Your search keyword '"Matthew W. A. Dixon"' showing total 70 results

1. Nanobodies against Pfs230 block Plasmodium falciparum transmission

Author

Melanie H. Dietrich, Mikha Gabriela, Kitsanapong Reaksudsan, Matthew W. A. Dixon, Li-Jin Chan, Amy Adair, Stephanie Trickey, Matthew T. O'Neill, Li Lynn Tan, Sash Lopaticki, Julie Healer, Sravya Keremane, Alan F. Cowman, and Wai-Hong Tham

Subjects

Plasmodium falciparum, Protozoan Proteins, Animals, Humans, Antibodies, Protozoan, Antigens, Protozoan, Cysteine, Cell Biology, Single-Domain Antibodies, Molecular Biology, Biochemistry, Malaria

Abstract

Transmission blocking interventions can stop malaria parasite transmission from mosquito to human by inhibiting parasite infection in mosquitos. One of the most advanced candidates for a malaria transmission blocking vaccine is Pfs230. Pfs230 is the largest member of the 6-cysteine protein family with 14 consecutive 6-cysteine domains and is expressed on the surface of gametocytes and gametes. Here, we present the crystal structure of the first two 6-cysteine domains of Pfs230. We identified high affinity Pfs230-specific nanobodies that recognized gametocytes and bind to distinct sites on Pfs230, which were isolated from immunized alpacas. Using two non-overlapping Pfs230 nanobodies, we show that these nanobodies significantly blocked P. falciparum transmission and reduced the formation of exflagellation centers. Crystal structures of the transmission blocking nanobodies with the first 6-cysteine domain of Pfs230 confirm that they bind to different epitopes. In addition, these nanobodies bind to Pfs230 in the absence of the prodomain, in contrast with the binding of known Pfs230 transmission blocking antibodies. These results provide additional structural insight into Pfs230 domains and elucidate a mechanism of action of transmission blocking Pfs230 nanobodies.

Published

2022

2. Repurposing the mitotic machinery to drive cellular elongation and chromatin reorganisation in Plasmodium falciparum gametocytes

Author

Jiahong Li, Gerald J. Shami, Ellie Cho, Boyin Liu, Eric Hanssen, Matthew W. A. Dixon, and Leann Tilley

Subjects

Multidisciplinary, Centromere, Plasmodium falciparum, General Physics and Astronomy, General Chemistry, Kinetochores, Microtubules, General Biochemistry, Genetics and Molecular Biology, Chromatin

Abstract

The sexual stage gametocytes of the malaria parasite, Plasmodium falciparum, adopt a falciform (crescent) shape driven by the assembly of a network of microtubules anchored to a cisternal inner membrane complex (IMC). Using 3D electron microscopy, we show that a non-mitotic microtubule organizing center (MTOC), embedded in the parasite’s nuclear membrane, orients the endoplasmic reticulum and the nascent IMC and seeds cytoplasmic microtubules. A bundle of microtubules extends into the nuclear lumen, elongating the nuclear envelope and capturing the chromatin. Classical mitotic machinery components, including centriolar plaque proteins, Pfcentrin-1 and −4, microtubule-associated protein, End-binding protein-1, kinetochore protein, PfNDC80 and centromere-associated protein, PfCENH3, are involved in the nuclear microtubule assembly/disassembly process. Depolymerisation of the microtubules using trifluralin prevents elongation and disrupts the chromatin, centromere and kinetochore organisation. We show that the unusual non-mitotic hemispindle plays a central role in chromatin organisation, IMC positioning and subpellicular microtubule formation in gametocytes.

Published

2022

3. Cell biological analysis reveals an essential role for Pfcerli2 in erythrocyte invasion by malaria parasites

Author

Benjamin Liffner, Juan Miguel Balbin, Gerald J. Shami, Ghizal Siddiqui, Jan Strauss, Sonja Frölich, Gary K. Heinemann, Ella May Edwards, Arne Alder, Jan Stephan Wichers, Darren J. Creek, Leann Tilley, Matthew W. A. Dixon, Tim-Wolf Gilberger, Danny W. Wilson, Liffner, Benjamin, Balbin, Juan Miguel, Shami, Gerald J, Siddiqui, Ghizal, Strauss, Jan, Frölich, Sonja, Heinemann, Gary K, Edwards, Ella May, Alder, Arne, Wichers, Jan Stephan, Creek, Darren J, Tilley, Leann, Dixon, Matthew WA, Gilberger, Tim-Wolf, and Wilson, Danny W

Subjects

riboswitches, Erythrocytes, QH301-705.5, Protozoan Proteins, Medicine (miscellaneous), General Biochemistry, Genetics and Molecular Biology, Malaria, 3. Good health, parasite biology, parasitic diseases, Animals, Humans, Parasites, Biology (General), General Agricultural and Biological Sciences, Phylogeny

Abstract

Merozoite invasion of host red blood cells (RBCs) is essential for survival of the human malaria parasite Plasmodium falciparum. Proteins involved with RBC binding and invasion are secreted from dual-club shaped organelles at the apical tip of the merozoite called the rhoptries. Here we characterise P. falciparum Cytosolically Exposed Rhoptry Leaflet Interacting protein 2 (PfCERLI2), as a rhoptry bulb protein that is essential for merozoite invasion. Phylogenetic analyses show that cerli2 arose through an ancestral gene duplication of cerli1. We show that PfCERLI2 is essential for blood-stage growth and localises to the cytosolic face of the rhoptry bulb. Inducible knockdown of PfCERLI2 led to a proportion of merozoites failing to invade and was associated with elongation of the rhoptry organelle during merozoite development and inhibition of rhoptry antigen processing. These findings identify PfCERLI2 as a protein that has key roles in rhoptry biology during merozoite invasion.

Published

2022

4. Virulence determinant, PTP7, controls vesicle budding from the Maurer’s clefts, adhesin protein trafficking and host cell remodeling inPlasmodium falciparum

Author

Adam J. Blanch, Boyin Liu, Matthew W. A. Dixon, Gerald J. Shami, Olivia M. S. Carmo, Leann Tilley, Snigdha Tiash, and Dezerae Cox

Subjects

Virulence, Plasmodium falciparum, Biology, biology.organism_classification, Plasmodium, Virulence factor, Cell biology, Bacterial adhesin, Red blood cell, medicine.anatomical_structure, Cytoplasm, parasitic diseases, Organelle, medicine

Abstract

Presentation of the variant antigen,Plasmodium falciparumerythrocyte membrane protein 1 (EMP1), at knob-like protrusions on the surface of infected red blood cells, underpinsP. falciparummalaria pathogenicity. Here we describe a protein PF3D7_0301700 (PTP7), that functions at the nexus between the intermediate trafficking organelle, the Maurer’s cleft, and the infected red blood cell surface. Genetic disruption of PTP7 leads to accumulation of vesicles at the Maurer’s clefts, grossly aberrant knob morphology, and failure to deliver EMP1 to the red blood cell surface. We show that an expanded low complexity sequence in the C-terminal region of PTP7, found only in theLaveraniaclade ofPlasmodium, is critical for efficient virulence protein trafficking.Author SummaryWe describe a malaria parasite protein involved in virulence factor trafficking (PTP7) that moves between different compartments in the host red blood cell cytoplasm in a stage-dependent manner. Upon disruption of the PTP7 locus, the Maurer’s cleft trafficking compartments become decorated with vesicles; the knobby protrusions on the host red blood cell surface are depleted and distorted; and trafficking of the virulence protein, EMP1, to the host red blood cell surface is ablated. We provide evidence that a region of PTP7 with low sequence complexity plays an important role in driving fission of vesicles from the Maurer’s clefts.

Published

2021

5. Safety, infectivity and immunogenicity of a genetically attenuated blood-stage malaria vaccine

Author

Leann Tilley, Helen Jennings, Paul M. Griffin, Stephen Woolley, Anthony T. Papenfuss, Michelle J. Boyle, Fiona H. Amante, Jocelyn Sietsma Penington, Silvana Sekuloski, James S. McCarthy, Fabian de Labastida Rivera, Katharine R. Trenholme, Bridget E. Barber, Jo-Anne Chan, Emily M. Eriksson, Christian R. Engwerda, Anand Odedra, Michael F. Duffy, Dean Andrew, Alister Craig, Krystal J. Evans, Priyanka Sathe, Matthew W. A. Dixon, Julie Healer, Janet Storm, Rebecca Webster, Adam J. Blanch, Alan F. Cowman, and Louis Schofield

Subjects

Male, Plasmodium falciparum, Protozoan Proteins, Parasitemia, KAHRP, Vaccines, Attenuated, qw_805, Antimalarials, Genetically attenuated, parasitic diseases, Malaria Vaccines, Vaccine Development, Medicine, Humans, Artemether, Malaria, Falciparum, Infectivity, biology, business.industry, Malaria vaccine, Immunogenicity, Artemether, Lumefantrine Drug Combination, Australia, General Medicine, medicine.disease, biology.organism_classification, Virology, wc_750, Malaria, PfEMP1, qu_450, business, Vaccine, medicine.drug, Research Article

Abstract

Background There is a clear need for novel approaches to malaria vaccine development. We aimed to develop a genetically attenuated blood-stage vaccine and test its safety, infectivity, and immunogenicity in healthy volunteers. Our approach was to target the gene encoding the knob-associated histidine-rich protein (KAHRP), which is responsible for the assembly of knob structures at the infected erythrocyte surface. Knobs are required for correct display of the polymorphic adhesion ligand P. falciparum erythrocyte membrane protein 1 (PfEMP1), a key virulence determinant encoded by a repertoire of var genes. Methods The gene encoding KAHRP was deleted from P. falciparum 3D7 and a master cell bank was produced in accordance with Good Manufacturing Practice. Eight malaria naïve males were intravenously inoculated (day 0) with 1800 (2 subjects), 1.8 × 105 (2 subjects), or 3 × 106 viable parasites (4 subjects). Parasitemia was measured using qPCR; immunogenicity was determined using standard assays. Parasites were rescued into culture for in vitro analyses (genome sequencing, cytoadhesion assays, scanning electron microscopy, var gene expression). Results None of the subjects who were administered with 1800 or 1.8 × 105 parasites developed parasitemia; 3/4 subjects administered 3× 106 parasites developed significant parasitemia, first detected on days 13, 18, and 22. One of these three subjects developed symptoms of malaria simultaneously with influenza B (day 17; 14,022 parasites/mL); one subject developed mild symptoms on day 28 (19,956 parasites/mL); and one subject remained asymptomatic up to day 35 (5046 parasites/mL). Parasitemia rapidly cleared with artemether/lumefantrine. Parasitemia induced a parasite-specific antibody and cell-mediated immune response. Parasites cultured ex vivo exhibited genotypic and phenotypic properties similar to inoculated parasites, although the var gene expression profile changed during growth in vivo. Conclusions This study represents the first clinical investigation of a genetically attenuated blood-stage human malaria vaccine. A P. falciparum 3D7 kahrp– strain was tested in vivo and found to be immunogenic but can lead to patent parasitemia at high doses. Trial registration Australian New Zealand Clinical Trials Registry (number: ACTRN12617000824369; date: 06 June 2017).

Published

2021

6. Pfcerli2, a duplicated gene in the malaria parasitePlasmodium falciparumessential for invasion of erythrocytes as revealed by phylogenetic and cell biological analysis

Author

Jan Strauss, Leann Tilley, Benjamin Liffner, Arne Alder, Matthew W. A. Dixon, Danny W. Wilson, Gerald J. Shami, Tim-Wolf Gilberger, Juan Miguel Balbin, Jan Stephan Wichers, Sonja Frölich, and Gary K. Heinemann

Subjects

Gene knockdown, medicine.anatomical_structure, biology, Rhoptry, Antigen processing, Cell, Gene duplication, Organelle, medicine, Plasmodium falciparum, biology.organism_classification, Gene, Cell biology

Abstract

Merozoite invasion of host red blood cells (RBCs) is essential for survival of the human malaria parasitePlasmodium falciparum. Proteins involved with RBC binding and invasion are secreted from dual-club shaped organelles at the apical tip of the merozoite called the rhoptries. Here we characteriseP. falciparumCytosolically Exposed Rhoptry Leaflet Interacting protein 2 (PfCERLI2), as a rhoptry bulb protein that is essential for merozoite invasion. Phylogenetic analyses show thatcerli2arose through an ancestral gene duplication ofcerli1, a related cytosolically exposed rhoptry bulb protein. We show that PfCERLI2 is essential for blood-stage growth and localises to the cytosolic face of the rhoptry bulb. Inducible knockdown of PfCERLI2 led to an inhibition of merozoite invasion after tight junction formation. PfCERLI2 knockdown was associated with inhibition of rhoptry antigen processing and a significant elongation of the rhoptries, suggesting that the inability of merozoites to invade is caused by aberrant rhoptry function due to PfCERLI2 deficiency. These findings identify PfCERLI2 as a protein that has key roles in rhoptry biology during merozoite invasion.

Published

2020

7. Plasmodium falciparum artemisinin-resistant K13 mutations confer a sexual-stage transmission advantage that can be overcome with atovaquone-proguanil

Author

Bridget E. Barber, Sachel Mok, James S. McCarthy, Hayley Mitchell, Anand Odedra, Joerg J. Moehrle, Jeremy Gower, Louise Marquart, David A. Fidock, Maria Rebelo, Gregory J. Robinson, Sam McEwan, Katharine A. Collins, Rebecca E. Watts, Claire Y. T. Wang, Lachlan Webb, Sean Lynch, Zuleima Pava, and Matthew W. A. Dixon

Subjects

biology, Transmission (medicine), Mutant, Plasmodium falciparum, biology.organism_classification, Atovaquone/proguanil, Virology, chemistry.chemical_compound, chemistry, Artesunate, parasitic diseases, medicine, Gametocyte, Artemisinin, Anopheles stephensi, medicine.drug

Abstract

Containing the spread of artemisinin (ART)-resistant Plasmodium falciparum will be assisted by improved understanding of its human-to-mosquito transmission. We compared gametocyte dynamics among field isolates containing K13 mutations conferring ART resistance and K13 wild-type parasites. In Pailin, Cambodia, the male to female gametocyte ratio was higher among K13 mutant infections compared to K13 wild-type infections. We also investigated the effects of artesunate and atovaquone-proguanil on the transmissibility of an ART-resistant K13 mutant strain, Cam3.IIR539T, in a volunteer infection study. Gametocyte production was higher after a single dose of artesunate (2 mg/kg) in volunteers infected with ART-resistant compared to ART-sensitive parasites. Despite the presence of gametocytes in volunteers infected with ART-resistant parasites, there was no infection observed in Anopheles stephensi mosquitoes after atovaquone-proguanil treatment. We report transmission determinants of ART-resistant infections that could be advantageous over ART-sensitive infections. Moreover, we show additional benefits of treating ART-resistant infections with atovaquone-proguanil treatment.

Published

2020

8. Surface area-to-volume ratio, not cellular rigidity, determines red blood cell traversal through small capillaries

Author

Matthew W. A. Dixon, Oliver Looker, Peter Vee Sin Lee, Olivia M. S. Carmo, Arman Namvar, Li-Jin Chan, Leann Tilley, Dean Andrew, Wai-Hong Tham, Vijay Rajagopal, Adam J. Blanch, Snigdha Tiash, and Boyin Liu

Subjects

Red blood cell, Rigidity (electromagnetism), medicine.anatomical_structure, Membrane, Surface-area-to-volume ratio, Chemistry, Biophysics, medicine, Marked effect, Rbc membrane, Viscoelasticity, circulatory and respiratory physiology

Abstract

SummaryThe remarkable deformability of red blood cells (RBCs) depends on the viscoelasticity of the plasma membrane and cell contents and the surface area to volume (SA:V) ratio; however, it remains unclear which of these factors is the key determinant for passage through small capillaries. We used a microfluidic device to examine the traversal of normal, stiffened, swollen, parasitised and immature RBCs. We show that dramatic stiffening of RBCs had no measurable effect on their ability to traverse small channels. By contrast, a moderate decrease in the SA:V ratio had a marked effect on the equivalent cylinder diameter that is traversable by RBCs of similar stiffness. We developed a finite element model that provides a coherent rationale for the experimental observations, based on the nonlinear mechanical behaviour of the RBC membrane skeleton. We conclude that the SA:V ratio should be given more prominence in studies of RBC pathologies.

Published

2020

9. Surface area-to-volume ratio, not cellular viscoelasticity, is the major determinant of red blood cell traversal through small channels

Author

Oliver Looker, Matthew W. A. Dixon, Peter Vee Sin Lee, Leann Tilley, Snigdha Tiash, Vijay Rajagopal, Arman Namvar, Adam J. Blanch, Olivia M. S. Carmo, Wai-Hong Tham, Boyin Liu, Li-Jin Chan, and Dean Andrew

Subjects

Erythrocytes, Immunology, red blood cell, Biology, Microbiology, Models, Biological, Viscoelasticity, Microcirculation, 03 medical and health sciences, Reticulocyte, Cell Movement, Virology, Erythrocyte Deformability, Lab-On-A-Chip Devices, medicine, Cylinder, Erythrocyte deformability, Humans, deformability, Cell Shape, Research Articles, 030304 developmental biology, Cell Size, 0303 health sciences, 030306 microbiology, reticulocyte, hemic and immune systems, Capillaries, Red blood cell, Membrane, medicine.anatomical_structure, Surface-area-to-volume ratio, plasmodium, Biophysics, surface area‐to‐volume ratio, circulatory and respiratory physiology, Research Article

Abstract

The remarkable deformability of red blood cells (RBCs) depends on the viscoelasticity of the plasma membrane and cell contents and the surface area to volume (SA:V) ratio; however, it remains unclear which of these factors is the key determinant for passage through small capillaries. We used a microfluidic device to examine the traversal of normal, stiffened, swollen, parasitised and immature RBCs. We show that dramatic stiffening of RBCs had no measurable effect on their ability to traverse small channels. By contrast, a moderate decrease in the SA:V ratio had a marked effect on the equivalent cylinder diameter that is traversable by RBCs of similar cellular viscoelasticity. We developed a finite element model that provides a coherent rationale for the experimental observations, based on the nonlinear mechanical behaviour of the RBC membrane skeleton. We conclude that the SA:V ratio should be given more prominence in studies of RBC pathologies.

Published

2020

10. Role of <named-content content-type='genus-species'>Plasmodium falciparum</named-content> Protein GEXP07 in Maurer’s Cleft Morphology, Knob Architecture, and <named-content content-type='genus-species'>P. falciparum</named-content> EMP1 Trafficking

Author

Oliver Looker, Matthew W. A. Dixon, Andy J. Y. Low, Emma McHugh, Olivia M. S. Carmo, Boyin Liu, Adam J. Blanch, Steven Batinovic, Dean Andrew, Snigdha Tiash, Hyun-Jung Cho, Paul J. McMillan, and Leann Tilley

Subjects

Erythrocytes, Plasmodium falciparum, Protozoan Proteins, malaria, Virulence, Microbiology, Green fluorescent protein, Cell Line, Host-Parasite Interactions, Host-Microbe Biology, 03 medical and health sciences, Antigen, Virology, Organelle, parasitic diseases, Humans, Protein Interaction Maps, 030304 developmental biology, 0303 health sciences, biology, 030306 microbiology, Erythrocyte Membrane, Membrane Proteins, Maurer's cleft, biology.organism_classification, QR1-502, 3. Good health, Transport protein, Cell biology, Protein Transport, Membrane protein, protein trafficking, Carrier Proteins, virulence determinants, Research Article

Abstract

The trafficking of the virulence antigen PfEMP1 and its presentation at the knob structures at the surface of parasite-infected RBCs are central to severe adhesion-related pathologies such as cerebral and placental malaria. This work adds to our understanding of how PfEMP1 is trafficked to the RBC membrane by defining the protein-protein interaction networks that function at the Maurer’s clefts controlling PfEMP1 loading and unloading. We characterize a protein needed for virulence protein trafficking and provide new insights into the mechanisms for host cell remodeling, parasite survival within the host, and virulence., The malaria parasite Plasmodium falciparum traffics the virulence protein P. falciparum erythrocyte membrane protein 1 (PfEMP1) to the surface of infected red blood cells (RBCs) via membranous organelles, known as the Maurer’s clefts. We developed a method for efficient enrichment of Maurer’s clefts and profiled the protein composition of this trafficking organelle. We identified 13 previously uncharacterized or poorly characterized Maurer’s cleft proteins. We generated transfectants expressing green fluorescent protein (GFP) fusions of 7 proteins and confirmed their Maurer’s cleft location. Using co-immunoprecipitation and mass spectrometry, we generated an interaction map of proteins at the Maurer’s clefts. We identified two key clusters that may function in the loading and unloading of PfEMP1 into and out of the Maurer’s clefts. We focus on a putative PfEMP1 loading complex that includes the protein GEXP07/CX3CL1-binding protein 2 (CBP2). Disruption of GEXP07 causes Maurer’s cleft fragmentation, aberrant knobs, ablation of PfEMP1 surface expression, and loss of the PfEMP1-mediated adhesion. ΔGEXP07 parasites have a growth advantage compared to wild-type parasites, and the infected RBCs are more deformable and more osmotically fragile.

Published

2020

11. PfCERLI1 is a conserved rhoptry associated protein essential for Plasmodium falciparum merozoite invasion of erythrocytes

Author

Boyin Liu, Benjamin Liffner, Danny W. Wilson, Matthew W. A. Dixon, Stuart A. Ralph, Gary K. Heinemann, Tim-Wolf Gilberger, Sonja Frölich, Liffner, Benjamin, Frölich, Sonja, Heinemann, Gary K, Liu, Boyin, Ralph, Stuart A, Dixon, Matthew WA, Gilberger, Tim Wolf, and Wilson, Danny W

Subjects

0301 basic medicine, Erythrocytes, Science, Plasmodium falciparum, 030106 microbiology, Protozoan Proteins, malaria, General Physics and Astronomy, erythrocyte invasion, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Schizogony, 03 medical and health sciences, parasitic diseases, Organelle, Humans, Secretion, Malaria, Falciparum, lcsh:Science, Organelles, plasmodium falciparu, Gene knockdown, Multidisciplinary, Rhoptry, Merozoites, General Chemistry, biology.organism_classification, 3. Good health, Cell biology, Parasite biology, Cytosol, 030104 developmental biology, lcsh:Q, Parasitology, Organelle biogenesis

Abstract

The disease-causing blood-stage of the Plasmodium falciparum lifecycle begins with invasion of human erythrocytes by merozoites. Many vaccine candidates with key roles in binding to the erythrocyte surface and entry are secreted from the large bulb-like rhoptry organelles at the apical tip of the merozoite. Here we identify an essential role for the conserved protein P. falciparum Cytosolically Exposed Rhoptry Leaflet Interacting protein 1 (PfCERLI1) in rhoptry function. We show that PfCERLI1 localises to the cytosolic face of the rhoptry bulb membrane and knockdown of PfCERLI1 inhibits merozoite invasion. While schizogony and merozoite organelle biogenesis appear normal, biochemical techniques and semi-quantitative super-resolution microscopy show that PfCERLI1 knockdown prevents secretion of key rhoptry antigens that coordinate merozoite invasion. PfCERLI1 is a rhoptry associated protein identified to have a direct role in function of this essential merozoite invasion organelle, which has broader implications for understanding apicomplexan invasion biology., Rhoptries are essential organelles for invasion of erythrocytes by Plasmodium. Here, the authors characterize the rhoptry-associated protein CERLI1 using quantitative super-resolution microscopy, showing that it is important for parasite invasion and secretion of rhoptry proteins including vaccine antigens.

Published

2020

12. The Metabolite Repair Enzyme Phosphoglycolate Phosphatase Regulates Central Carbon Metabolism and Fosmidomycin Sensitivity in Plasmodium falciparum

Author

Simon A. Cobbold, Phillip L. van der Peet, Spencer J. Williams, Matthew W. A. Dixon, Alan F. Cowman, Danushka S. Marapana, Leann Tilley, Mark B. Richardson, Malcolm J. McConville, Laure Dumont, and Tony Triglia

Subjects

parasitology, fosmidomycin, Metabolite, Plasmodium falciparum, Phosphatase, Drug Resistance, Pentose phosphate pathway, Microbiology, Host-Microbe Biology, Antimalarials, 03 medical and health sciences, chemistry.chemical_compound, Fosfomycin, Virology, pentose, medicine, Humans, Glycolysis, Malaria, Falciparum, 030304 developmental biology, 0303 health sciences, antimalarial, isoprenoid, Chemistry, 030302 biochemistry & molecular biology, Sugar Acids, Metabolism, glycolysis, metabolomics, QR1-502, Carbon, Phosphoric Monoester Hydrolases, Fosmidomycin, 3. Good health, Biochemistry, CRISPR, Lactates, metabolic regulation, metabolism, Flux (metabolism), Phosphoglycolate phosphatase, Research Article, medicine.drug

Abstract

The malaria parasite has a voracious appetite, requiring large amounts of glucose and nutrients for its rapid growth and proliferation inside human red blood cells. The host cell is resource rich, but this is a double-edged sword; nutrient excess can lead to undesirable metabolic reactions and harmful by-products. Here, we demonstrate that the parasite possesses a metabolite repair enzyme (PGP) that suppresses harmful metabolic by-products (via substrate dephosphorylation) and allows the parasite to maintain central carbon metabolism. Loss of PGP leads to the accumulation of two damaged metabolites and causes a domino effect of metabolic dysregulation. Accumulation of one damaged metabolite inhibits an essential enzyme in the pentose phosphate pathway, leading to substrate accumulation and secondary inhibition of glycolysis. This work highlights how the parasite coordinates metabolic flux by eliminating harmful metabolic by-products to ensure rapid proliferation in its resource-rich niche., Members of the haloacid dehalogenase (HAD) family of metabolite phosphatases play an important role in regulating multiple pathways in Plasmodium falciparum central carbon metabolism. We show that the P. falciparum HAD protein, phosphoglycolate phosphatase (PGP), regulates glycolysis and pentose pathway flux in asexual blood stages via detoxifying the damaged metabolite 4-phosphoerythronate (4-PE). Disruption of the P. falciparum pgp gene caused accumulation of two previously uncharacterized metabolites, 2-phospholactate and 4-PE. 4-PE is a putative side product of the glycolytic enzyme, glyceraldehyde-3-phosphate dehydrogenase, and its accumulation inhibits the pentose phosphate pathway enzyme, 6-phosphogluconate dehydrogenase (6-PGD). Inhibition of 6-PGD by 4-PE leads to an unexpected feedback response that includes increased flux into the pentose phosphate pathway as a result of partial inhibition of upper glycolysis, with concomitant increased sensitivity to antimalarials that target pathways downstream of glycolysis. These results highlight the role of metabolite detoxification in regulating central carbon metabolism and drug sensitivity of the malaria parasite.

Published

2019

13. Plasmodium falciparum goes bananas for sex

Author

Matthew W. A. Dixon and Leann Tilley

Subjects

Male, Erythrocytes, Shape change, Plasmodium falciparum, 030231 tropical medicine, Biology, Microtubules, Gametogenesis, Host-Parasite Interactions, 03 medical and health sciences, 0302 clinical medicine, Reproduction, Asexual, parasitic diseases, medicine, Gametocyte, Animals, Humans, Parasite hosting, Malaria, Falciparum, Molecular Biology, 030304 developmental biology, Spherical shape, Life Cycle Stages, 0303 health sciences, Inner membrane complex, medicine.disease, biology.organism_classification, Biomechanical Phenomena, Insect Vectors, 3. Good health, Culicidae, Evolutionary biology, Vector (epidemiology), Hepatocytes, Female, Parasitology, Malaria

Abstract

The sexual blood stages of the human malaria parasite Plasmodium falciparum undergo a remarkable transformation from a roughly spherical shape to an elongated crescent or "falciform" morphology from which the species gets its name. In this review, the molecular events that drive this spectacular shape change are discussed and some questions that remain regarding the mechanistic underpinnings are posed. We speculate on the role of the shape changes in promoting sequestration and release of the developing gametocyte, thereby facilitating parasite survival in the host and underpinning transmission to the mosquito vector.

Published

2021

14. Initiation of gametocytogenesis at very low parasite density in Plasmodium falciparum infection

Author

Leann Tilley, Matthew W. A. Dixon, Ryan Farid, and James S. McCarthy

Subjects

Adult, Male, Gametocyte EXported Protein-5, 0301 basic medicine, Plasmodium, Artemether/lumefantrine, Adolescent, Plasmodium falciparum, Protozoan Proteins, Parasitemia, Biology, Parasite load, Parasite Load, Antimalarials, Young Adult, 03 medical and health sciences, experimentally induced blood stage malaria, Piperaquine, parasitic diseases, Major Article, Gametocyte, medicine, Animals, Humans, Immunology and Allergy, Malaria, Falciparum, Life Cycle Stages, Australia, Membrane Proteins, piperaquine, Middle Aged, biology.organism_classification, medicine.disease, Virology, early gametocyte marker, 3. Good health, 030104 developmental biology, Infectious Diseases, Linear Models, Quinolines, Female, Carrier Proteins, Biomarkers, Malaria, medicine.drug

Abstract

The recent focus on the elimination of malaria has led to an increased interest in the role of sexual stages in its transmission. We introduce Plasmodium falciparum gametocyte exported protein-5 (PfGEXP5) transcript analysis as an important tool for evaluating the earliest (ring) stage sexual gametocytes in the blood of infected individuals. We show that gametocyte rings are detected in the peripheral blood immediately following establishment of asexual infections—without the need for triggers such as high-density asexual parasitemia or drug treatment. Committed gametocytes are refractory to the commonly used drug piperaquine, and mature gametocytes reappear in the bloodstream 10 days after the initial appearance of gametocyte rings. A further wave of commitment is observed following recrudescent asexual parasitemia, and these gametocytes are again refractory to piperaquine treatment. This work has implications for monitoring gametocyte and transmission dynamics and responses to drug treatment.

Published

2017

15. PfCERLI1, a conserved rhoptry associated protein essential for invasion by Plasmodium falciparum merozoites

Author

Benjamin Liffner, Tim-Wolf Gilberger, Matthew W. A. Dixon, Danny W. Wilson, Boyin Liu, Sonja Frölich, and Gary K. Heinemann

Subjects

0303 health sciences, Gene knockdown, Rhoptry, Plasmodium falciparum, Biology, biology.organism_classification, 3. Good health, Cell biology, Schizogony, 03 medical and health sciences, Cytosol, 0302 clinical medicine, Organelle, parasitic diseases, Secretion, Organelle biogenesis, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

The disease-causing blood stage of thePlasmodium falciparumlifecycle begins with invasion of human erythrocytes by merozoites. Many vaccine candidates with key roles in binding to the erythrocyte surface and entry are secreted from the large bulb-like rhoptry organelles at the apical tip of the merozoite. Here we identify an essential role for the conserved proteinP. falciparumCytosolicallyExposedRhoptryLeafletInteracting protein 1 (PfCERLI1) in rhoptry function. We show that PfCERLI1 localises to the cytosolic face of the rhoptry bulb membrane and knockdown of PfCERLI1 inhibits merozoite invasion. While schizogony and merozoite organelle biogenesis appear normal, biochemical techniques and semi-quantitative super-resolution microscopy show that PfCERLI1 knockdown prevents secretion of key rhoptry antigens that coordinate merozoite invasion. PfCERLI1 is the first rhoptry associated protein identified to have a direct role in function of this essential malaria invasion organelle which has broader implications for understanding apicomplexan invasion biology.

Published

2019

16. The knob protein KAHRP assembles into a ring-shaped structure that underpins virulence complex assembly

Author

Leann Tilley, Matthew W. A. Dixon, Oliver Looker, Paul J. McMillan, Adam J. Blanch, Boyin Liu, and Juan Nunez-Iglesias

Subjects

Luminescence, Erythrocytes, Polymers, Protozoan Proteins, Spectrins, KAHRP, Biochemistry, chemistry.chemical_compound, Protein structure, Contractile Proteins, Medicine and Health Sciences, Macromolecular Structure Analysis, Electron Microscopy, Malaria, Falciparum, Biology (General), Materials, Cytochalasin D, 0303 health sciences, Microscopy, Virulence, Physics, Electromagnetic Radiation, 030302 biochemistry & molecular biology, Adhesion, 3. Good health, Chemistry, Membrane, Macromolecules, Physical Sciences, Scanning Electron Microscopy, Research Article, Protein Structure, Imaging Techniques, QH301-705.5, Immunology, Materials Science, Plasmodium falciparum, Research and Analysis Methods, Microbiology, Fluorescence, Microbeads, 03 medical and health sciences, Virology, Fluorescence Imaging, parasitic diseases, Genetics, Parasitic Diseases, Humans, Molecular Biology, Actin, 030304 developmental biology, Erythrocyte Membrane, Actin remodeling, Biology and Life Sciences, Proteins, RC581-607, Polymer Chemistry, Actins, Cytoskeletal Proteins, Electron tomography, chemistry, Biophysics, Microscopy, Electron, Scanning, Parasitology, Immunologic diseases. Allergy, Peptides

Abstract

Plasmodium falciparum mediates adhesion of infected red blood cells (RBCs) to blood vessel walls by assembling a multi-protein complex at the RBC surface. This virulence-mediating structure, called the knob, acts as a scaffold for the presentation of the major virulence antigen, P. falciparum Erythrocyte Membrane Protein-1 (PfEMP1). In this work we developed correlative STochastic Optical Reconstruction Microscopy–Scanning Electron Microscopy (STORM-SEM) to spatially and temporally map the delivery of the knob-associated histidine-rich protein (KAHRP) and PfEMP1 to the RBC membrane skeleton. We show that KAHRP is delivered as individual modules that assemble in situ, giving a ring-shaped fluorescence profile around a dimpled disk that can be visualized by SEM. Electron tomography of negatively-stained membranes reveals a previously observed spiral scaffold underpinning the assembled knobs. Truncation of the C-terminal region of KAHRP leads to loss of the ring structures, disruption of the raised disks and aberrant formation of the spiral scaffold, pointing to a critical role for KAHRP in assembling the physical knob structure. We show that host cell actin remodeling plays an important role in assembly of the virulence complex, with cytochalasin D blocking knob assembly. Additionally, PfEMP1 appears to be delivered to the RBC membrane, then inserted laterally into knob structures., Author summary The human malaria parasite Plasmodium falciparum causes severe disease, which is initiated by the adhesion of parasite-infected RBCs to receptors on the walls of the host’s capillaries. Adhesion is mediated by a structure called the knob, which acts as a scaffold for the presentation of the virulence protein, P. falciparum erythrocyte membrane protein-1 (PfEMP1). In this work we investigate the assembly of this complex at different stages of parasite development using a multimodal imaging approach that combines dSTORM localization microscopy and scanning electron microscopy (STORM-SEM). We show that the knob-associated histidine-rich protein (KAHRP) is delivered to the RBC membrane skeleton as individual protein modules that assemble into a ring-shaped complex. We provide evidence that host cell remodeling, driven by association of KAHRP with spectrin and the reorganization of actin, is required for assembly of the ring complex, which in turn supports a spiral scaffold that is required for correct knob morphology. Finally, we provide evidence that PfEMP1 is delivered to the RBC membrane before associating with knob complexes.

Published

2019

17. Decreased K13 Abundance Reduces Hemoglobin Catabolism and Proteotoxic Stress, Underpinning Artemisinin Resistance

Author

Malcolm J. McConville, Madel V Tutor, Matthew W. A. Dixon, Paul J. McMillan, Stuart A. Ralph, Stanley C. Xie, Lee M. Yeoh, David L. Gillett, Tuo Yang, Jessica L. Bridgford, Leann Tilley, Michael F. Duffy, and Simon A. Cobbold

Subjects

0301 basic medicine, medicine.medical_treatment, Cell, Plasmodium falciparum, Dihydroartemisinin, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Hemoglobins, 0302 clinical medicine, parasitic diseases, medicine, Humans, Artemisinin, Malaria, Falciparum, lcsh:QH301-705.5, Mutation, biology, Protein turnover, biology.organism_classification, Artemisinins, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Proteotoxicity, lcsh:Biology (General), Hemoglobin, 030217 neurology & neurosurgery, medicine.drug

Abstract

Summary: Increased tolerance of Plasmodium falciparum to front-line artemisinin antimalarials (ARTs) is associated with mutations in Kelch13 (K13), although the precise role of K13 remains unclear. Here, we show that K13 mutations result in decreased expression of this protein, while mislocalization of K13 mimics resistance-conferring mutations, pinpointing partial loss of function of K13 as the relevant molecular event. K13-GFP is associated with ∼170 nm diameter doughnut-shaped structures at the parasite periphery, consistent with the location and dimensions of cytostomes. Moreover, the hemoglobin-peptide profile of ring-stage parasites is reduced when K13 is mislocalized. We developed a pulse-SILAC approach to quantify protein turnover and observe less disruption to protein turnover following ART exposure when K13 is mislocalized. Our findings suggest that K13 regulates digestive vacuole biogenesis and the uptake/degradation of hemoglobin and that ART resistance is mediated by a decrease in heme-dependent drug activation, less proteotoxicity, and increased survival of parasite ring stages. : Artemisinin resistance in P. falciparum is associated with Kelch13 (K13) mutations. Yang et al. report that K13 is located in cytostome-like structures, consistent with a role in hemoglobin uptake. K13 is less abundant in mutants, and hemoglobin catabolism is impaired. The resultant decrease in artemisinin activation likely underpins artemisinin resistance. Keywords: malaria, artemisinin, antimalarial, kelch13, proteomics, SILAC, protein turnover, cytostome

Published

2019

18. Multimodal analysis of Plasmodium knowlesi ‐infected erythrocytes reveals large invaginations, swelling of the host cell, and rheological defects

Author

Eric Hanssen, Leann Tilley, Adam J. Blanch, Vijay Rajagopal, Matthew W. A. Dixon, Dean Andrew, Olivia M. S. Carmo, Arman Namvar, Snigdha Tiash, and Boyin Liu

Subjects

Cytoplasm, Erythrocytes, Lysis, Plasmodium falciparum, Schizonts, Immunology, Vacuole, Microbiology, Host-Parasite Interactions, Hemoglobins, 03 medical and health sciences, Osmotic Pressure, Virology, Humans, Plasmodium knowlesi, Trophozoites, Research Articles, 030304 developmental biology, 0303 health sciences, biology, Merozoites, 030306 microbiology, Vesicle, Erythrocyte Membrane, biology.organism_classification, 3. Good health, Cell biology, Vacuoles, Host cell cytoplasm, Microscopy, Electron, Scanning, Ultrastructure, Research Article

Abstract

The simian parasite Plasmodium knowlesi causes severe and fatal malaria infections in humans, but the process of host cell remodelling that underpins the pathology of this zoonotic parasite is only poorly understood. We have used serial block‐face scanning electron microscopy to explore the topography of P. knowlesi‐infected red blood cells (RBCs) at different stages of asexual development. The parasite elaborates large flattened cisternae (Sinton Mulligan's clefts) and tubular vesicles in the host cell cytoplasm, as well as parasitophorous vacuole membrane bulges and blebs, and caveolar structures at the RBC membrane. Large invaginations of host RBC cytoplasm are formed early in development, both from classical cytostomal structures and from larger stabilised pores. Although degradation of haemoglobin is observed in multiple disconnected digestive vacuoles, the persistence of large invaginations during development suggests inefficient consumption of the host cell cytoplasm. The parasite eventually occupies ~40% of the host RBC volume, inducing a 20% increase in volume of the host RBC and an 11% decrease in the surface area to volume ratio, which collectively decreases the ability of the P. knowlesi‐infected RBCs to enter small capillaries of a human erythrocyte microchannel analyser. Ektacytometry reveals a markedly decreased deformability, whereas correlative light microscopy/scanning electron microscopy and python‐based skeleton analysis (Skan) reveal modifications to the surface of infected RBCs that underpin these physical changes. We show that P. knowlesi‐infected RBCs are refractory to treatment with sorbitol lysis but are hypersensitive to hypotonic lysis. The observed physical changes in the host RBCs may underpin the pathology observed in patients infected with P. knowlesi.

Published

2019

19. Plasmodium-specific antibodies block in vivo parasite growth without clearing infected red blood cells

Author

Trish Elliott, Pawat Laohamonthonkul, David S. Khoury, Megan S. F. Soon, Arya SheelaNair, Ashraful Haque, Jessica A. Engel, Jasmin Akter, Miles P. Davenport, Ismail Sebina, Clara P. S. Pernold, Lianne I. M. Lansink, Kylie R. James, Bryce S. Thomas, Deborah Cromer, Matthew W. A. Dixon, Rosemary A. Aogo, and Lily Fogg

Subjects

Plasmodium, Erythrocytes, Physiology, Quantitative Parasitology, Complement System, Antibodies, Protozoan, Parasitemia, Biochemistry, Plasmodium chabaudi, Mice, Immune Physiology, Medicine and Health Sciences, lcsh:QH301-705.5, Protozoans, 0303 health sciences, Phagocytes, Immune System Proteins, biology, 030302 biochemistry & molecular biology, Malarial Parasites, Eukaryota, Animal Models, 3. Good health, Body Fluids, medicine.anatomical_structure, Blood, Experimental Organism Systems, Antibody, Anatomy, Plasmodium yoelii, Research Article, lcsh:Immunologic diseases. Allergy, Immunology, Spleen, Mouse Models, Research and Analysis Methods, Microbiology, Antibodies, 03 medical and health sciences, Model Organisms, In vivo, Immunity, Virology, Parasite Groups, parasitic diseases, Genetics, medicine, Parasitic Diseases, Animals, Humans, Parasites, Molecular Biology, 030304 developmental biology, Merozoites, Organisms, Biology and Life Sciences, Proteins, Blood Serum, biology.organism_classification, medicine.disease, Parasitic Protozoans, Malaria, Disease Models, Animal, lcsh:Biology (General), Immune System, Humoral immunity, biology.protein, Animal Studies, Parasitology, lcsh:RC581-607, Immune Serum, Apicomplexa

Abstract

Plasmodium parasites invade and multiply inside red blood cells (RBC). Through a cycle of maturation, asexual replication, rupture and release of multiple infective merozoites, parasitised RBC (pRBC) can reach very high numbers in vivo, a process that correlates with disease severity in humans and experimental animals. Thus, controlling pRBC numbers can prevent or ameliorate malaria. In endemic regions, circulating parasite-specific antibodies associate with immunity to high parasitemia. Although in vitro assays reveal that protective antibodies could control pRBC via multiple mechanisms, in vivo assessment of antibody function remains challenging. Here, we employed two mouse models of antibody-mediated immunity to malaria, P. yoelii 17XNL and P. chabaudi chabaudi AS infection, to study infection-induced, parasite-specific antibody function in vivo. By tracking a single generation of pRBC, we tested the hypothesis that parasite-specific antibodies accelerate pRBC clearance. Though strongly protective against homologous re-challenge, parasite-specific IgG did not alter the rate of pRBC clearance, even in the presence of ongoing, systemic inflammation. Instead, antibodies prevented parasites progressing from one generation of RBC to the next. In vivo depletion studies using clodronate liposomes or cobra venom factor, suggested that optimal antibody function required splenic macrophages and dendritic cells, but not complement C3/C5-mediated killing. Finally, parasite-specific IgG bound poorly to the surface of pRBC, yet strongly to structures likely exposed by the rupture of mature schizonts. Thus, in our models of humoral immunity to malaria, infection-induced antibodies did not accelerate pRBC clearance, and instead co-operated with splenic phagocytes to block subsequent generations of pRBC., Author summary Malaria occurs when Plasmodium parasites replicate inside red blood cells, with the number of parasitised cells (pRBC) correlating with disease severity. Antibodies are highly effective at controlling pRBC numbers in the bloodstream, and yet we know very little about how they function in vivo. Human in vitro studies predict that antibodies may function in a number of ways, including via phagocytes or different complement mechanisms. However, to date it has been challenging to explore how antibodies might control parasite numbers in vivo. Here, we have used a unique method in mice, where clearance and replication of a single cohort of pRBC was closely tracked in the presence of protective antibodies. Surprisingly, antibodies played no role whatsoever in accelerating the removal of pRBC. Instead, antibodies were highly effective at preventing parasites from progressing from one generation of pRBC to the next. This process partly depended on host phagocytes. However, we found no role for complement-mediated direct killing. Together, our in vivo data suggest in mouse models that naturally-acquired antibodies do not clear pRBC, and instead prevent transition from one red blood cell to the next.

Published

2019

20. Surface Area-to-Volume Ratio, not Cellular Viscoelasticity is the Major Determinant of Red Blood Cell Traversal through Small Channels

Author

Peter Vee Sin Lee, Matthew W. A. Dixon, Leann Tilley, Arman Namvar, Boyin Liu, Oliver Looker, Vijay Rajagopal, Olivia M. S. Carmo, Wai-Hong Tham, Snigdha Tiash, Adam J. Blanch, Li-Jin Chan, and Dean Andrew

Subjects

Chemistry, Biophysics, hemic and immune systems, Marked effect, Rbc membrane, Viscoelasticity, Red blood cell, Membrane, medicine.anatomical_structure, Surface-area-to-volume ratio, medicine, Cylinder, circulatory and respiratory physiology

Abstract

The remarkable deformability of red blood cells (RBCs) depends on the viscoelasticity of the plasma membrane and cell contents and the surface area to volume (SA:V) ratio; however, it remains unclear which of these factors is the key determinant for passage through small capillaries. We used a microfluidic device to examine the traversal of normal, stiffened, swollen, parasitised and immature RBCs. We show that dramatic stiffening of RBCs had no measurable effect on their ability to traverse small channels. By contrast, a moderate decrease in the SA:V ratio had a marked effect on the equivalent cylinder diameter that is traversable by RBCs of similar cellular viscoelasticity. We developed a finite element model that provides a coherent rationale for the experimental observations, based on the nonlinear mechanical behaviour of the RBC membrane skeleton. We conclude that the SA:V ratio should be given more prominence in studies of RBC pathologies.

Published

2021

21. Plasmodium species: master renovators of their host cells

Author

Paul R. Gilson, Leann Tilley, Matthew W. A. Dixon, and Tania F. de Koning-Ward

Subjects

0301 basic medicine, Erythrocytes, Plasmodium berghei, Amino Acid Motifs, Plasmodium falciparum, 030106 microbiology, Protozoan Proteins, Protein Sorting Signals, Biology, Microbiology, 03 medical and health sciences, parasitic diseases, medicine, Animals, Humans, Parasite hosting, Malaria, Falciparum, Transport Vesicles, Immune Evasion, General Immunology and Microbiology, Host (biology), medicine.disease, biology.organism_classification, Translocon, Malaria, Transport protein, Cell biology, Protein Transport, 030104 developmental biology, Infectious Diseases, Host-Pathogen Interactions, Protein Translocation Systems, Intracellular

Abstract

Plasmodium parasites, the causative agents of malaria, have developed elaborate strategies that they use to survive and thrive within different intracellular environments. During the blood stage of infection, the parasite is a master renovator of its erythrocyte host cell, and the changes in cell morphology and function that are induced by the parasite promote survival and contribute to the pathogenesis of severe malaria. In this Review, we discuss how Plasmodium parasites use the protein trafficking motif Plasmodium export element (PEXEL), protease-mediated polypeptide processing, a novel translocon termed the Plasmodium translocon of exported proteins (PTEX) and exomembranous structures to export hundreds of proteins to discrete subcellular locations in the host erythrocytes, which enables the parasite to gain access to vital nutrients and to evade the immune defence mechanisms of the host.

Published

2016

22. Reversible host cell remodeling underpins deformability changes in malaria parasite sexual blood stages

Author

Leann Tilley, Oliver Looker, James M. Osborne, Megan K. Dearnley, Trang T. T. Chu, Yao Zhang, Mohit Arora, Rajesh Chandramohanadas, Matthew W. A. Dixon, Changjin Huang, Shannon Kenny, Sulin Zhang, Jeffrey A. Yeoman, and Nectarios Klonis

Subjects

0301 basic medicine, Erythrocytes, Plasmodium falciparum, 030106 microbiology, Microtubules, Models, Biological, 03 medical and health sciences, chemistry.chemical_compound, Erythrocyte Deformability, parasitic diseases, Gametocyte, Erythrocyte deformability, Computer Simulation, Spectrin, Cytoskeleton, Cytochalasin D, Life Cycle Stages, Multidisciplinary, biology, Fluorescence recovery after photobleaching, Biological Sciences, biology.organism_classification, Actin cytoskeleton, Actins, Cell biology, 030104 developmental biology, chemistry, sense organs

Abstract

The sexual blood stage of the human malaria parasite Plasmodium falciparum undergoes remarkable biophysical changes as it prepares for transmission to mosquitoes. During maturation, midstage gametocytes show low deformability and sequester in the bone marrow and spleen cords, thus avoiding clearance during passage through splenic sinuses. Mature gametocytes exhibit increased deformability and reappear in the peripheral circulation, allowing uptake by mosquitoes. Here we define the reversible changes in erythrocyte membrane organization that underpin this biomechanical transformation. Atomic force microscopy reveals that the length of the spectrin cross-members and the size of the skeletal meshwork increase in developing gametocytes, then decrease in mature-stage gametocytes. These changes are accompanied by relocation of actin from the erythrocyte membrane to the Maurer's clefts. Fluorescence recovery after photobleaching reveals reversible changes in the level of coupling between the membrane skeleton and the plasma membrane. Treatment of midstage gametocytes with cytochalasin D decreases the vertical coupling and increases their filterability. A computationally efficient coarse-grained model of the erythrocyte membrane reveals that restructuring and constraining the spectrin meshwork can fully account for the observed changes in deformability.

Published

2016

23. The metabolic repair enzyme phosphoglycolate phosphatase regulates central carbon metabolism and fosmidomycin sensitivity inPlasmodium falciparum

Author

Spencer J. Williams, Malcolm J. McConville, Phillip L. van der Peet, Matthew W. A. Dixon, Mark B. Richardson, Laure Dumont, Simon A. Cobbold, and Leann Tilley

Subjects

biology, Methylglyoxal, Phosphatase, Plasmodium falciparum, Pentose phosphate pathway, biology.organism_classification, Fosmidomycin, chemistry.chemical_compound, chemistry, Biochemistry, medicine, Glycolysis, Methylglyoxal pathway, Phosphoglycolate phosphatase, medicine.drug

Abstract

The asexual blood stages of the malaria parasite,Plasmodium falciparumare highly dependent on glycolysis for ATP synthesis, redox balance and provision of essential anabolic precursors. Recent studies have suggested that members of the haloacid dehalogenase (HAD) family of metabolite phosphatases may play an important role in regulating multiple pathways inP. falciparumcentral carbon metabolism. Here, we show that theP. falciparumHAD protein, phosphoglycolate phosphatase (PfPGP), which is homologous to yeast Pho13 and mammalian PGP, regulates glycolysis in asexual blood stages by controlling intracellular levels of several intermediates and novel end-products of this pathway. Deletion of theP. falciparum pgpgene significantly attenuated asexual parasite growth in red blood cells, while comprehensive metabolomic analysis revealed the accumulation of two previously uncharacterized metabolites, as well as changes in a number of intermediates in glycolysis and the pentose phosphate pathway. The two unknown metabolites were assigned as 2-phospho-lactate and 4-phosphoerythronate by comparison of their mass spectra with synthetic standards. 2-Phospho-lactate was significantly elevated in wildtype and ΔPfPGP parasites cultivated in the presence of methylglyoxal and D-lactate, but not L-lactate, indicating that it is a novel end-product of the methylglyoxal pathway. 4-Phosphoerythronate is a putative side product of the glycolytic enzyme, glyceraldehyde dehydrogenase and the accumulation of both 4-phosphoerythronate and 2-phospho-D-lactate were associated with changes in glycolytic and the pentose phosphate pathway fluxes as shown by13C-glucose labelling studies and increased sensitivity of the ΔPfPGP parasites to the drug fosmidomycin. Our results suggest thatPfPGP contributes to a novel futile metabolic cycle involving the phosphorylation/dephosphorylation of D-lactate as well as detoxification of metabolites, such as 4-phosphoerythronate, and both may have important roles in regulatingP. falciparumcentral carbon metabolism.Author summaryThe major pathogenic stages of the malaria parasite,Plasmodium falciparum, develop in red blood cells where they have access to an abundant supply of glucose. Unsurprisingly these parasite stages are addicted to using glucose, which is catabolized in the glycolytic and the pentose phosphate pathways. While these pathways also exist in host cells, there is increasing evidence thatP. falciparumhas evolved novel ways for regulating glucose metabolism that could be targeted by next-generation of anti-malarial drugs. In this study, we show the red blood cell stages ofP. falciparumexpress an enzyme that is specifically involved in regulating the intracellular levels of two metabolites that are novel end-products or side products of glycolysis. Parasite mutants lacking this enzyme are viable but exhibit diminished growth rates in red blood cells. These mutant lines accumulate the two metabolites, and exhibit global changes in central carbon metabolism. Our findings suggest that metabolic end/side products of glycolysis directly regulate the metabolism of these parasites, and that the intracellular levels of these are tightly controlled by previously uncharacterized metabolite phosphatases.

Published

2018

24. A new Python library to analyse skeleton images confirms malaria parasite remodelling of the red blood cell membrane skeleton

Author

Matthew W. A. Dixon, Leann Tilley, Oliver Looker, Juan Nunez-Iglesias, and Adam J. Blanch

Subjects

0301 basic medicine, Bioinformatics, Skeleton analysis, Computer science, lcsh:Medicine, computer.software_genre, Biochemistry, Computational Science, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Computer graphics (images), Plug-in, Cytoskeleton, computer.programming_language, Application programming interface, General Neuroscience, lcsh:R, General Medicine, Python (programming language), Data structure, Malaria, 3. Good health, Red blood cell, 030104 developmental biology, Parasitology, General Agricultural and Biological Sciences, computer, 030217 neurology & neurosurgery, Python

Abstract

We present Skan (Skeleton analysis), a Python library for the analysis of the skeleton structures of objects. It was inspired by the “analyse skeletons” plugin for the Fiji image analysis software, but its extensive Application Programming Interface (API) allows users to examine and manipulate any intermediate data structures produced during the analysis. Further, its use of common Python data structures such as SciPy sparse matrices and pandas data frames opens the results to analysis within the extensive ecosystem of scientific libraries available in Python. We demonstrate the validity of Skan’s measurements by comparing its output to the established Analyze Skeletons Fiji plugin, and, with a new scanning electron microscopy (SEM)-based method, we confirm that the malaria parasite Plasmodium falciparum remodels the host red blood cell cytoskeleton, increasing the average distance between spectrin-actin junctions.

Published

2018

25. Erythrocyte β spectrin can be genetically targeted to protect mice from malaria

Author

Matthew W. A. Dixon, Hong Ming Huang, Patrick M. Lelliott, Arman Namvar, Adam J. Blanch, Vijay Rajagopal, Cevayir Coban, Gaetan Burgio, Simon J. Foote, Brendan J. McMorran, and Leann Tilley

Subjects

0301 basic medicine, chemistry.chemical_classification, Mutant, Plasmodium falciparum, Hematology, Glycophorin C, Biology, medicine.disease, biology.organism_classification, Cell biology, 03 medical and health sciences, Red blood cell, 030104 developmental biology, 0302 clinical medicine, Immune system, medicine.anatomical_structure, Red Cells, Iron, and Erythropoiesis, chemistry, 030220 oncology & carcinogenesis, parasitic diseases, medicine, Ankyrin, Spectrin, Malaria

Abstract

The malaria parasite hijacks host erythrocytes to shield itself from the immune system and proliferate. Red blood cell abnormalities can provide protection from malaria by impeding parasite invasion and growth within the cell or by compromising the ability of parasites to avoid host clearance. Here, we describe 2 N-ethyl-N-nitrosourea-induced mouse lines, SptbMRI26194 and SptbMRI53426 , containing single-point mutations in the erythrocyte membrane skeleton gene, β spectrin (Sptb), which exhibit microcytosis but retain a relatively normal ratio of erythrocyte surface area to volume and are highly resistant to rodent malaria. We propose the major factor responsible for malaria protection is the specific clearance of mutant erythrocytes, although an enhanced clearance of uninfected mutant erythrocytes was also observed (ie, the bystander effect). Using an in vivo erythrocyte tracking assay, we established that this phenomenon occurs irrespective of host environment, precluding the involvement of nonerythrocytic cells in the resistance mechanism. Furthermore, we recapitulated this phenotype by disrupting the interaction between ankyrin-1 and β spectrin in vivo using CRISPR/Cas9 genome editing technology, thereby genetically validating a potential antimalarial target. This study sheds new light on the role of β spectrin during Plasmodium infection and highlights how changes in the erythrocyte cytoskeleton can substantially influence malaria susceptibility with minimal adverse consequences for the host.

Published

2017

26. A repeat sequence domain of the ring-exported protein-1 ofPlasmodium falciparumcontrols export machinery architecture and virulence protein trafficking

Author

Matthew W. A. Dixon, Katharine R. Trenholme, Emma McHugh, Paul J. McMillan, Steven Batinovic, Michael D. W. Griffin, Eric Hanssen, Simon Crawford, Leann Tilley, Donald L. Gardiner, and Shannon Kenny

Subjects

Mutation, biology, Virulence, Plasmodium falciparum, KAHRP, biology.organism_classification, medicine.disease_cause, Microbiology, Transport protein, Cell biology, Red blood cell, Protein structure, medicine.anatomical_structure, parasitic diseases, Organelle, medicine, Molecular Biology

Abstract

The malaria parasite Plasmodium falciparum dramatically remodels its host red blood cell to enhance its own survival, using a secretory membrane system that it establishes outside its own cell. Cisternal organelles, called Maurer's clefts, act as a staging point for the forward trafficking of virulence proteins to the red blood cell (RBC) membrane. The Ring-EXported Protein-1 (REX1) is a Maurer's cleft resident protein. We show that inducible knockdown of REX1 causes stacking of Maurer's cleft cisternae without disrupting the organization of the knob-associated histidine-rich protein at the RBC membrane. Genetic dissection of the REX1 sequence shows that loss of a repeat sequence domain results in the formation of giant Maurer's cleft stacks. The stacked Maurer's clefts are decorated with tether-like structures and retain the ability to dock onto the RBC membrane skeleton. The REX1 mutant parasites show deficient export of the major virulence protein, PfEMP1, to the red blood cell surface and markedly reduced binding to the endothelial cell receptor, CD36. REX1 is predicted to form a largely α-helical structure, with a repetitive charge pattern in the repeat sequence domain, providing potential insights into the role of REX1 in Maurer's cleft sculpting.

Published

2015

27. Disrupting assembly of the inner membrane complex blocks Plasmodium falciparum sexual stage development

Author

Eric Hanssen, Dean Andrew, Annika Suttie, Emma McHugh, Boyin Liu, Matthew W. A. Dixon, Marion Hliscs, Steven Batinovic, Molly Parkyn Schneider, Nicholas A. Williamson, Paul J. McMillan, Philipp Glock, and Leann Tilley

Subjects

0301 basic medicine, Plasmodium, Cell Membranes, Vacuole, Gametocytes, Microtubules, Fluorescence Microscopy, Animal Cells, Biology (General), Cytoskeleton, Microscopy, biology, Sexual Development, Light Microscopy, 3. Good health, Transport protein, Cell biology, Protein Transport, Cellular Types, Cellular Structures and Organelles, Research Article, Immunofluorescence Microscopy, QH301-705.5, Plasmodium falciparum, 030106 microbiology, Immunology, Research and Analysis Methods, Microbiology, 03 medical and health sciences, Microtubule, Virology, Parasite Groups, Genetics, Gametocyte, Animals, Molecular Biology, Inner membrane complex, Biology and Life Sciences, Membrane Proteins, Cell Biology, RC581-607, biology.organism_classification, Microscopy, Electron, Germ Cells, 030104 developmental biology, Membrane protein, Vacuoles, Parasitology, Immunologic diseases. Allergy, Apicomplexa

Abstract

Transmission of malaria parasites relies on the formation of a specialized blood form called the gametocyte. Gametocytes of the human pathogen, Plasmodium falciparum, adopt a crescent shape. Their dramatic morphogenesis is driven by the assembly of a network of microtubules and an underpinning inner membrane complex (IMC). Using super-resolution optical and electron microscopies we define the ultrastructure of the IMC at different stages of gametocyte development. We characterize two new proteins of the gametocyte IMC, called PhIL1 and PIP1. Genetic disruption of PhIL1 or PIP1 ablates elongation and prevents formation of transmission-ready mature gametocytes. The maturation defect is accompanied by failure to form an enveloping IMC and a marked swelling of the digestive vacuole, suggesting PhIL1 and PIP1 are required for correct membrane trafficking. Using immunoprecipitation and mass spectrometry we reveal that PhIL1 interacts with known and new components of the gametocyte IMC., Author summary Transmission of the malaria parasite from humans to mosquitoes relies on the formation of the specialised blood stage gametocyte. Plasmodium falciparum gametocytes mature over about 10 days, during which time they undergo a remarkable morphological transformation, eventually adopting a characteristic crescent shape. The shape changes are thought to facilitate the mechanical sequestration of maturing gametocytes within the bone marrow and spleen, as well as the eventual release into the circulation. Failure to mature correctly leads to a failure to transmit. Despite the importance of this process, little is known about the molecular basis of elongation. In this work, we introduce 3D Electron Microscopy of P. falciparum gametocytes and use it, in a combination with super-resolution optical microscopy, to elucidate the genesis and expansion of the molecular structures that drive gametocyte elongation. We use protein interaction profiling to identify some of the proteins that help drive the shape change and employ inducible gene knockdown strategies to show that these proteins play a role in remodeling membranes, and are needed for gametocyte elongation. This work points to potential targets for the development of transmission-blocking therapies.

Published

2017

28. An exported protein-interacting complex involved in the trafficking of virulence determinants in Plasmodium-infected erythrocytes

Author

Molly Parkyn Schneider, Laure Dumont, Scott A. Chisholm, Emma McHugh, Paul R. Gilson, Steven Batinovic, Tania F. de Koning-Ward, Sarah C. Charnaud, Matthew W. A. Dixon, Boiyin Liu, Leann Tilley, and Kathryn Matthews

Subjects

0301 basic medicine, Plasmodium berghei, Science, Plasmodium falciparum, Protozoan Proteins, General Physics and Astronomy, Virulence, Bioinformatics, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, parasitic diseases, Cell Adhesion, Antigenic variation, Animals, Multidisciplinary, 030102 biochemistry & molecular biology, biology, Membrane Proteins, General Chemistry, biology.organism_classification, Translocon, Transport protein, Cell biology, Mice, Inbred C57BL, Protein Transport, 030104 developmental biology, Membrane protein, Cytoplasm, Gene Knockdown Techniques, Host-Pathogen Interactions, Female, Carrier Proteins

Abstract

The malaria parasite, Plasmodium falciparum, displays the P. falciparum erythrocyte membrane protein 1 (PfEMP1) on the surface of infected red blood cells (RBCs). We here examine the physical organization of PfEMP1 trafficking intermediates in infected RBCs and determine interacting partners using an epitope-tagged minimal construct (PfEMP1B). We show that parasitophorous vacuole (PV)-located PfEMP1B interacts with components of the PTEX (Plasmodium Translocon of EXported proteins) as well as a novel protein complex, EPIC (Exported Protein-Interacting Complex). Within the RBC cytoplasm PfEMP1B interacts with components of the Maurer’s clefts and the RBC chaperonin complex. We define the EPIC interactome and, using an inducible knockdown approach, show that depletion of one of its components, the parasitophorous vacuolar protein-1 (PV1), results in altered knob morphology, reduced cell rigidity and decreased binding to CD36. Accordingly, we show that deletion of the Plasmodium berghei homologue of PV1 is associated with attenuation of parasite virulence in vivo., Plasmodium-infected red blood cells export virulence factors, such as PfEMP1, to the cell surface. Here, the authors identify a protein complex termed EPIC that interacts with PfEMP1 during export, and they show that knockdown of an EPIC component affects parasite virulence.

Published

2017

29. Ankyrin-1 gene exhibits allelic heterogeneity in conferring protection against malaria

Author

Leann Tilley, Brendan J. McMorran, Denis C. Bauer, Gaetan Burgio, Patrick M. Lelliott, Simon J. Foote, Matthew W. A. Dixon, and Hong Ming Huang

Subjects

Male, 0301 basic medicine, Erythrocytes, Erythrocyte clearance, erythrocyte cytoskeleton, QH426-470, medicine.disease_cause, Plasmodium chabaudi, Mice, 0302 clinical medicine, ankyrin-1, Genetics (clinical), Disease Resistance, Genetics, 0303 health sciences, education.field_of_study, Mutation, Phenotype, 3. Good health, Female, Allelic heterogeneity, Ankyrins, Population, malaria, Mutagenesis (molecular biology technique), Spherocytosis, Hereditary, Investigations, Biology, Host-Parasite Interactions, Genetic Heterogeneity, 03 medical and health sciences, medicine, Animals, Genetic Predisposition to Disease, Allele, education, Molecular Biology, Gene, Alleles, 030304 developmental biology, Whole Genome Sequencing, Genetic heterogeneity, allelic heterogeneity, biology.organism_classification, Disease Models, Animal, Osmotic Fragility, 030104 developmental biology, 030215 immunology

Abstract

Allelic heterogeneity is a common phenomenon where a gene exhibit different phenotype depending on the nature of its genetic mutations. In the context of genes affecting malaria susceptibility, it allowed us to explore and understand the intricate host-parasite interactions during malaria infections. In this study, we described a gene encoding erythrocytic ankyrin-1 (Ank-1) which exhibits allelic-dependent heterogeneous phenotypes during malaria infections. We conducted an ENU mutagenesis screen on mice and identified twoAnk-1mutations, one resulted in an amino acid substitution (MRI95845), and the other a truncatedAnk-1protein (MRI96570). Both mutations caused hereditary spherocytosis-like phenotypes and confer differing protection againstPlasmodium chabaudiinfections. Upon further examination, theAnk-1(MRI96570)mutation was found to inhibit intra-erythrocytic parasite maturation, whereasAnk-1(MW95845)caused increased bystander erythrocyte clearance during infection. This is the first description of allelic heterogeneity in ankyrin-1 from the direct comparison between twoAnk-1mutations. Despite the lack of direct evidence from population studies, this data further supported the protective roles of ankyrin-1 mutations in conferring malaria protection. This study also emphasized the importance of such phenomenon to achieve a better understanding of host-parasite interactions, which could be the basis of future studies.

Published

2017

30. The exported chaperone Hsp70-x supports virulence functions for Plasmodium falciparum blood stage parasites

Author

Eric Hanssen, Brendan S. Crabb, Leann Tilley, Catherine Q Nie, Sarah C. Charnaud, Adam J. Blanch, Matthew Berriman, Lia Chappell, Jo-Anne Chan, Thomas Nebl, Julian C. Rayner, Paul R. Gilson, James G. Beeson, Jude M. Przyborski, Matthew W. A. Dixon, and Paul R Sanders

Subjects

0301 basic medicine, Proteomics, Life Cycles, Plasmodium, Cell, Protozoan Proteins, lcsh:Medicine, Biochemistry, Parasitic Cell Cycles, Animal Cells, Red Blood Cells, Medicine and Health Sciences, Malaria, Falciparum, lcsh:Science, Multidisciplinary, Spectrometric Identification of Proteins, biology, Virulence, Stable Isotope Labeling by Amino Acids in Cell Culture, 3. Good health, medicine.anatomical_structure, Cellular Types, Research Article, Parasitic Life Cycles, Plasmodium falciparum, Research and Analysis Methods, Microbiology, 03 medical and health sciences, Parasite Groups, parasitic diseases, medicine, Parasitic Diseases, Cell Adhesion, Animals, HSP70 Heat-Shock Proteins, Parasites, Trophozoites, Cell adhesion, Molecular Biology Techniques, Molecular Biology, Blood Cells, 030102 biochemistry & molecular biology, Erythrocyte Membrane, lcsh:R, Biology and Life Sciences, Proteins, Endothelial Cells, Cell Biology, medicine.disease, biology.organism_classification, In vitro, Hsp70, Chaperone Proteins, 030104 developmental biology, Chaperone (protein), biology.protein, Parasitology, lcsh:Q, Apicomplexa, Malaria, Developmental Biology, Cloning, Molecular Chaperones

Abstract

Malaria is caused by five different Plasmodium spp. in humans each of which modifies the host erythrocyte to survive and replicate. The two main causes of malaria, P. falciparum and P. vivax, differ in their ability to cause severe disease, mainly due to differences in the cytoadhesion of infected erythrocytes (IE) in the microvasculature. Cytoadhesion of P. falciparum in the brain leads to a large number of deaths each year and is a consequence of exported parasite proteins, some of which modify the erythrocyte cytoskeleton while others such as PfEMP1 project onto the erythrocyte surface where they bind to endothelial cells. Here we investigate the effects of knocking out an exported Hsp70-type chaperone termed Hsp70-x that is present in P. falciparum but not P. vivax. Although the growth of Δhsp70-x parasites was unaffected, the export of PfEMP1 cytoadherence proteins was delayed and Δhsp70-x IE had reduced adhesion. The Δhsp70-x IE were also more rigid than wild-type controls indicating changes in the way the parasites modified their host erythrocyte. To investigate the cause of this, transcriptional and translational changes in exported and chaperone proteins were monitored and some changes were observed. We propose that PfHsp70-x is not essential for survival in vitro, but may be required for the efficient export and functioning of some P. falciparum exported proteins.

Published

2017

31. Organization and function of an actin cytoskeleton inPlasmodium falciparumgametocytes

Author

Coralie Ode Millet, Marion Hliscs, Inga Siden-Kiamos, Matthew W. A. Dixon, Paul J. McMillan, and Leann Tilley

Subjects

biology, Immunology, Actin remodeling, Arp2/3 complex, macromolecular substances, Actin cytoskeleton, Microbiology, Filamentous actin, Cell biology, Profilin, Virology, Formins, Gametocyte, biology.protein, Cytoskeleton

Abstract

In preparation for transmission to its mosquito vector, Plasmodium falciparum, the most virulent of the human malaria parasites, adopts an unusual elongated shape. Here we describe a previously unrecognized actin-based cytoskeleton that is assembled in maturing P. falciparum gametocytes. Differential extraction reveals the presence of a highly stabilized population of F-actin at all stages of development. Super-resolution microscopy reveals an F-actin cytoskeleton that is concentrated at the ends of the elongating gametocyte but extends inward along the microtubule cytoskeleton. Formin-1 is also concentrated at the gametocyte ends suggesting a role in actin stabilization. Immunoelectron microscopy confirms that the actin cytoskeleton is located under the inner membrane complex rather than in the sub-alveolar space. In stage V gametocytes, the actin and microtubule cytoskeletons are reorganized in a coordinated fashion. The actin-depolymerizing agent, cytochalasin D, depletes actin from the end of the gametocytes, whereas the actin-stabilizing compound, jasplakinolide, induces formation of large bundles and prevents late-stage disassembly of the actin cytoskeleton. Long-term treatment with these compounds is associated with disruption of the normal mitochondrial organization and decreased gametocyte viability.

Published

2014

32. Red Blood Cells Polarize Green Laser Light Revealing Hemoglobin's Enhanced Non-Fundamental Raman Modes

Author

Malgorzata Baranska, Matthew W. A. Dixon, Leann Tilley, Donald McNaughton, David Perez-Guaita, Bayden R. Wood, Marleen de Veij, and Katarzyna M. Marzec

Subjects

Erythrocytes, Overtone, Plasmodium falciparum, Analytical chemistry, porphyrinoids, malaria diagnostic, Heme, Spectrum Analysis, Raman, Molecular physics, Spectral line, law.invention, chemistry.chemical_compound, symbols.namesake, Hemoglobins, law, Humans, Physical and Theoretical Chemistry, Malaria, Falciparum, Spectroscopy, Scattering, Lasers, Articles, Laser, Polarization (waves), Atomic and Molecular Physics, and Optics, chemistry, Raman spectroscopy, symbols, overtone/combination modes, red blood cells

Abstract

In general, the first overtone modes produce weak bands that appear at approximately twice the wavenumber value of the fundamental transitions in vibrational spectra. Here, we report the existence of a series of enhanced non-fundamental bands in resonance Raman (RR) spectra recorded for hemoglobin (Hb) inside the highly concentrated heme environment of the red blood cell (RBC) by exciting with a 514.5 nm laser line. Such bands are most intense when detecting parallel-polarized light. The enhancement is explained through excitonic theory invoking a type C scattering mechanism and bands have been assigned to overtone and combination bands based on symmetry arguments and polarization measurements. By using malaria diagnosis as an example, we demonstrate that combining the non-fundamental and fundamental regions of the RR spectrum improves the sensitivity and diagnostic capability of the technique. The discovery will have considerable implications for the ongoing development of Raman spectroscopy for blood disease diagnoses and monitoring heme perturbation in response to environmental stimuli.

Published

2014

33. Diagnosing malaria infected cells at the single cell level using focal plane array Fourier transform infrared imaging spectroscopy

Author

Eric C. Mattson, Keith R. Bambery, Leann Tilley, Matthew W. A. Dixon, Carol J. Hirschmugl, Michael J. Nasse, and Bayden R. Wood

Subjects

Photomicrography, Erythrocytes, Microscope, Plasmodium falciparum, Analytical chemistry, Image processing, Tissue Array Analysis, Biochemistry, Analytical Chemistry, law.invention, Optics, law, Spectroscopy, Fourier Transform Infrared, Image Processing, Computer-Assisted, Electrochemistry, Humans, Environmental Chemistry, Spectroscopy, Principal Component Analysis, business.industry, Synchrotron light source, Malaria, Imaging spectroscopy, Cardinal point, Deconvolution, Single-Cell Analysis, Molecular imaging, business

Abstract

New methods are needed to rapidly identify malaria parasites in blood smears. The coupling of a Focal Plane Array (FPA) infrared microscope system to a synchrotron light source at IRENI enables rapid molecular imaging at high spatial resolution. The technique, in combination with hyper-spectral processing, enables imaging and diagnosis of early stage malaria parasites at the single cell level in a blood smear. The method relies on the detection of distinct lipid signatures associated with the different stages of the malaria parasite and utilises resonant Mie extended multiplicative scatter correction to pre-process the spectra followed by full bandwidth image deconvolution to resolve the single cells. This work demonstrates the potential of focal plane technology to diagnose single cells in a blood smear. Brighter laboratory based infrared sources, optical refinements and higher sensitive detectors will soon see the emergence of focal plane array imaging in the clinical environment.

Published

2014

34. ThePlasmodiumtranslocon of exported proteins (PTEX) component thioredoxin-2 is important for maintaining normal blood-stage growth

Author

Silvia Haase, Thomas Nebl, Christopher D. Goodman, Fiona W. Fraser, Scott A. Chisholm, Angelika Sturm, Matthew W. A. Dixon, Paul R Sanders, Tania F. de Koning-Ward, Kathryn Matthews, Geoffrey I. McFadden, Paul R. Gilson, Brendan S. Crabb, and Ming Kalanon

Subjects

Genetics, Host cell cytosol, biology, Plasmodium berghei, Transfection, Thioredoxin, biology.organism_classification, Translocon, Molecular Biology, Microbiology, Plasmodium, Phenotype, Function (biology)

Abstract

Summary Plasmodium parasites remodel their vertebrate host cells by translocating hundreds of proteins across an encasing membrane into the host cell cytosol via a putative export machinery termed PTEX. Previously PTEX150, HSP101 and EXP2 have been shown to be bona fide members of PTEX. Here we validate that PTEX88 and TRX2 are also genuine members of PTEX and provide evidence that expression of PTEX components are also expressed in early gametocytes, mosquito and liver stages, consistent with observations that protein export is not restricted to asexual stages. Although amenable to genetic tagging, HSP101, PTEX150, EXP2 and PTEX88 could not be genetically deleted in Plasmodium berghei, in keeping with the obligatory role this complex is postulated to have in maintaining normal blood-stage growth. In contrast, the putative thioredoxin-like protein TRX2 could be deleted, with knockout parasites displaying reduced grow-rates, both in vivo and in vitro, and reduced capacity to cause severe disease in a cerebral malaria model. Thus, while not essential for parasite survival, TRX2 may help to optimize PTEX activity. Importantly, the generation of TRX2 knockout parasites that display altered phenotypes provides a much-needed tool to dissect PTEX function.

Published

2013

35. Spatial and temporal mapping of the PfEMP1 export pathway inPlasmodium falciparum

Author

David A. Fidock, Eric Hanssen, Rebecca A. Muhle, Shannon Kenny, Joseph D. Smith, Matthew W. A. Dixon, Steven Batinovic, Coralie Ode Millet, Martin Melcher, Mauro Maiorca, Leann Tilley, and Paul J. McMillan

Subjects

Host cell cytosol, biology, Vesicle, Immunology, Plasmodium falciparum, Transfection, biology.organism_classification, Microbiology, Transport protein, Green fluorescent protein, Cell biology, chemistry.chemical_compound, chemistry, Virology, parasitic diseases, Ultrastructure, Cytochalasin D

Abstract

The human malaria parasite, Plasmodium falciparum, modifies the red blood cells (RBCs) that it infects by exporting proteins to the host cell. One key virulence protein, P. falciparum Erythrocyte Membrane Protein-1 (PfEMP1), is trafficked to the surface of the infected RBC, where it mediates adhesion to the vascular endothelium. We have investigated the organization and development of the exomembrane system that is used for PfEMP1 trafficking. Maurer's cleft cisternae are formed early after invasion and proteins are delivered to these (initially mobile) structures in a temporally staggered and spatially segregated manner. Membrane-Associated Histidine-Rich Protein-2 (MAHRP2)-containing tether-like structures are generated as early as 4 h post invasion and become attached to Maurer's clefts. The tether/Maurer's cleft complex docks onto the RBC membrane at ~20 h post invasion via a process that is not affected by cytochalasin D treatment. We have examined the trafficking of a GFP chimera of PfEMP1 expressed in transfected parasites. PfEMP1B-GFP accumulates near the parasite surface, within membranous structures exhibiting a defined ultrastructure, before being transferred to pre-formed mobile Maurer's clefts. Endogenous PfEMP1 and PfEMP1B-GFP are associated with Electron-Dense Vesicles that may be responsible for trafficking PfEMP1 from the Maurer's clefts to the RBC membrane.

Published

2013

36. A Plasmodium falciparum S33 proline aminopeptidase is associated with changes in erythrocyte deformability

Author

Colin M. Stack, Fabio L. da Silva, Malcolm K. Jones, Erica Lovas, Tina S. Skinner-Adams, Donald L. Gardiner, Elena Taran, John P. Dalton, Franka Teuscher, Christopher L. Brown, Matthew W. A. Dixon, Katharine R. Trenholme, and Leann Tilley

Subjects

0301 basic medicine, Erythrocytes, 030106 microbiology, Immunology, Blotting, Western, Plasmodium falciparum, Antibodies, Protozoan, Biology, Microscopy, Atomic Force, Real-Time Polymerase Chain Reaction, Transfection, Aminopeptidases, 03 medical and health sciences, Gene Knockout Techniques, Microscopy, Electron, Transmission, Erythrocyte Deformability, parasitic diseases, medicine, Cell Adhesion, Erythrocyte deformability, Humans, Amino Acid Sequence, Cell adhesion, Receptor, Erythrocyte Membrane, General Medicine, Exopeptidase, biology.organism_classification, Blotting, Northern, Elasticity, Recombinant Proteins, Endothelial stem cell, Red blood cell, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Biochemistry, Microscopy, Fluorescence, Proline aminopeptidase, biology.protein, Parasitology, Sequence Alignment, RNA, Protozoan

Abstract

Infection with the apicomplexan parasite Plasmodium falciparum is a major cause of morbidity and mortality worldwide. One of the striking features of this parasite is its ability to remodel and decrease the deformability of host red blood cells, a process that contributes to disease. To further understand the virulence of Pf we investigated the biochemistry and function of a putative Pf S33 proline aminopeptidase (PfPAP). Unlike other P. falciparum aminopeptidases, PfPAP contains a predicted protein export element that is non-syntenic with other human infecting Plasmodium species. Characterization of PfPAP demonstrated that it is exported into the host red blood cell and that it is a prolyl aminopeptidase with a preference for N-terminal proline substrates. In addition genetic deletion of this exopeptidase was shown to lead to an increase in the deformability of parasite-infected red cells and in reduced adherence to the endothelial cell receptor CD36 under flow conditions. Our studies suggest that PfPAP plays a role in the rigidification and adhesion of infected red blood cells to endothelial surface receptors, a role that may make this protein a novel target for anti-disease interventions strategies.

Published

2016

37. Contrasting Inducible Knockdown of the Auxiliary PTEX Component PTEX88 in P. falciparum and P. berghei Unmasks a Role in Parasite Virulence

Author

Leann Tilley, Sreejoyee Ghosh, Matthew W. A. Dixon, Rachel J. Lundie, Meredith O’Keefe, Scott A. Chisholm, Ming Kalanon, Tania F. de Koning-Ward, and Emma McHugh

Subjects

CD36 Antigens, 0301 basic medicine, Plasmodium, Life Cycles, Physiology, Quantitative Parasitology, Plasmodium berghei, CD36, Protozoan Proteins, lcsh:Medicine, Plasma protein binding, Parasitemia, Parasitic Cell Cycles, Animal Cells, Red Blood Cells, Immune Physiology, Medicine and Health Sciences, lcsh:Science, Protozoans, Glucosamine, Gene knockdown, Multidisciplinary, Virulence, biology, Malarial Parasites, Translocon, 3. Good health, Transport protein, Cell biology, Protein Transport, Gene Knockdown Techniques, Female, Cellular Types, Research Article, Protein Binding, Parasitic Life Cycles, Plasmodium falciparum, 03 medical and health sciences, Parasite Groups, parasitic diseases, Parasitic Diseases, Cell Adhesion, Animals, Parasites, Inflammation, Parasitic life cycles, Blood Cells, lcsh:R, Organisms, Immunity, Biology and Life Sciences, Cell Biology, biology.organism_classification, Virology, Parasitic Protozoans, Mice, Inbred C57BL, 030104 developmental biology, biology.protein, Parasitology, lcsh:Q, Apicomplexa, Spleen, Developmental Biology

Abstract

Pathogenesis of malaria infections is linked to remodeling of erythrocytes, a process dependent on the trafficking of hundreds of parasite-derived proteins into the host erythrocyte. Recent studies have demonstrated that the Plasmodium translocon of exported proteins (PTEX) serves as the central gateway for trafficking of these proteins, as inducible knockdown of the core PTEX constituents blocked the trafficking of all classes of cargo into the erythrocyte. However, the role of the auxiliary component PTEX88 in protein export remains less clear. Here we have used inducible knockdown technologies in P. falciparum and P. berghei to assess the role of PTEX88 in parasite development and protein export, which reveal that the in vivo growth of PTEX88-deficient parasites is hindered. Interestingly, we were unable to link this observation to a general defect in export of a variety of known parasite proteins, suggesting that PTEX88 functions in a different fashion to the core PTEX components. Strikingly, PTEX88-deficient P. berghei were incapable of causing cerebral malaria despite a robust pro-inflammatory response from the host. These parasites also exhibited a reduced ability to sequester in peripheral tissues and were removed more readily from the circulation by the spleen. In keeping with these findings, PTEX88-deficient P. falciparum-infected erythrocytes displayed reduced binding to the endothelial cell receptor, CD36. This suggests that PTEX88 likely plays a specific direct or indirect role in mediating parasite sequestration rather than making a universal contribution to the trafficking of all exported proteins.

Published

2016

38. Shape-shifting gametocytes: how and why does P. falciparum go banana-shaped?

Author

Megan K. Dearnley, Matthew W. A. Dixon, Leann Tilley, Tim W. Gilberger, and Eric Hanssen

Subjects

Life Cycle Stages, Inner membrane complex, biology, Cell Membrane, Plasmodium falciparum, biology.organism_classification, medicine.disease, Virology, Culicidae, Infectious Diseases, parasitic diseases, medicine, Gametocyte, Animals, Humans, Parasitology, Infected erythrocyte, Blood stream, Spleen, Malaria

Abstract

Plasmodium falciparum is named for the crescent or falciform shape it adopts when preparing to undergo transfer to a mosquito vector. By contrast, gametocytes of the other (less virulent) human malaria parasites retain a more rounded shape. We describe the machinery that elongates falciparum gametocytes and discuss its relation with the machinery that elongates the invasive zoites. We address the question - why do falciparum malaria gametocytes go banana-shaped? The answer may lie in the finding that gametocyte maturation is associated with an increase in cellular deformability. The shape-shifting ability of gametocytes may facilitate the sequestration of early-stage gametocytes, while enabling late-stage gametocytes to circulate in the blood stream without being removed by the mechanical filtering mechanisms in the host spleen.

Published

2012

39. Genetic ablation of a Maurer's cleft protein prevents assembly of the Plasmodium falciparum virulence complex

Author

Eric Hanssen, Donald L. Gardiner, Katharine R. Trenholme, Leann Tilley, Paul J. McMillan, Matthew W. A. Dixon, and Shannon Kenny

Subjects

biology, Virulence, Plasmodium falciparum, Maurer's cleft, KAHRP, biology.organism_classification, Microbiology, Molecular biology, Transport protein, Green fluorescent protein, Membrane protein, parasitic diseases, Antigenic variation, Molecular Biology

Abstract

The malaria parasite Plasmodium falciparum assembles knob structures underneath the erythrocyte membrane that help present the major virulence protein, P. falciparum erythrocyte membrane protein-1 (PfEMP1). Membranous structures called Maurer's clefts are established in the erythrocyte cytoplasm and function as sorting compartments for proteins en route to the RBC membrane, including the knob-associated histidine-rich protein (KAHRP), and PfEMP1. We have generated mutants in which the Maurer's cleft protein, the ring exported protein-1 (REX1) is truncated or deleted. Removal of the C-terminal domain of REX1 compromises Maurer's cleft architecture and PfEMP1-mediated cytoadherance but permits some trafficking of PfEMP1 to the erythrocyte surface. Deletion of the coiled-coil region of REX1 ablates PfEMP1 surface display, trapping PfEMP1 at the Maurer's clefts. Complementation of mutants with REX1 partly restores PfEMP1-mediated binding to the endothelial cell ligand, CD36. Deletion of the coiled-coil region or complete deletion of REX1 is tightly associated with the loss of a subtelomeric region of chromosome 2, encoding KAHRP and other proteins. A KAHRP-green fluorescent protein (GFP) fusion expressed in the REX1-deletion parasites shows defective trafficking. Thus, loss of functional REX1 directly or indirectly ablates the assembly of the P. falciparum virulence complex at the surface of host erythrocytes.

Published

2011

40. The Plasmodium falciparum-infected red blood cell

Author

Leann Tilley, Kiaran Kirk, and Matthew W. A. Dixon

Subjects

Erythrocytes, Plasmodium falciparum, Drug Resistance, Antigens, Protozoan, Biochemistry, Antimalarials, parasitic diseases, Cell Adhesion, medicine, Gametocyte, Animals, Humans, Malaria, Falciparum, Life Cycle Stages, biology, Malaria vaccine, Anopheles, Cell Biology, medicine.disease, biology.organism_classification, Antigenic Variation, Virology, Bacterial adhesin, Red blood cell, medicine.anatomical_structure, Host cell cytoplasm, Endothelium, Vascular, Malaria

Abstract

Plasmodium falciparum, the most virulent of the human malaria parasites, causes up to one million deaths per year. The parasite spends part of its lifecycle inside the red blood cells (RBCs) of its host. As it grows it ingests the RBC cytoplasm, digesting it in an acidic vacuole. Free haem released during haemoglobin digestion is detoxified by conversion to inert crystals of haemozoin. Malaria pathology is evident during the blood stage of the infection and is exacerbated by adhesion of infected RBCs to blood vessel walls, which prevents splenic clearance of the infected cells. Cytoadherence is mediated by surface-exposed virulence proteins that bind to endothelial cell receptors. These 'adhesins' are exported to the RBC surface via an exomembrane system that is established outside the parasite in the host cell cytoplasm. Antimalarial drugs that interfere with haem detoxification, or target other parasite-specific processes, have been effective in the treatment of malaria, but their use has been dogged by the development of resistance. Similarly, efforts to develop an effective blood vaccine are hindered by the variability of surface-exposed antigens.

Published

2011

41. Effect of Antimalarial Drugs onPlasmodium falciparumGametocytes

Author

Christopher L. Peatey, James S. McCarthy, Matthew W. A. Dixon, Katharine R. Trenholme, Donald L. Gardiner, and Tina S. Skinner-Adams

Subjects

Male, biology, Plasmodium falciparum, biology.organism_classification, medicine.disease, Virology, Genetically modified organism, Animals, Genetically Modified, Apicomplexa, Antimalarials, Infectious Diseases, Parasitic Sensitivity Tests, In vivo, parasitic diseases, medicine, Gametocyte, Animals, Immunology and Allergy, Parasite hosting, Protozoa, Female, Malaria

Abstract

Gametocytes are the sexual stage of the malaria parasite and are essential for transmission to the mosquito. Antimalarial drugs have been reported to affect gametocyte production in vivo, which leads to a potential increase in transmission. We used transgenic Plasmodium falciparum parasites expressing a green fluorescent protein tag in a fluorescence-activated cell sorting-based assay to measure the effect of 8 antimalarial drugs on gametocyte production in vitro. Exposure to antimalarial drugs resulted in an increase in the number of gametocytes in test cultures. Although a dose-dependent reduction in late-stage gametocyte viability was observed, none of the drugs tested statistically significantly reduced gametocyte numbers.

Published

2009

42. Targeting of the Ring Exported Protein 1 to the Maurers Clefts is Mediated by a Two-Phase Process

Author

Donald L. Gardiner, Katharine R. Trenholme, Karen Anderson, Tobias Spielmann, Matthew W. A. Dixon, and Paula L. Hawthorne

Subjects

Erythrocytes, Transgene, Green Fluorescent Proteins, Plasmodium falciparum, Protozoan Proteins, Protein Export, Transfection, Models, Biological, Biochemistry, Animals, Genetically Modified, Cytosol, Structural Biology, parasitic diseases, Genetics, Animals, Molecular Biology, DNA Primers, chemistry.chemical_classification, biology, Cell Biology, biology.organism_classification, Amino acid, Transport protein, Cell biology, Protein Transport, Microscopy, Fluorescence, chemistry, Vacuolar transport, Vacuoles

Abstract

Early development of Plasmodium falciparum within the erythrocyte is characterized by the large-scale export of proteins to the host cell. In many cases, export is mediated by a short sequence called the Plasmodium export element (PEXEL) or vacuolar transport signal; however, a number of previously characterized exported proteins do not contain such an element. In this study, we investigated the mechanisms of export of the PEXEL-negative ring exported protein 1 (REX1). This protein localizes to the Maurer's clefts, parasite-induced structures in the host-cell cytosol. Transgenic parasites expressing green fluorescent protein-REX1 chimeras revealed that the single hydrophobic stretch plus an additional 10 amino acids mediate the export of REX1. Biochemical characterization of these chimeras indicated that REX1 was exported as a soluble protein. Inclusion of a sequence containing a predicted coiled-coil motif led to the correct localization of REX1 at the Maurer's clefts, suggesting that association with the clefts occurs at the final stage of protein export only. These results indicate that PEXEL-negative exported proteins can be exported in a soluble state and that sequences without any apparent resemblance to a PEXEL motif can mediate export across the parasitophorous vacuole membrane.

Published

2008

43. Sex in Plasmodium: a sign of commitment

Author

Donald L. Gardiner, Matthew W. A. Dixon, Katharine R. Trenholme, and Joanne Thompson

Subjects

Male, Plasmodium, Sex Differentiation, Protozoan Proteins, Genome, Host-Parasite Interactions, Transcriptome, parasitic diseases, medicine, Gametocyte, Animals, Parasite hosting, Genetics, Life Cycle Stages, Sex Characteristics, biology, Gene Expression Regulation, Developmental, medicine.disease, biology.organism_classification, Infectious Diseases, Sporozoites, Proteome, Female, Parasitology, Malaria, Sex characteristics

Abstract

The gametocyte, or sexual blood-stage, of the malaria parasite represents the only stage of the parasite that can be transmitted to the mosquito vector following sexual development within the infected bloodmeal. Little is known about the processes leading to this cellular differentiation and specialization. The recent completion of the Plasmodium genome, and subsequent transcriptome and proteome analyses have revealed for the first time a molecular map of the genes that are differentially regulated at the onset of and during gametocytogenesis. In this review, we outline the underlying mechanisms involved in this process, focusing on the transition between the asexual and the sexual blood-stages of the parasite.

Published

2008

44. A repeat sequence domain of the ring-exported protein-1 of Plasmodium falciparum controls export machinery architecture and virulence protein trafficking

Author

Emma, McHugh, Steven, Batinovic, Eric, Hanssen, Paul J, McMillan, Shannon, Kenny, Michael D W, Griffin, Simon, Crawford, Katharine R, Trenholme, Donald L, Gardiner, Matthew W A, Dixon, and Leann, Tilley

Subjects

CD36 Antigens, Erythrocytes, Virulence Factors, Erythrocyte Membrane, Plasmodium falciparum, Protozoan Proteins, Proteins, DNA, Protozoan, Article, Protein Structure, Tertiary, Protein Transport, Gene Knockdown Techniques, parasitic diseases, Mutation, Humans, Repetitive Sequences, Nucleic Acid

Abstract

The malaria parasite Plasmodium falciparum dramatically remodels its host red blood cell to enhance its own survival, using a secretory membrane system that it establishes outside its own cell. Cisternal organelles, called Maurer’s clefts, act as a staging point for the forward trafficking of virulence proteins to the red blood cell (RBC) membrane. The Ring-EXported Protein-1 (REX1) is a Maurer’s cleft resident protein. We show that inducible knockdown of REX1 causes stacking of Maurer’s cleft cisternae without disrupting the organization of the knob-associated histidine-rich protein at the RBC membrane. Genetic dissection of the REX1 sequence shows that loss of a repeat sequence domain results in the formation of giant Maurer’s cleft stacks. The stacked Maurer’s clefts are decorated with tether-like structures and retain the ability to dock onto the RBC membrane skeleton. The REX1 mutant parasites show deficient export of the major virulence protein, PfEMP1, to the red blood cell surface and markedly reduced binding to the endothelial cell receptor, CD36. REX1 is predicted to form a largely α-helical structure, with a repetitive charge pattern in the repeat sequence domain, providing potential insights into the role of REX1 in Maurer’s cleft sculpting.

Published

2015

45. Specific expression and export of the Plasmodium falciparum Gametocyte EXported Protein-5 marks the gametocyte ring stage

Author

Oliver Looker, Sumera Younis Younis, Matthew W. A. Dixon, Pietro Alano, Marta Tibúrcio, and Leann Tilley

Subjects

Cytoplasm, Plasmodium, Erythrocytes, Plasmodium falciparum, Protozoan Proteins, Gametocyte, Biology, Host-Parasite Interactions, medicine, Humans, Exported protein, Early gametocyte marker, Gene, Regulation of gene expression, Genetics, Chromosome 9, Life Cycle Stages, Sexual differentiation, Research, biology.organism_classification, medicine.disease, Subtelomere, 3. Good health, Infectious Diseases, Gene Expression Regulation, Commitment, Parasitology, Malaria

Abstract

Background Plasmodium falciparum sexual development plays a fundamental role in the transmission and spread of malaria. The ability to generate gametocytes can be lost during culture in vitro, often associated with the loss of a subtelomeric region of chromosome 9. Gametocytogenesis starts with erythrocyte invasion by a sexually committed merozoite, but the first available specific marker of sexual differentiation appears only from 24 h post invasion. Methods Specific antibodies and gene fusions were produced to study the timing of expression and the sub-cellular localization of the P. falciparum Gametocyte EXported Protein-5 (PfGEXP5), encoded in the subtelomeric region of chromosome 9. Expression patterns were examined in wild-type parasites and in parasite lines mutated in the Apetala2-G (AP2-G) transcription factor, governing a cascade of early sexual stage specific genes. Results PfGEXP5 is highly expressed in early sexual stages and it is actively exported to the infected erythrocyte cytoplasm from as early as 14 h post-invasion in haemozoin-free, ring stage-like parasites. The pattern of PfGEXP5 expression and export is similar in wild-type parasites and in independent AP2-G defective parasite lines unable to produce gametocytes. Conclusions PfGEXP5 represents the earliest post-invasion sexual stage marker described to date. This provides a tool that can be used to identify sexually committed ring stage parasites in natural infections. This early gametocyte marker would enable the identification and mapping of malaria transmission reservoirs in human populations and the study of gametocyte sequestration dynamics in infected individuals. The fact that regulation of PfGEXP5 does not depend on the AP2-G master regulator of parasite sexual development suggests that, after sexual commitment, differentiation progresses through multiple checkpoints in the early phase of gametocytogenesis. Electronic supplementary material The online version of this article (doi:10.1186/s12936-015-0853-6) contains supplementary material, which is available to authorized users.

Published

2015

46. Multiple stiffening effects of nanoscale knobs on human red blood cells infected with Plasmodium falciparum malaria parasite

Author

Yao Zhang, Matthew W. A. Dixon, Changjin Huang, Ju Li, Mahdi Golkaram, Leann Tilley, Subra Suresh, Sangtae Kim, and Sulin Zhang

Subjects

Erythrocytes, viruses, Lipid Bilayers, Plasmodium falciparum, Molecular Dynamics Simulation, parasitic diseases, medicine, Parasite hosting, Humans, Spectrin, Computer Simulation, Malaria, Falciparum, Cytoskeleton, Lipid bilayer, Multidisciplinary, biology, Strain (chemistry), Erythrocyte Membrane, Biological Sciences, biology.organism_classification, medicine.disease, Virology, 3. Good health, Cell biology, Red blood cell, medicine.anatomical_structure, Erythrocyte Count, Stress, Mechanical, Shear Strength, Malaria, circulatory and respiratory physiology

Abstract

During its asexual development within the red blood cell (RBC), Plasmodium falciparum (Pf), the most virulent human malaria parasite, exports proteins that modify the host RBC membrane. The attendant increase in cell stiffness and cytoadherence leads to sequestration of infected RBCs in microvasculature, which enables the parasite to evade the spleen, and leads to organ dysfunction in severe cases of malaria. Despite progress in understanding malaria pathogenesis, the molecular mechanisms responsible for the dramatic loss of deformability of Pf-infected RBCs have remained elusive. By recourse to a coarse-grained (CG) model that captures the molecular structures of Pf-infected RBC membrane, here we show that nanoscale surface protrusions, known as “knobs,” introduce multiple stiffening mechanisms through composite strengthening, strain hardening, and knob density-dependent vertical coupling. On one hand, the knobs act as structural strengtheners for the spectrin network; on the other, the presence of knobs results in strain inhomogeneity in the spectrin network with elevated shear strain in the knob-free regions, which, given its strain-hardening property, effectively stiffens the network. From the trophozoite to the schizont stage that ensues within 24–48 h of parasite invasion into the RBC, the rise in the knob density results in the increased number of vertical constraints between the spectrin network and the lipid bilayer, which further stiffens the membrane. The shear moduli of Pf-infected RBCs predicted by the CG model at different stages of parasite maturation are in agreement with experimental results. In addition to providing a fundamental understanding of the stiffening mechanisms of Pf-infected RBCs, our simulation results suggest potential targets for antimalarial therapies.

Published

2015

47. Reliable transfection of Plasmodium falciparum using non-commercial plasmid mini preparations

Author

Mandy Hannemann, Donald L. Gardiner, Tobias Spielmann, Maria Hernandez-Valladares, Katharine R. Trenholme, and Matthew W. A. Dixon

Subjects

animal structures, Non commercial, viruses, Genes, Protozoan, Plasmodium falciparum, Protozoan Proteins, Transfection, Apicomplexa, Plasmid, Plasmid dna, parasitic diseases, Animals, Transgenes, Protozoal disease, biology, fungi, Membrane Proteins, DNA, Protozoan, biology.organism_classification, Virology, Molecular biology, Infectious Diseases, embryonic structures, Parasitology, Plasmids

Abstract

Transfection of Plasmodium falciparum is instrumental in the research on this parasite. However, the actual transfection protocol has not changed significantly since the first description and it is generally believed that large amounts of highly pure plasmid DNA are needed for successful transfection. Here, we report the transfection of P. falciparum using a protocol based on non-commercial mini-preparations of plasmid DNA. This method permits the reliable transfection of P. falciparum using less resources and lower costs, with a success rate comparable with currently used methods. A moderate throughput may be achieved using this method, providing a first step towards systematic transfection approaches in this parasite.

Published

2006

48. A Cluster of Ring Stage–specific Genes Linked to a Locus Implicated in Cytoadherence inPlasmodium falciparumCodes for PEXEL-negative and PEXEL-positive Proteins Exported into the Host Cell

Author

Kathleen Klotz, Leann Tilley, Nectarios Klonis, Tobias Spielmann, Katharine R. Trenholme, Mandy Hannemann, David J. Kemp, Matthew W. A. Dixon, Donald L. Gardiner, and Paula L. Hawthorne

Subjects

Cytoplasm, Erythrocytes, Genes, Protozoan, Plasmodium falciparum, Protozoan Proteins, Virulence, Genome, Chromosomes, Mice, Animals, Molecular Biology, Gene, Genetics, Life Cycle Stages, Sequence Homology, Amino Acid, biology, Articles, Exons, Cell Biology, Physical Chromosome Mapping, biology.organism_classification, Recombinant Proteins, Transport protein, Protein Transport, Solubility, Membrane protein, Vacuolar transport, Sequence motif, Genome, Protozoan

Abstract

Blood stages of Plasmodium falciparum export proteins into their erythrocyte host, thereby inducing extensive host cell modifications that become apparent after the first half of the asexual development cycle (ring stage). This is responsible for a major part of parasite virulence. Export of many parasite proteins depends on a sequence motif termed Plasmodium export element (PEXEL) or vacuolar transport signal (VTS). This motif has allowed the prediction of the Plasmodium exportome. Using published genome sequence, we redetermined the boundaries of a previously studied region linked to P. falciparum virulence, reducing the number of candidate genes in this region to 13. Among these, we identified a cluster of four ring stage-specific genes, one of which is known to encode an exported protein. We demonstrate that all four genes code for proteins exported into the host cell, although only two genes contain an obvious PEXEL/VTS motif. We propose that the systematic analysis of ring stage-specific genes will reveal a cohort of exported proteins not present in the currently predicted exportome. Moreover, this provides further evidence that host cell remodeling is a major task of this developmental stage. Biochemical and photobleaching studies using these proteins reveal new properties of the parasite-induced membrane compartments in the host cell. This has important implications for the biogenesis and connectivity of these structures.

Published

2006

49. Bio-sensing with butterfly wings: naturally occurring nano-structures for SERS-based malaria parasite detection

Author

Ryo Sekine, Keith R. Bambery, Matthew W. A. Dixon, Bayden R. Wood, Leann Tilley, Natalie L. Garrett, Garrett, Natalie L, Sekine, Ryo, Dixon, Matthew WA, Tilley, Leann, Bambery, Keith R, and Wood, Bayden R

Subjects

Hemeproteins, Plasmodium, Erythrocytes, General Physics and Astronomy, Nanotechnology, 02 engineering and technology, 010402 general chemistry, Spectrum Analysis, Raman, 01 natural sciences, symbols.namesake, Optics, Microscopy, Nano, medicine, Parasite hosting, Animals, Humans, Wings, Animal, Physical and Theoretical Chemistry, business.industry, Hemozoin, 021001 nanoscience & nanotechnology, medicine.disease, 3. Good health, 0104 chemical sciences, Malaria, Nanostructures, Blood smear, symbols, Gold, 0210 nano-technology, Raman spectroscopy, business, Butterflies, Raman scattering

Abstract

Surface enhanced Raman scattering (SERS) is a powerful tool with great potential to provide improved bio-sensing capabilities. The current 'gold-standard' method for diagnosis of malaria involves visual inspection of blood smears using light microscopy, which is time consuming and can prevent early diagnosis of the disease. We present a novel surface-enhanced Raman spectroscopy substrate based on gold-coated butterfly wings, which enabled detection of malarial hemozoin pigment within lysed blood samples containing 0.005%and 0.0005% infected red blood cells Refereed/Peer-reviewed

Published

2014

50. Implication of a Plasmodium falciparum gene in the switch between asexual reproduction and gametocytogenesis

Author

Donald L. Gardiner, Paula L. Hawthorne, Tina S. Skinner-Adams, Katharine R. Trenholme, David J. Kemp, Tobias Spielmann, Maria R. Ortega, and Matthew W. A. Dixon

Subjects

Genes, Protozoan, Plasmodium falciparum, Antigens, Protozoan, Asexual reproduction, Biology, Gametogenesis, Reproduction, Asexual, parasitic diseases, Gametocyte, medicine, Animals, Vector (molecular biology), Molecular Biology, Gene, Genetics, Genetic Complementation Test, Membrane Proteins, Transfection, Blotting, Northern, medicine.disease, biology.organism_classification, Virology, Parasitology, Malaria

Abstract

Gametocytogenesis is fundamental for transmission of the malaria parasite Plasmodium falciparum from the human host to the mosquito vector, yet very little is understood about what triggers the switch between asexual reproduction and gametocytogenesis. Arresting the progression through the sexual cycle would block transmission of this disease. Here we identify a novel gene in P. falciparum that when genetically silenced reduces gametocyte production by a factor of 6, and when complemented up-regulates gametocyte-specific gene transcription.

Published

2005