Your search keyword '"Simon J. Draper"' showing total 5 results

1. Mapping immune variation and var gene switching in naive hosts infected with Plasmodium falciparum

Author

Matthew Berriman, J. Alexandra Rowe, Simon J. Draper, Michael P. Barrett, Sarah E. Silk, Geetha Sankaranarayanan, Wiebke Nahrendorf, Philip J Spence, Diana Munoz Sandoval, Mandy Sanders, Angela M. Minassian, Clément Regnault, Alasdair Ivens, Ruth O. Payne, N Venkatraman, Adam J. Reid, Magda E. Lotkowska, Áine O'Toole, Kathryn H. Milne, Nick J. Edwards, and Adrian V. S. Hill

Subjects

Myeloid, QH301-705.5, Science, Inflammation, systems immunology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, var gene switching, parasitic diseases, medicine, Parasite hosting, Biology (General), 030304 developmental biology, 0303 health sciences, General Immunology and Microbiology, biology, General Neuroscience, Plasmodium falciparum, General Medicine, biology.organism_classification, medicine.disease, metabolomics, 3. Good health, medicine.anatomical_structure, human immune variation, Infectious disease (medical specialty), inflammation, Immunology, falciparum malaria, Medicine, medicine.symptom, 030217 neurology & neurosurgery, Malaria

Abstract

Falciparum malaria is clinically heterogeneous and the relative contribution of parasite and host in shaping disease severity remains unclear. We explored the interaction between inflammation and parasite variant surface antigen (VSA) expression, asking whether this relationship underpins the variation observed in controlled human malaria infection (CHMI). We uncovered marked heterogeneity in the host response to blood challenge; some volunteers remained quiescent, others triggered interferon-stimulated inflammation and some showed transcriptional evidence of myeloid cell suppression. Significantly, only inflammatory volunteers experienced hallmark symptoms of malaria. When we tracked temporal changes in parasite VSA expression to ask whether variants associated with severe disease rapidly expand in naive hosts, we found no transcriptional evidence to support this hypothesis. These data indicate that parasite variants that dominate severe malaria do not have an intrinsic growth or survival advantage; instead, they presumably rely upon infection-induced changes in their within-host environment for selection.

Published

2021

2. Mapping immune variation and

Author

Kathryn, Milne, Alasdair, Ivens, Adam J, Reid, Magda E, Lotkowska, Aine, O'Toole, Geetha, Sankaranarayanan, Diana, Munoz Sandoval, Wiebke, Nahrendorf, Clement, Regnault, Nick J, Edwards, Sarah E, Silk, Ruth O, Payne, Angela M, Minassian, Navin, Venkatraman, Mandy J, Sanders, Adrian Vs, Hill, Michael, Barrett, Matthew, Berriman, Simon J, Draper, J Alexandra, Rowe, and Philip J, Spence

Subjects

Adult, Male, Erythrocytes, Plasmodium falciparum, Protozoan Proteins, Antibodies, Protozoan, Antigens, Protozoan, systems immunology, P. falciparum, Immunology and Inflammation, var gene switching, parasitic diseases, Anopheles, Animals, Humans, Malaria, Falciparum, Inflammation, Microbiology and Infectious Disease, Antigenic Variation, metabolomics, human immune variation, Host-Pathogen Interactions, falciparum malaria, Female, Research Article, Human

Abstract

Falciparum malaria is clinically heterogeneous and the relative contribution of parasite and host in shaping disease severity remains unclear. We explored the interaction between inflammation and parasite variant surface antigen (VSA) expression, asking whether this relationship underpins the variation observed in controlled human malaria infection (CHMI). We uncovered marked heterogeneity in the host response to blood challenge; some volunteers remained quiescent, others triggered interferon-stimulated inflammation and some showed transcriptional evidence of myeloid cell suppression. Significantly, only inflammatory volunteers experienced hallmark symptoms of malaria. When we tracked temporal changes in parasite VSA expression to ask whether variants associated with severe disease rapidly expand in naive hosts, we found no transcriptional evidence to support this hypothesis. These data indicate that parasite variants that dominate severe malaria do not have an intrinsic growth or survival advantage; instead, they presumably rely upon infection-induced changes in their within-host environment for selection.

Published

2020

3. Rapid and iterative genome editing in the malaria parasite

Author

Franziska, Mohring, Melissa Natalie, Hart, Thomas A, Rawlinson, Ryan, Henrici, James A, Charleston, Ernest, Diez Benavente, Avnish, Patel, Joanna, Hall, Neil, Almond, Susana, Campino, Taane G, Clark, Colin J, Sutherland, David A, Baker, Simon J, Draper, and Robert William, Moon

Subjects

Gene Editing, Microbiology and Infectious Disease, Biomedical Research, Protozoan Proteins, Antigens, Protozoan, Receptors, Cell Surface, Genetics and Genomics, Duffy binding protein, P. falciparum, Malaria, Tools and Resources, vaccine, parasitic diseases, Malaria Vaccines, Malaria, Vivax, Animals, Humans, Parasites, Plasmodium knowlesi, Other, CRISPR-Cas9, genome-editing, Plasmodium vivax

Abstract

Tackling relapsing Plasmodium vivax and zoonotic Plasmodium knowlesi infections is critical to reducing malaria incidence and mortality worldwide. Understanding the biology of these important and related parasites was previously constrained by the lack of robust molecular and genetic approaches. Here, we establish CRISPR-Cas9 genome editing in a culture-adapted P. knowlesi strain and define parameters for optimal homology-driven repair. We establish a scalable protocol for the production of repair templates by PCR and demonstrate the flexibility of the system by tagging proteins with distinct cellular localisations. Using iterative rounds of genome-editing we generate a transgenic line expressing P. vivax Duffy binding protein (PvDBP), a lead vaccine candidate. We demonstrate that PvDBP plays no role in reticulocyte restriction but can alter the macaque/human host cell tropism of P. knowlesi. Critically, antibodies raised against the P. vivax antigen potently inhibit proliferation of this strain, providing an invaluable tool to support vaccine development.

Published

2019

4. Erythrocyte invasion-neutralising antibodies prevent Plasmodium falciparum RH5 from binding to basigin-containing membrane protein complexes

Author

Abhishek Jamwal, Cristina F Constantin, Stephan Hirschi, Sebastian Henrich, Wolfgang Bildl, Bernd Fakler, Simon J Draper, Uwe Schulte, and Matthew K Higgins

Subjects

PfRH5, basigin, monoclonal antibody, PMCA, MCT1, malaria, Medicine, Science, Biology (General), QH301-705.5

Abstract

Basigin is an essential host receptor for invasion of Plasmodium falciparum into human erythrocytes, interacting with parasite surface protein PfRH5. PfRH5 is a leading blood-stage malaria vaccine candidate and a target of growth-inhibitory antibodies. Here, we show that erythrocyte basigin is exclusively found in one of two macromolecular complexes, bound either to plasma membrane Ca2+-ATPase 1/4 (PMCA1/4) or to monocarboxylate transporter 1 (MCT1). PfRH5 binds to each of these complexes with a higher affinity than to isolated basigin ectodomain, making it likely that these are the physiological targets of PfRH5. PMCA-mediated Ca2+ export is not affected by PfRH5, making it unlikely that this is the mechanism underlying changes in calcium flux at the interface between an erythrocyte and the invading parasite. However, our studies rationalise the function of the most effective growth-inhibitory antibodies targeting PfRH5. While these antibodies do not reduce the binding of PfRH5 to monomeric basigin, they do reduce its binding to basigin-PMCA and basigin-MCT complexes. This indicates that the most effective PfRH5-targeting antibodies inhibit growth by sterically blocking the essential interaction of PfRH5 with basigin in its physiological context.

Published

2023

5. Mapping immune variation and var gene switching in naive hosts infected with Plasmodium falciparum

Author

Kathryn Milne, Alasdair Ivens, Adam J Reid, Magda E Lotkowska, Aine O'Toole, Geetha Sankaranarayanan, Diana Munoz Sandoval, Wiebke Nahrendorf, Clement Regnault, Nick J Edwards, Sarah E Silk, Ruth O Payne, Angela M Minassian, Navin Venkatraman, Mandy J Sanders, Adrian VS Hill, Michael Barrett, Matthew Berriman, Simon J Draper, J Alexandra Rowe, and Philip J Spence

Subjects

falciparum malaria, human immune variation, inflammation, var gene switching, metabolomics, systems immunology, Medicine, Science, Biology (General), QH301-705.5

Abstract

Falciparum malaria is clinically heterogeneous and the relative contribution of parasite and host in shaping disease severity remains unclear. We explored the interaction between inflammation and parasite variant surface antigen (VSA) expression, asking whether this relationship underpins the variation observed in controlled human malaria infection (CHMI). We uncovered marked heterogeneity in the host response to blood challenge; some volunteers remained quiescent, others triggered interferon-stimulated inflammation and some showed transcriptional evidence of myeloid cell suppression. Significantly, only inflammatory volunteers experienced hallmark symptoms of malaria. When we tracked temporal changes in parasite VSA expression to ask whether variants associated with severe disease rapidly expand in naive hosts, we found no transcriptional evidence to support this hypothesis. These data indicate that parasite variants that dominate severe malaria do not have an intrinsic growth or survival advantage; instead, they presumably rely upon infection-induced changes in their within-host environment for selection.

Published

2021