sepúlveda N, Berhane A, Mihreteab S, Kaaya R, Phelan J, Moser K, van Schalkwyk DA, Campino S, Parr JB, Juliano JJ, Chiodini P, Cunningham J, Sutherland CJ, Drakeley C, and Beshir KB

Subjects

Diagnostic Tests, Routine, Gene Expression, Humans, Kenya epidemiology, Malaria, Falciparum epidemiology, Malaria, Falciparum parasitology, Multiplex Polymerase Chain Reaction standards, Plasmodium falciparum pathogenicity, Tanzania epidemiology, Travel, United Kingdom epidemiology, Antigens, Protozoan genetics, DNA, Protozoan genetics, Gene Deletion, Malaria, Falciparum diagnosis, Multiplex Polymerase Chain Reaction methods, Plasmodium falciparum genetics, Protozoan Proteins genetics

Abstract

Background: Many health facilities in malaria endemic countries are dependent on Rapid diagnostic tests (RDTs) for diagnosis and some National Health Service (NHS) hospitals without expert microscopists rely on them for diagnosis out of hours. The emergence of P. falciparum lacking the gene encoding histidine-rich protein 2 and 3 (HRP2 and HRP3) and escaping RDT detection threatens progress in malaria control and elimination. Currently, confirmation of RDT negative due to the deletion of pfhrp2 and pfhrp3, which encodes a cross-reactive protein isoform, requires a series of PCR assays. These tests have different limits of detection and many laboratories have reported difficulty in confirming the absence of the deletions with certainty., Methods: We developed and validated a novel and rapid multiplex real time quantitative (qPCR) assay to detect pfhrp2, pfhrp3, confirmatory parasite and human reference genes simultaneously. We also applied the assay to detect pfhrp2 and pfhrp3 deletion in 462 field samples from different endemic countries and UK travellers., Results: The qPCR assay demonstrated diagnostic sensitivity of 100% (n = 19, 95% CI= (82.3%; 100%)) and diagnostic specificity of 100% (n = 31; 95% CI= (88.8%; 100%)) in detecting pfhrp2 and pfhrp3 deletions. In addition, the assay estimates P. falciparum parasite density and accurately detects pfhrp2 and pfhrp3 deletions masked in polyclonal infections. We report pfhrp2 and pfhrp3 deletions in parasite isolates from Kenya, Tanzania and in UK travellers., Interpretation: The new qPCR is easily scalable to routine surveillance studies in countries where P. falciparum parasites lacking pfhrp2 and pfhrp3 are a threat to malaria control., Competing Interests: Declaration of Competing Interest JBP reports non-financial support in the form of in-kind donation of laboratory testing and reagents from Abbott Laboratories for studies of viral hepatitis and financial support from the World Health Organization. Other authors declare no conflict of interest., (Copyright © 2020 The Author(s). Published by Elsevier B.V. All rights reserved.)

Published

2020

23. A molecular barcode to inform the geographical origin and transmission dynamics of Plasmodium vivax malaria.

Author

Diez Benavente E, Campos M, Phelan J, Nolder D, Dombrowski JG, Marinho CRF, Sriprawat K, Taylor AR, Watson J, Roper C, Nosten F, Sutherland CJ, Campino S, and Clark TG

Subjects

Africa, Eastern, Asia, Datasets as Topic, Disease Eradication methods, Genetic Markers genetics, Genotype, Geography, Humans, Malaria, Vivax epidemiology, Malaria, Vivax parasitology, Metadata, Microsatellite Repeats genetics, Plasmodium vivax isolation & purification, Polymorphism, Single Nucleotide genetics, Predictive Value of Tests, South America, Travel-Related Illness, United Kingdom, Whole Genome Sequencing, Disease Outbreaks prevention & control, Genome, Protozoan genetics, Genotyping Techniques methods, Malaria, Vivax transmission, Plasmodium vivax genetics

Abstract

Although Plasmodium vivax parasites are the predominant cause of malaria outside of sub-Saharan Africa, they not always prioritised by elimination programmes. P. vivax is resilient and poses challenges through its ability to re-emerge from dormancy in the human liver. With observed growing drug-resistance and the increasing reports of life-threatening infections, new tools to inform elimination efforts are needed. In order to halt transmission, we need to better understand the dynamics of transmission, the movement of parasites, and the reservoirs of infection in order to design targeted interventions. The use of molecular genetics and epidemiology for tracking and studying malaria parasite populations has been applied successfully in P. falciparum species and here we sought to develop a molecular genetic tool for P. vivax. By assembling the largest set of P. vivax whole genome sequences (n = 433) spanning 17 countries, and applying a machine learning approach, we created a 71 SNP barcode with high predictive ability to identify geographic origin (91.4%). Further, due to the inclusion of markers for within population variability, the barcode may also distinguish local transmission networks. By using P. vivax data from a low-transmission setting in Malaysia, we demonstrate the potential ability to infer outbreak events. By characterising the barcoding SNP genotypes in P. vivax DNA sourced from UK travellers (n = 132) to ten malaria endemic countries predominantly not used in the barcode construction, we correctly predicted the geographic region of infection origin. Overall, the 71 SNP barcode outperforms previously published genotyping methods and when rolled-out within new portable platforms, is likely to be an invaluable tool for informing targeted interventions towards elimination of this resilient human malaria., Competing Interests: The authors have declared that no competing interests exist.

Published

2020

24. Geographical and temporal trends and seasonal relapse in Plasmodium ovale spp. and Plasmodium malariae infections imported to the UK between 1987 and 2015.

Author

Nabarro LEB, Nolder D, Broderick C, Nadjm B, Smith V, Blaze M, Checkley AM, Chiodini PL, Sutherland CJ, and Whitty CJM

Subjects

Chronic Disease, Female, Humans, Male, Plasmodium malariae, Plasmodium ovale, Travel, United Kingdom epidemiology, Malaria epidemiology

Abstract

Background: Plasmodium ovale spp. and P. malariae cause illness in endemic regions and returning travellers. Far less is known about these species than P. falciparum and P. vivax., Methods: The UK national surveillance data, collected 1987 to 2015, were collated with the International Passenger Survey and climatic data to determine geographical, temporal and seasonal trends of imported P. ovale spp. and P. malariae infection., Results: Of 52,242 notified cases of malaria, 6.04% (3157) were caused by P. ovale spp. and 1.61% (841) by P. malariae; mortality was 0.03% (1) and 0.12% (1), respectively. Almost all travellers acquired infection in West or East Africa. Infection rate per travel episode fell fivefold during the study period. The median latency of P. malariae and P. ovale spp. was 18 and 76 days, respectively; delayed presentation occurred with both species. The latency of P. ovale spp. infection imported from West Africa was significantly shorter in those arriving in the UK during the West African peak malarial season compared to those arriving outside it (44 days vs 94 days, p < 0.0001), implying that relapse synchronises with the period of high malarial transmission. This trend was not seen in P. ovale spp. imported from East Africa nor in P. malariae., Conclusion: In West Africa, where malaria transmission is highly seasonal, P. ovale spp. may have evolved to relapse during the malarial high transmission season. This has public health implications. Deaths are very rare, supporting current guidelines emphasising outpatient treatment. However, late presentations do occur.

Published

2018

25. pfk13 -Independent Treatment Failure in Four Imported Cases of Plasmodium falciparum Malaria Treated with Artemether-Lumefantrine in the United Kingdom.

Author

Sutherland CJ, Lansdell P, Sanders M, Muwanguzi J, van Schalkwyk DA, Kaur H, Nolder D, Tucker J, Bennett HM, Otto TD, Berriman M, Patel TA, Lynn R, Gkrania-Klotsas E, and Chiodini PL

Subjects

Africa, Aged, Artemether, Lumefantrine Drug Combination, Drug Combinations, Female, Gene Expression, Genetic Loci, Humans, Malaria, Falciparum parasitology, Malaria, Falciparum pathology, Male, Parasitemia parasitology, Parasitemia pathology, Plasmodium falciparum genetics, Plasmodium falciparum growth & development, Recurrence, Travel, Treatment Failure, United Kingdom, Young Adult, Antimalarials therapeutic use, Artemisinins therapeutic use, Drug Resistance genetics, Ethanolamines therapeutic use, Fluorenes therapeutic use, Malaria, Falciparum drug therapy, Parasitemia drug therapy, Plasmodium falciparum drug effects, Protozoan Proteins genetics

Abstract

We present case histories of four patients treated with artemether-lumefantrine for falciparum malaria in UK hospitals in 2015 to 2016. Each subsequently presented with recurrent symptoms and Plasmodium falciparum parasitemia within 6 weeks of treatment with no intervening travel to countries where malaria is endemic. Parasite isolates, all of African origin, harbored variants at some candidate resistance loci. No evidence of pfk13 -mediated artemisinin resistance was found. Vigilance for signs of unsatisfactory antimalarial efficacy among imported cases of malaria is recommended., (Copyright © 2017 Sutherland et al.)

Published

2017

26. Selective Whole-Genome Amplification Is a Robust Method That Enables Scalable Whole-Genome Sequencing of Plasmodium vivax from Unprocessed Clinical Samples.

Author

Cowell AN, Loy DE, Sundararaman SA, Valdivia H, Fisch K, Lescano AG, Baldeviano GC, Durand S, Gerbasi V, Sutherland CJ, Nolder D, Vinetz JM, Hahn BH, and Winzeler EA

Subjects

Humans, Peru, Blood parasitology, Malaria, Vivax parasitology, Nucleic Acid Amplification Techniques methods, Plasmodium vivax genetics, Plasmodium vivax isolation & purification, Sequence Analysis, DNA methods

Abstract

Whole-genome sequencing (WGS) of microbial pathogens from clinical samples is a highly sensitive tool used to gain a deeper understanding of the biology, epidemiology, and drug resistance mechanisms of many infections. However, WGS of organisms which exhibit low densities in their hosts is challenging due to high levels of host genomic DNA (gDNA), which leads to very low coverage of the microbial genome. WGS of Plasmodium vivax, the most widely distributed form of malaria, is especially difficult because of low parasite densities and the lack of an ex vivo culture system. Current techniques used to enrich P. vivax DNA from clinical samples require significant resources or are not consistently effective. Here, we demonstrate that selective whole-genome amplification (SWGA) can enrich P. vivax gDNA from unprocessed human blood samples and dried blood spots for high-quality WGS, allowing genetic characterization of isolates that would otherwise have been prohibitively expensive or impossible to sequence. We achieved an average genome coverage of 24×, with up to 95% of the P. vivax core genome covered by ≥5 reads. The single-nucleotide polymorphism (SNP) characteristics and drug resistance mutations seen were consistent with those of other P. vivax sequences from a similar region in Peru, demonstrating that SWGA produces high-quality sequences for downstream analysis. SWGA is a robust tool that will enable efficient, cost-effective WGS of P. vivax isolates from clinical samples that can be applied to other neglected microbial pathogens., Importance: Malaria is a disease caused by Plasmodium parasites that caused 214 million symptomatic cases and 438,000 deaths in 2015. Plasmodium vivax is the most widely distributed species, causing the majority of malaria infections outside sub-Saharan Africa. Whole-genome sequencing (WGS) of Plasmodium parasites from clinical samples has revealed important insights into the epidemiology and mechanisms of drug resistance of malaria. However, WGS of P. vivax is challenging due to low parasite levels in humans and the lack of a routine system to culture the parasites. Selective whole-genome amplification (SWGA) preferentially amplifies the genomes of pathogens from mixtures of target and host gDNA. Here, we demonstrate that SWGA is a simple, robust method that can be used to enrich P. vivax genomic DNA (gDNA) from unprocessed human blood samples and dried blood spots for cost-effective, high-quality WGS., (Copyright © 2017 Cowell et al.)

Published

2017

27. Paper-Origami-Based Multiplexed Malaria Diagnostics from Whole Blood.

Author

Xu G, Nolder D, Reboud J, Oguike MC, van Schalkwyk DA, Sutherland CJ, and Cooper JM

Subjects

Humans, Malaria blood, Polymerase Chain Reaction, Sensitivity and Specificity, Malaria diagnosis, Nucleic Acid Amplification Techniques, Paper, Plasmodium isolation & purification

Abstract

We demonstrate, for the first time, the multiplexed determination of microbial species from whole blood using the paper-folding technique of origami to enable the sequential steps of DNA extraction, loop-mediated isothermal amplification (LAMP), and array-based fluorescence detection. A low-cost handheld flashlight reveals the presence of the final DNA amplicon to the naked eye, providing a "sample-to-answer" diagnosis from a finger-prick volume of human blood, within 45 min, with minimal user intervention. To demonstrate the method, we showed the identification of three species of Plasmodium, analyzing 80 patient samples benchmarked against the gold-standard polymerase chain reaction (PCR) assay in an operator-blinded study. We also show that the test retains its diagnostic accuracy when using stored or fixed reference samples., (© 2016 The Authors. Published by Wiley-VCH Verlag GmbH & Co. KGaA.)

Published

2016

28. Delayed Onset of Symptoms and Atovaquone-Proguanil Chemoprophylaxis Breakthrough by Plasmodium malariae in the Absence of Mutation at Codon 268 of pmcytb.

Author

Teo BH, Lansdell P, Smith V, Blaze M, Nolder D, Beshir KB, Chiodini PL, Cao J, Färnert A, and Sutherland CJ

Subjects

Codon, Drug Combinations, Plasmodium malariae genetics, Antimalarials pharmacology, Atovaquone pharmacology, Cytochromes b genetics, Mutation, Plasmodium malariae drug effects, Proguanil pharmacology

Abstract

Plasmodium malariae is widely distributed across the tropics, causing symptomatic malaria in humans with a 72-hour fever periodicity, and may present after latency periods lasting up to many decades. Delayed occurrence of symptoms is observed in humans using chemoprophylaxis, or patients having received therapies targeting P. falciparum intraerythrocytic asexual stages, but few investigators have addressed the biological basis of the ability of P. malariae to persist in the human host. To investigate these interesting features of P. malariae epidemiology, we assembled, here, an extensive case series of P. malariae malaria patients presenting in non-endemic China, Sweden, and the UK who returned from travel in endemic countries, mainly in Africa. Out of 378 evaluable P. malariae cases, 100 (26.2%) reported using at least partial chemoprophylaxis, resembling the pattern seen with the relapsing parasites P. ovale spp. and P. vivax. In contrast, for only 7.5% of imported UK cases of non-relapsing P. falciparum was any chemoprophylaxis use reported. Genotyping of parasites from six patients reporting use of atovaquone-proguanil chemoprophylaxis did not reveal mutations at codon 268 of the cytb locus of the P. malariae mitochondrial genome. While travellers with P. malariae malaria are significantly more likely to report prophylaxis use during endemic country travel than are those with P. falciparum infections, atovaquone-proguanil prophylaxis breakthrough was not associated with pmcytb mutations. These preliminary studies, together with consistent observations of the remarkable longevity of P. malariae, lead us to propose re-examination of the dogma that this species is not a relapsing parasite. Further studies are needed to investigate our favoured hypothesis, namely that P. malariae can initiate a latent hypnozoite developmental programme in the human hepatocyte: if validated this will explain the consistent observations of remarkable longevity of parasitism, even in the presence of antimalarial prophylaxis or treatment.

Published

2015

29. African origin of the malaria parasite Plasmodium vivax.

Author

Liu W, Li Y, Shaw KS, Learn GH, Plenderleith LJ, Malenke JA, Sundararaman SA, Ramirez MA, Crystal PA, Smith AG, Bibollet-Ruche F, Ayouba A, Locatelli S, Esteban A, Mouacha F, Guichet E, Butel C, Ahuka-Mundeke S, Inogwabini BI, Ndjango JB, Speede S, Sanz CM, Morgan DB, Gonder MK, Kranzusch PJ, Walsh PD, Georgiev AV, Muller MN, Piel AK, Stewart FA, Wilson ML, Pusey AE, Cui L, Wang Z, Färnert A, Sutherland CJ, Nolder D, Hart JA, Hart TB, Bertolani P, Gillis A, LeBreton M, Tafon B, Kiyang J, Djoko CF, Schneider BS, Wolfe ND, Mpoudi-Ngole E, Delaporte E, Carter R, Culleton RL, Shaw GM, Rayner JC, Peeters M, Hahn BH, and Sharp PM

Subjects

Africa, Animals, Asia, Evolution, Molecular, Phylogeny, Plasmodium vivax pathogenicity, Malaria physiopathology, Plasmodium vivax classification, Plasmodium vivax genetics

Abstract

Plasmodium vivax is the leading cause of human malaria in Asia and Latin America but is absent from most of central Africa due to the near fixation of a mutation that inhibits the expression of its receptor, the Duffy antigen, on human erythrocytes. The emergence of this protective allele is not understood because P. vivax is believed to have originated in Asia. Here we show, using a non-invasive approach, that wild chimpanzees and gorillas throughout central Africa are endemically infected with parasites that are closely related to human P. vivax. Sequence analyses reveal that ape parasites lack host specificity and are much more diverse than human parasites, which form a monophyletic lineage within the ape parasite radiation. These findings indicate that human P. vivax is of African origin and likely selected for the Duffy-negative mutation. All extant human P. vivax parasites are derived from a single ancestor that escaped out of Africa.

Published

2014

30. An observational study of malaria in British travellers: Plasmodium ovale wallikeri and Plasmodium ovale curtisi differ significantly in the duration of latency.

Author

Nolder D, Oguike MC, Maxwell-Scott H, Niyazi HA, Smith V, Chiodini PL, and Sutherland CJ

Abstract

Objectives: Ovale malaria is caused by two closely related species of protozoan parasite: Plasmodium ovale curtisi and Plasmodium ovale wallikeri Although clearly distinct genetically, there have been no studies comparing the morphology, life cycle or epidemiology of these parasites. We tested the hypothesis that the two species differ in the duration of latency prior to presentation with symptoms of blood-stage infection., Design: PCR was used to identify P ovale curtisi and P ovale wallikeri infections among archived blood from UK malaria patients. Latency periods, estimated as the time between entry into the UK and diagnosis of malaria, were compared between the two groups., Setting: UK National Reference Laboratory., Participants: None. Archived parasite material and surveillance data for 74 P ovale curtisi and 60 P ovale wallikeri infections were analysed. Additional epidemiological data were taken from a database of 1045 imported cases., Outcomes: None., Results: No differences between the two species were identified by a detailed comparison of parasite morphology (N=9, N=8, respectively) and sex ratio (N=5, N=4) in archived blood films. The geometric mean latency period in P ovale wallikeri was 40.6 days (95% CI 28.9 to 57.0), whereas that for P ovale curtisi was more than twice as long at 85.7 days (95% CI 66.1 to 111.1; p=0.002). Further, the proportion of ovale malaria sensu lato which occurred in patients reporting chemoprophylaxis use was higher than for Plasmodium falciparum (OR 7.56; p<0.0001) or P vivax (OR 1.82; p<0.0001)., Conclusions: These findings provide the first difference of epidemiological significance observed between the two parasites which cause ovale malaria, and suggest that control measures aimed at P falciparum may not be adequate for reducing the burden of malaria caused by P ovale curtisi and P ovale wallikeri.

Published

2013

31. Plasmodium ovale curtisi and Plasmodium ovale wallikeri circulate simultaneously in African communities.

Author

Oguike MC, Betson M, Burke M, Nolder D, Stothard JR, Kleinschmidt I, Proietti C, Bousema T, Ndounga M, Tanabe K, Ntege E, Culleton R, and Sutherland CJ

Subjects

Animals, Congo epidemiology, DNA, Protozoan chemistry, DNA, Protozoan genetics, Guinea epidemiology, Humans, Molecular Sequence Data, Plasmodium ovale isolation & purification, Protozoan Proteins genetics, Sequence Analysis, DNA, Uganda epidemiology, Malaria epidemiology, Malaria parasitology, Phylogeography, Plasmodium ovale classification, Plasmodium ovale genetics

Abstract

It has been proposed that ovale malaria in humans is caused by two closely related but distinct species of malaria parasite, Plasmodium ovale curtisi and Plasmodium ovale wallikeri. It was recently shown that these two parasite types are sympatric at the country level. However, it remains possible that localised geographic, temporal or ecological barriers exist within endemic countries which prevent recombination between the genomes of the two species. Here, using conventional and real-time quantitative PCR (qPCR) methods specifically designed to discriminate P. o. curtisi and P. o. wallikeri, it is shown that both species are present among clinic attendees in Congo-Brazzaville, and occur simultaneously both in lake-side and inland districts in Uganda and on Bioko Island, Equatorial Guinea. Thus P. o. curtisi and P. o. wallikeri in these localities are exactly sympatric in both time and space. These findings are consistent with the existence of a biological barrier, rather than geographical or ecological factors, preventing recombination between P. o. curtisi and P. o. wallikeri. In cross-sectional surveys carried out in Uganda and Bioko, our results show that infections with P. ovale spp. are more common than previously thought, occurring at a frequency of 1-6% in population samples, with both proposed species contributing to ovale malaria in six sites. Malaria elimination programmes in Africa need to include strategies for control of P. o. curtisi and P. o. wallikeri., (Copyright © 2011 Australian Society for Parasitology Inc. Published by Elsevier Ltd. All rights reserved.)

Published

2011

32. International study to evaluate PCR methods for detection of Trypanosoma cruzi DNA in blood samples from Chagas disease patients.

Author

Schijman AG, Bisio M, Orellana L, Sued M, Duffy T, Mejia Jaramillo AM, Cura C, Auter F, Veron V, Qvarnstrom Y, Deborggraeve S, Hijar G, Zulantay I, Lucero RH, Velazquez E, Tellez T, Sanchez Leon Z, Galvão L, Nolder D, Monje Rumi M, Levi JE, Ramirez JD, Zorrilla P, Flores M, Jercic MI, Crisante G, Añez N, De Castro AM, Gonzalez CI, Acosta Viana K, Yachelini P, Torrico F, Robello C, Diosque P, Triana Chavez O, Aznar C, Russomando G, Büscher P, Assal A, Guhl F, Sosa Estani S, DaSilva A, Britto C, Luquetti A, and Ladzins J

Subjects

Chagas Disease parasitology, Humans, International Cooperation, Sensitivity and Specificity, Trypanosoma cruzi genetics, Chagas Disease diagnosis, DNA, Protozoan blood, Parasitology methods, Polymerase Chain Reaction methods, Trypanosoma cruzi isolation & purification

Abstract

Background: A century after its discovery, Chagas disease still represents a major neglected tropical threat. Accurate diagnostics tools as well as surrogate markers of parasitological response to treatment are research priorities in the field. The purpose of this study was to evaluate the performance of PCR methods in detection of Trypanosoma cruzi DNA by an external quality evaluation., Methodology/findings: An international collaborative study was launched by expert PCR laboratories from 16 countries. Currently used strategies were challenged against serial dilutions of purified DNA from stocks representing T. cruzi discrete typing units (DTU) I, IV and VI (set A), human blood spiked with parasite cells (set B) and Guanidine Hidrochloride-EDTA blood samples from 32 seropositive and 10 seronegative patients from Southern Cone countries (set C). Forty eight PCR tests were reported for set A and 44 for sets B and C; 28 targeted minicircle DNA (kDNA), 13 satellite DNA (Sat-DNA) and the remainder low copy number sequences. In set A, commercial master mixes and Sat-DNA Real Time PCR showed better specificity, but kDNA-PCR was more sensitive to detect DTU I DNA. In set B, commercial DNA extraction kits presented better specificity than solvent extraction protocols. Sat-DNA PCR tests had higher specificity, with sensitivities of 0.05-0.5 parasites/mL whereas specific kDNA tests detected 5.10(-3) par/mL. Sixteen specific and coherent methods had a Good Performance in both sets A and B (10 fg/µl of DNA from all stocks, 5 par/mL spiked blood). The median values of sensitivities, specificities and accuracies obtained in testing the Set C samples with the 16 tests determined to be good performing by analyzing Sets A and B samples varied considerably. Out of them, four methods depicted the best performing parameters in all three sets of samples, detecting at least 10 fg/µl for each DNA stock, 0.5 par/mL and a sensitivity between 83.3-94.4%, specificity of 85-95%, accuracy of 86.8-89.5% and kappa index of 0.7-0.8 compared to consensus PCR reports of the 16 good performing tests and 63-69%, 100%, 71.4-76.2% and 0.4-0.5, respectively compared to serodiagnosis. Method LbD2 used solvent extraction followed by Sybr-Green based Real time PCR targeted to Sat-DNA; method LbD3 used solvent DNA extraction followed by conventional PCR targeted to Sat-DNA. The third method (LbF1) used glass fiber column based DNA extraction followed by TaqMan Real Time PCR targeted to Sat-DNA (cruzi 1/cruzi 2 and cruzi 3 TaqMan probe) and the fourth method (LbQ) used solvent DNA extraction followed by conventional hot-start PCR targeted to kDNA (primer pairs 121/122). These four methods were further evaluated at the coordinating laboratory in a subset of human blood samples, confirming the performance obtained by the participating laboratories., Conclusion/significance: This study represents a first crucial step towards international validation of PCR procedures for detection of T. cruzi in human blood samples.

Published

2011

33. Two nonrecombining sympatric forms of the human malaria parasite Plasmodium ovale occur globally.

Author

Sutherland CJ, Tanomsing N, Nolder D, Oguike M, Jennison C, Pukrittayakamee S, Dolecek C, Hien TT, do Rosário VE, Arez AP, Pinto J, Michon P, Escalante AA, Nosten F, Burke M, Lee R, Blaze M, Otto TD, Barnwell JW, Pain A, Williams J, White NJ, Day NP, Snounou G, Lockhart PJ, Chiodini PL, Imwong M, and Polley SD

Subjects

Animals, Genetic Variation, Genotype, Global Health, Humans, Malaria epidemiology, Phylogeny, Plasmodium ovale classification, RNA, Ribosomal genetics, Malaria parasitology, Plasmodium ovale genetics

Abstract

Background: Malaria in humans is caused by apicomplexan parasites belonging to 5 species of the genus Plasmodium. Infections with Plasmodium ovale are widely distributed but rarely investigated, and the resulting burden of disease is not known. Dimorphism in defined genes has led to P. ovale parasites being divided into classic and variant types. We hypothesized that these dimorphs represent distinct parasite species., Methods: Multilocus sequence analysis of 6 genetic characters was carried out among 55 isolates from 12 African and 3 Asia-Pacific countries., Results: Each genetic character displayed complete dimorphism and segregated perfectly between the 2 types. Both types were identified in samples from Ghana, Nigeria, São Tomé, Sierra Leone, and Uganda and have been described previously in Myanmar. Splitting of the 2 lineages is estimated to have occurred between 1.0 and 3.5 million years ago in hominid hosts., Conclusions: We propose that P. ovale comprises 2 nonrecombining species that are sympatric in Africa and Asia. We speculate on possible scenarios that could have led to this speciation. Furthermore, the relatively high frequency of imported cases of symptomatic P. ovale infection in the United Kingdom suggests that the morbidity caused by ovale malaria has been underestimated.

Published

2010

34. Human Infections with Plasmodium knowlesi, the Philippines.

Author

Luchavez J, Espino F, Curameng P, Espina R, Bell D, Chiodini P, Nolder D, Sutherland C, Lee KS, and Singh B

Subjects

Adult, Animals, Anopheles parasitology, Humans, Malaria parasitology, Male, Monkey Diseases parasitology, Philippines epidemiology, Plasmodium knowlesi genetics, Plasmodium knowlesi isolation & purification, Polymerase Chain Reaction methods, Zoonoses parasitology, Macaca fascicularis parasitology, Malaria diagnosis, Malaria epidemiology, Monkey Diseases transmission, Plasmodium knowlesi pathogenicity, Zoonoses transmission

Abstract

Five human cases of infection with the simian malaria parasite Plasmodium knowlesi from Palawan, the Philippines, were confirmed by nested PCR. This study suggests that this zoonotic infection is found across a relatively wide area in Palawan and documents autochthonous cases in the country.

Published

2008

35. Multiple hybrid genotypes of Leishmania (viannia) in a focus of mucocutaneous Leishmaniasis.

Author

Nolder D, Roncal N, Davies CR, Llanos-Cuentas A, and Miles MA

Subjects

Animals, Electrophoresis, Genotype, Humans, Isoenzymes analysis, Leishmania genetics, Microsatellite Repeats, Sequence Analysis, DNA, Leishmania classification, Leishmaniasis, Mucocutaneous parasitology

Abstract

The principal agent of mucocutaneous leishmaniasis (MCL) is the South American protozoan parasite Leishmania (Viannia) braziliensis. This organism is generally considered to be clonal, that is, it does not to undergo genetic exchange. Nevertheless, apparent hybrids between several Leishmania species have been reported in the New World and the Old World. When we characterized isolates of Leishmania (Viannia) from a single focus of cutaneous leishmaniasis (CL) and MCL, we found a remarkable phenotypic and genotypic diversity, with 12 zymodemes and 20 microsatellite genotypes. Furthermore, 26 of the 59 isolates were L. braziliensis/L. peruviana phenotypic hybrids that displayed 7 different microsatellite genotypes. A hybrid genotype was the only organism isolated from 4 patients with MCL. Thus hybrids must be included among the potential agents of MCL. Despite the propensity for clonality, hybrids are also an important feature of Leishmania (Viannia) and may give rise to epidemiologically important emergent genotypes.

Published

2007

36. Acanthamoeba genotype T4 from the UK and Iran and isolation of the T2 genotype from clinical isolates.

Author

Maghsood AH, Sissons J, Rezaian M, Nolder D, Warhurst D, and Khan NA

Subjects

Acanthamoeba genetics, Acanthamoeba pathogenicity, Acanthamoeba Keratitis parasitology, Animals, Genotype, Iran, RNA, Ribosomal, 18S analysis, RNA, Ribosomal, 18S genetics, Sequence Analysis, DNA, United Kingdom, Acanthamoeba isolation & purification, Acanthamoeba physiology

Abstract

The majority of the keratitis-causing Acanthamoeba isolates are genotype T4. In an attempt to determine whether predominance of T4 isolates in Acanthamoeba keratitis is due to greater virulence or greater prevalence of this genotype, Acanthamoeba genotypes were determined for 13 keratitis isolates and 12 environmental isolates from Iran. Among 13 clinical isolates, eight (61.5%) belonged to T4, two (15.3%) belonged to T3 and three (23%) belonged to the T2 genotype. In contrast, the majority of 12 environmental isolates tested in the present study belonged to T2 (7/12, 58.3%), followed by 4/12 T4 isolates (33.3%). In addition, the genotypes of six new Acanthamoeba isolates from UK keratitis cases were determined. Of these, five (83.3%) belonged to T4 and one was T3 (16.6%), supporting the expected high frequency of T4 in Acanthamoeba keratitis. In total, the genotypes of 24 Acanthamoeba keratitis isolates from the UK and Iran were determined. Of these, 17 belonged to T4 (70.8%), three belonged to T2 (12.5%), three belonged to T3 (12.5%) and one belonged to T11 (4.1%), confirming that T4 is the predominant genotype (S2=4.167; P=0.0412) in Acanthamoeba keratitis.

Published

2005

37. Post-mortem culture of Balamuthia mandrillaris from the brain and cerebrospinal fluid of a case of granulomatous amoebic meningoencephalitis, using human brain microvascular endothelial cells.

Author

Jayasekera S, Sissons J, Tucker J, Rogers C, Nolder D, Warhurst D, Alsam S, White JML, Higgins EM, and Khan NA

Subjects

Animals, Blood-Brain Barrier, Brain blood supply, Humans, Papio, Polymerase Chain Reaction, Amebiasis parasitology, Amoeba isolation & purification, Brain parasitology, Central Nervous System Protozoal Infections parasitology, Cerebrospinal Fluid parasitology, Endothelial Cells parasitology, Granuloma parasitology

Abstract

The first isolation in the UK of Balamuthia mandrillaris amoebae from a fatal case of granulomatous amoebic meningoencephalitis is reported. Using primary cultures of human brain microvascular endothelial cells (HBMECs), amoebae were isolated from the brain and cerebrospinal fluid (CSF). The cultures showed a cytopathic effect at 20-28 days, but morphologically identifiable B. mandrillaris amoebae were seen in cleared plaques in subcultures at 45 days. The identification of the organism was later confirmed using PCR on Chelex-treated extracts. Serum taken while the patient was still alive reacted strongly with slide antigen prepared from cultures of the post-mortem isolate, and also with those from a baboon B. mandrillaris strain at 1:10,000 in indirect immunofluorescence, but with Acanthamoeba castellanii (Neff) at 1:160, supporting B. mandrillaris to be the causative agent. If the presence of amoebae in the post-mortem CSF reflects the condition in life, PCR studies on CSF and on biopsies of cutaneous lesions may also be a valuable tool. The role of HBMECs in understanding the interactions of B. mandrillaris with the blood-brain barrier is discussed.

Published

2004

38. In vitro activity of nitazoxanide and related compounds against isolates of Giardia intestinalis, Entamoeba histolytica and Trichomonas vaginalis.

Author

Adagu IS, Nolder D, Warhurst DC, and Rossignol JF

Subjects

Amebicides chemistry, Amebicides metabolism, Amebicides pharmacology, Animals, Antiprotozoal Agents chemistry, Antiprotozoal Agents metabolism, Antitrichomonal Agents chemistry, Antitrichomonal Agents metabolism, Antitrichomonal Agents pharmacology, Drug Resistance, Microbial physiology, Entamoeba histolytica isolation & purification, Giardia lamblia isolation & purification, Humans, Microbial Sensitivity Tests statistics & numerical data, Nitro Compounds, Structure-Activity Relationship, Thiazoles chemistry, Thiazoles metabolism, Trichomonas vaginalis isolation & purification, Antiprotozoal Agents pharmacology, Entamoeba histolytica drug effects, Giardia lamblia drug effects, Thiazoles pharmacology, Trichomonas vaginalis drug effects

Abstract

The activities of the N-(nitrothiazolyl) salicylamide nitazoxanide and its metabolite tizoxanide were compared with metronidazole in vitro in microplates against six axenic isolates of Giardia intestinalis. Tizoxanide was eight times more active than metronidazole against metronidazole-susceptible isolates and twice as active against a resistant isolate. In 10 axenic isolates of Entamoeba histolytica, while tizoxanide was almost twice as active as metronidazole against more susceptible isolates, it was more than twice as active against less susceptible isolates. Fourteen metronidazole-susceptible isolates of Trichomonas vaginalis were 1.5 times more susceptible to tizoxanide, which was nearly five times as active against resistant isolates. Two highly metronidazole-resistant isolates retained complete susceptibility to tizoxanide, and one moderately resistant isolate showed reduced susceptibility. In all three organisms, nitazoxanide results paralleled those of tizoxanide. Analogues lacking the reducible nitro-group had similar low activities against susceptible G. intestinalis, E. histolytica and T. vaginalis, indicating that nitro-reduction and free radical production was a probable mode of action. Nitazoxanide and its metabolite tizoxanide are more active in vitro than metronidazole against G. intestinalis, E. histolytica and T. vaginalis. Although, like metronidazole, they depend on the presence of a nitro-group for activity, they retain some activity against metronidazole-resistant strains, particularly of T. vaginalis. The results suggest that resistance mechanisms for metronidazole can be bypassed by nitazoxanide and tizoxanide.

Published

2002

39. Lessons from a child health system on opportunities and threats to quality from networked record systems.

Author

Nolder D and Rigby MJ

Subjects

Child, Humans, United Kingdom, Child Health Services standards, Computer Communication Networks standards, Medical Records Systems, Computerized standards

Published

1995

40. Lessons from a child health system on opportunities and threats to quality from networked record systems.

Author

Rigby MJ and Nolder D

Subjects

Child, Data Collection, Humans, Preventive Health Services statistics & numerical data, United Kingdom, Child Health Services statistics & numerical data, Health Services Accessibility statistics & numerical data, Medical Informatics Applications, Medical Records Systems, Computerized statistics & numerical data

Abstract

The British Child Health System has been designed and widely implemented to support equity of access to preventive child health services, using case-based integrated records. Lately, telematics has been increasingly applied to improve the timeliness of data entry. A special project has been established to monitor overall quality of the system's use and of the resultant preventive services. The telematics application has been found to be a potential threat to quality in a way which would apply to all remote networked patient-based systems. The demonstration will show the methodology and interim results.

Published

1994