Your search keyword '"Sash Lopaticki"' showing total 36 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. Publisher Correction: Tryptophan C-mannosylation is critical for Plasmodium falciparum transmission

Author

Sash Lopaticki, Robyn McConville, Alan John, Niall Geoghegan, Shihab Deen Mohamed, Lisa Verzier, Ryan W. J. Steel, Cindy Evelyn, Matthew T. O’Neill, Niccolay Madiedo Soler, Nichollas E. Scott, Kelly L. Rogers, Ethan D. Goddard-Borger, and Justin A. Boddey

Subjects

Multidisciplinary, General Physics and Astronomy, General Chemistry, General Biochemistry, Genetics and Molecular Biology

Published

2022

3. Tryptophan C-mannosylation is critical for Plasmodium falciparum transmission

Author

Sash Lopaticki, Robyn McConville, Alan John, Niall Geoghegan, Shihab Deen Mohamed, Lisa Verzier, Ryan W. J. Steel, Cindy Evelyn, Matthew T. O’Neill, Niccolay Madiedo Soler, Nichollas E. Scott, Kelly L. Rogers, Ethan D. Goddard-Borger, and Justin A. Boddey

Subjects

Multidisciplinary, General Physics and Astronomy, General Chemistry, General Biochemistry, Genetics and Molecular Biology

Abstract

Tryptophan C-mannosylation stabilizes proteins bearing a thrombospondin repeat (TSR) domain in metazoans. Here we show that Plasmodium falciparum expresses a DPY19 tryptophan C-mannosyltransferase in the endoplasmic reticulum and that DPY19-deficiency abolishes C-glycosylation, destabilizes members of the TRAP adhesin family and inhibits transmission to mosquitoes. Imaging P. falciparum gametogenesis in its entirety in four dimensions using lattice light-sheet microscopy reveals defects in ΔDPY19 gametocyte egress and exflagellation. While egress is diminished, ΔDPY19 microgametes still fertilize macrogametes, forming ookinetes, but these are abrogated for mosquito infection. The gametogenesis defects correspond with destabilization of MTRAP, which we show is C-mannosylated in P. falciparum, and the ookinete defect is concordant with defective CTRP secretion on the ΔDPY19 background. Genetic complementation of DPY19 restores ookinete infectivity, sporozoite production and C-mannosylation activity. Therefore, tryptophan C-mannosylation by DPY19 ensures TSR protein quality control at two lifecycle stages for successful transmission of the human malaria parasite.

Published

2022

4. Tryptophan C-mannosylation is critical for Plasmodium falciparum transmission

Author

Sash, Lopaticki, Robyn, McConville, Alan, John, Niall, Geoghegan, Shihab Deen, Mohamed, Lisa, Verzier, Ryan W J, Steel, Cindy, Evelyn, Matthew T, O'Neill, Niccolay Madiedo, Soler, Nichollas E, Scott, Kelly L, Rogers, Ethan D, Goddard-Borger, and Justin A, Boddey

Subjects

Culicidae, Glycosylation, Plasmodium falciparum, Protozoan Proteins, Tryptophan, Animals, Humans, Malaria, Falciparum, Thrombospondins

Abstract

Tryptophan C-mannosylation stabilizes proteins bearing a thrombospondin repeat (TSR) domain in metazoans. Here we show that Plasmodium falciparum expresses a DPY19 tryptophan C-mannosyltransferase in the endoplasmic reticulum and that DPY19-deficiency abolishes C-glycosylation, destabilizes members of the TRAP adhesin family and inhibits transmission to mosquitoes. Imaging P. falciparum gametogenesis in its entirety in four dimensions using lattice light-sheet microscopy reveals defects in ΔDPY19 gametocyte egress and exflagellation. While egress is diminished, ΔDPY19 microgametes still fertilize macrogametes, forming ookinetes, but these are abrogated for mosquito infection. The gametogenesis defects correspond with destabilization of MTRAP, which we show is C-mannosylated in P. falciparum, and the ookinete defect is concordant with defective CTRP secretion on the ΔDPY19 background. Genetic complementation of DPY19 restores ookinete infectivity, sporozoite production and C-mannosylation activity. Therefore, tryptophan C-mannosylation by DPY19 ensures TSR protein quality control at two lifecycle stages for successful transmission of the human malaria parasite.

Published

2022

5. Tryptophan C-mannosylation is critical for Plasmodium falciparum transmission

Author

Sash Lopaticki, Robyn McConville, Alan John, Niall Geoghegan, Shihab Deen Mohamed, Lisa Verzier, Ryan Steel, Cindy Evelyn, Matthew O'Neill, Sabrina Caiazzo, Niccolay Madiedo Soler, Nichollas Scott, Kelly Rogers, Ethan Goddard-Borger, and Justin Boddey

Abstract

C-mannosylation stabilizes proteins bearing a thrombospondin repeat (TSR) domain in metazoans. Here we show that Plasmodium falciparum expresses a DPY19 C-mannosyltransferase in the endoplasmic reticulum and that DPY19-deficiency abolishes C-glycosylation, destabilizes members of the TRAP adhesin family and inhibits transmission to mosquitoes. P. falciparum gametogenesis was imaged in its entirety in four dimensions using lattice light-sheet microscopy. This revealed defects in egress and exflagellation for DDPY19 microgametes. While exflagellation was diminished, DDPY19 microgametes still fertilized macrogametes, forming ookinetes but these were abrogated for mosquito infection. The gametogenesis defects corresponded with destabilization of MTRAP, which we show is C-mannosylated in P. falciparum, and the ookinete defect was concordant with defective CTRP secretion on the DDPY19 background. Genetic complementation of DPY19 restored ookinete infectivity, sporozoite production and C-mannosylation activity. Therefore, tryptophan C-mannosylation by DPY19 in the early secretory pathway ensures TSR protein quality control at two lifecycle stages for successful transmission of the human malaria parasite.

Published

2022

6. Epigenetic Silencing of RIPK3 in Hepatocytes Prevents MLKL-mediated Necroptosis From Contributing to Liver Pathologies

Author

Simon P. Preston, Michael D. Stutz, Cody C. Allison, Ueli Nachbur, Quentin Gouil, Bang Manh Tran, Valerie Duvivier, Philip Arandjelovic, James P. Cooney, Liana Mackiewicz, Yanxiang Meng, Jan Schaefer, Stefanie M. Bader, Hongke Peng, Zina Valaydon, Pravin Rajasekaran, Charlie Jennison, Sash Lopaticki, Ann Farrell, Marno Ryan, Jess Howell, Catherine Croagh, Denuja Karunakaran, Carole Schuster-Klein, James M. Murphy, Theodora Fifis, Christopher Christophi, Elizabeth Vincan, Marnie E. Blewitt, Alexander Thompson, Justin A. Boddey, Marcel Doerflinger, and Marc Pellegrini

Subjects

Male, Mice, Hepatology, Non-alcoholic Fatty Liver Disease, Receptor-Interacting Protein Serine-Threonine Kinases, Necroptosis, Gastroenterology, Hepatocytes, Humans, Animals, Female, Protein Kinases, Epigenesis, Genetic

Abstract

Necroptosis is a highly inflammatory mode of cell death that has been implicated in causing hepatic injury including steatohepatitis/ nonalcoholic steatohepatitis (NASH); however, the evidence supporting these claims has been controversial. A comprehensive, fundamental understanding of cell death pathways involved in liver disease critically underpins rational strategies for therapeutic intervention. We sought to define the role and relevance of necroptosis in liver pathology.Several animal models of human liver pathology, including diet-induced steatohepatitis in male mice and diverse infections in both male and female mice, were used to dissect the relevance of necroptosis in liver pathobiology. We applied necroptotic stimuli to primary mouse and human hepatocytes to measure their susceptibility to necroptosis. Paired liver biospecimens from patients with NASH, before and after intervention, were analyzed. DNA methylation sequencing was also performed to investigate the epigenetic regulation of RIPK3 expression in primary human and mouse hepatocytes.Identical infection kinetics and pathologic outcomes were observed in mice deficient in an essential necroptotic effector protein, MLKL, compared with control animals. Mice lacking MLKL were indistinguishable from wild-type mice when fed a high-fat diet to induce NASH. Under all conditions tested, we were unable to induce necroptosis in hepatocytes. We confirmed that a critical activator of necroptosis, RIPK3, was epigenetically silenced in mouse and human primary hepatocytes and rendered them unable to undergo necroptosis.We have provided compelling evidence that necroptosis is disabled in hepatocytes during homeostasis and in the pathologic conditions tested in this study.

Published

2021

7. Dual Plasmepsin-Targeting Antimalarial Agents Disrupt Multiple Stages of the Malaria Parasite Life Cycle

Author

Janni Christensen, David B. Olsen, Kitsanapong Reaksudsan, Jennifer K. Thompson, Kai-Yuan Guo, Wai-Hong Tham, Tony Triglia, Christopher W. Boyce, Justin A Boddey, Lianyun Zhao, Nicholas Murgolo, Marissa Vavrek, Tanweer A. Khan, Alan F. Cowman, Helene Jousset Sabroux, Jocelyn Sietsma Penington, Ryan W.J. Steel, Manuel de Lera Ruiz, Brad E. Sleebs, Jonathan A. Robbins, Zhuyan Guo, Matthias Rottmann, Paola Favuzza, Anna Ngo, Lachlan Richardson, Julie Healer, John A. Mccauley, Kate E. Jarman, Sash Lopaticki, Tony Papenfuss, Melanie H. Dietrich, and Mengwei Hu

Subjects

Plasmodium, Combination therapy, Plasmodium berghei, Plasmodium falciparum, Plasmepsin, plasmepsin, Mice, Transgenic, Pharmacology, Microbiology, Article, 03 medical and health sciences, Antimalarials, Mice, 0302 clinical medicine, Virology, parasitic diseases, medicine, Disease Transmission, Infectious, Animals, Aspartic Acid Endopeptidases, Parasites, Antimalarial Agent, plasmepsin X, 030304 developmental biology, 0303 health sciences, Life Cycle Stages, antimalarial, biology, Merozoites, Intracellular parasite, medicine.disease, biology.organism_classification, plasmepsin IX, merozoite, 3. Good health, Malaria, Humanized mouse, Parasitology, humanized mouse, 030217 neurology & neurosurgery

Abstract

Summary Artemisin combination therapy (ACT) is the main treatment option for malaria, which is caused by the intracellular parasite Plasmodium. However, increased resistance to ACT highlights the importance of finding new drugs. Recently, the aspartic proteases Plasmepsin IX and X (PMIX and PMX) were identified as promising drug targets. In this study, we describe dual inhibitors of PMIX and PMX, including WM382, that block multiple stages of the Plasmodium life cycle. We demonstrate that PMX is a master modulator of merozoite invasion and direct maturation of proteins required for invasion, parasite development, and egress. Oral administration of WM382 cured mice of P. berghei and prevented blood infection from the liver. In addition, WM382 was efficacious against P. falciparum asexual infection in humanized mice and prevented transmission to mosquitoes. Selection of resistant P. falciparum in vitro was not achievable. Together, these show that dual PMIX and PMX inhibitors are promising candidates for malaria treatment and prevention., Graphical Abstract, Highlights • Specific compounds against P. falciparum Plasmepsin IX and X were identified • PMIX and PMX are modulators of parasite proteins for egress, invasion, and development • Anti-PMIX and anti-PMX compounds inhibit liver, blood, and mosquito stages of Plasmodium • One compound, WM382, can clear mouse models of P. berghei and P. falciparum parasites, We describe inhibitors of essential aspartic proteases from malaria parasites that block multiple life cycle stages. PMIX and PMX are master modulators processing proteins required for invasion, development, and egress. Administration of WM382 cured mice of malaria infection, showing that these inhibitors are promising candidates for malaria treatment and prevention.

Published

2019

8. Export of malaria proteins requires co-translational processing of the PEXEL motif independent of phosphatidylinositol-3-phosphate binding

Author

Stephan Wawra, Justin A Boddey, Anthony N. Hodder, Matthew T. O'Neill, Sven Flemming, Zeinab Ebrahimzadeh, Jeffrey J. Babon, Alan F. Cowman, Tobias Spielmann, Teresa Carvalho, Pieter van West, Jude M. Przyborski, Dave Richard, Sash Lopaticki, and Thomas Nebl

Subjects

0301 basic medicine, Signal peptide, Science, 030106 microbiology, Mutant, Amino Acid Motifs, Plasmodium falciparum, Protozoan Proteins, General Physics and Astronomy, Plasma protein binding, KAHRP, Biology, General Biochemistry, Genetics and Molecular Biology, Article, Lopinavir, 03 medical and health sciences, Phosphatidylinositol Phosphates, parasitic diseases, Escherichia coli, Multidisciplinary, Effector, Endoplasmic reticulum, Cell Membrane, General Chemistry, biology.organism_classification, 3. Good health, Biochemistry, FYVE domain, Protein Binding

Abstract

Plasmodium falciparum exports proteins into erythrocytes using the Plasmodium export element (PEXEL) motif, which is cleaved in the endoplasmic reticulum (ER) by plasmepsin V (PMV). A recent study reported that phosphatidylinositol-3-phosphate (PI(3)P) concentrated in the ER binds to PEXEL motifs and is required for export independent of PMV, and that PEXEL motifs are functionally interchangeable with RxLR motifs of oomycete effectors. Here we show that the PEXEL does not bind PI(3)P, and that this lipid is not concentrated in the ER. We find that RxLR motifs cannot mediate export in P. falciparum. Parasites expressing a mutated version of KAHRP, with the PEXEL motif repositioned near the signal sequence, prevented PMV cleavage. This mutant possessed the putative PI(3)P-binding residues but is not exported. Reinstatement of PEXEL to its original location restores processing by PMV and export. These results challenge the PI(3)P hypothesis and provide evidence that PEXEL position is conserved for co-translational processing and export., Export of Plasmodium falciparum proteins into infected erythrocytes relies upon the PEXEL motif in target proteins. Here Boddey et al. challenge the hypothesis that the PEXEL motif mediates export by binding PI(3)P and instead suggest it acts via cleavage by plasmepsin V.

Published

2016

9. Targeting the Extrinsic Pathway of Hepatocyte Apoptosis Promotes Clearance of Plasmodium Liver Infection

Author

Justin A Boddey, Marc Pellegrini, Annie S. P. Yang, Pravin Rajasekaran, Sash Lopaticki, Lisa J Ioannidis, Liana Mackiewicz, Gregor Ebert, Cody C. Allison, Ryan W.J. Steel, Matthew T. O'Neill, Marcel Doerflinger, Philip Arandjelovic, Sara M. Erickson, and John Silke

Subjects

0301 basic medicine, Plasmodium, Indoles, Protozoan Proteins, Administration, Oral, Biological Availability, Apoptosis, Inhibitor of apoptosis, General Biochemistry, Genetics and Molecular Biology, Inhibitor of Apoptosis Proteins, 03 medical and health sciences, 0302 clinical medicine, Immunity, medicine, Animals, Caspase, Life Cycle Stages, Liver infection, biology, Caspase 3, Tumor Necrosis Factor-alpha, Intracellular parasite, Dipeptides, biology.organism_classification, Malaria, Cell biology, Thiazoles, Culicidae, 030104 developmental biology, medicine.anatomical_structure, Liver, Sporozoites, Hepatocyte, Hepatocytes, biology.protein, 030217 neurology & neurosurgery

Abstract

Plasmodium sporozoites infect the liver and develop into exoerythrocytic merozoites that initiate blood-stage disease. The hepatocyte molecular pathways that permit or abrogate parasite replication and merozoite formation have not been thoroughly explored, and a deeper understanding may identify therapeutic strategies to mitigate malaria. Cellular inhibitor of apoptosis (cIAP) proteins regulate cell survival and are co-opted by intracellular pathogens to support development. Here, we show that cIAP1 levels are upregulated during Plasmodium liver infection and that genetic or pharmacological targeting of cIAPs using clinical-stage antagonists preferentially kills infected hepatocytes and promotes immunity. Using gene-targeted mice, the mechanism was defined as TNF-TNFR1-mediated apoptosis via caspases 3 and 8 to clear parasites. This study reveals the importance of cIAPs to Plasmodium infection and demonstrates that host-directed antimalarial drugs can eliminate liver parasites and induce immunity while likely providing a high barrier to resistance in the parasite.

Published

2020

10. Plasmodium falciparum subtilisin-like ookinete protein SOPT plays an important and conserved role during ookinete infection of the Anopheles stephensi midgut

Author

Pravin Rajasekaran, Kirsten K. Hanson, Sash Lopaticki, Peter Liehl, Jennifer S. Armistead, Takeshi Annoura, Justin A Boddey, Sara M. Erickson, Shahid M. Khan, Christopher J. Tonkin, Charlie Jennison, Matthew T. O'Neill, and Maria M. Mota

Subjects

0301 basic medicine, Signal peptide, Plasmodium falciparum, Protozoan Proteins, Virulence, Mosquito Vectors, Microbiology, 03 medical and health sciences, Anopheles, parasitic diseases, Animals, Parasite hosting, Malaria, Falciparum, Molecular Biology, Gene, Anopheles stephensi, biology, fungi, Oocysts, Subtilisin, Midgut, biology.organism_classification, Cell biology, 030104 developmental biology, Sporozoites, Digestive System

Abstract

Transmission of the malaria parasite Plasmodium falciparum involves infection of Anopheles mosquitoes. Here we characterize SOPT, a protein expressed in P. falciparum ookinetes that facilitates infection of the mosquito midgut. SOPT was identified on the basis that it contains a signal peptide, a PEXEL-like sequence and is expressed in asexual, ookinete and sporozoite stages, suggesting it is involved in infecting the human or mosquito host. SOPT is predicted to contain a subtilisin-like fold with a non-canonical catalytic triad and is orthologous to P. berghei PIMMS2. Localization studies reveal that SOPT is not exported to the erythrocyte but is expressed in ookinetes at the parasite periphery. SOPT-deficient parasites develop normally through the asexual and sexual stages and produce equivalent numbers of ookinetes to NF54 controls, however, they form fewer oocysts and sporozoites in mosquitoes. SOPT-deficient parasites were also unable to activate the immune-responsive midgut invasion marker SRPN6 after mosquito ingestion, suggesting they are defective for entry into the midgut. Disruption of SOPT in P. berghei (PIMMS2) did not affect other lifecycle stages or ookinete development but again resulted in fewer oocysts and sporozoites in mosquitoes. Collectively, this study shows that SOPT/PIMMS2 plays a conserved role in ookinetes of different Plasmodium species.

Published

2018

11. Structural basis for plasmepsin V inhibition that blocks export of malaria proteins to human erythrocytes

Author

Matthew T. O'Neill, Brian J. Smith, Peter E. Czabotar, Alan F. Cowman, Tony Triglia, Justin A Boddey, Yibin Xu, Anthony N. Hodder, Brad E. Sleebs, Kym N Lowes, Sash Lopaticki, Thomas Nebl, and Michelle Gazdik

Subjects

Models, Molecular, Erythrocytes, Amino Acid Motifs, Green Fluorescent Proteins, Immunoblotting, Molecular Sequence Data, Plasmodium falciparum, Plasmodium vivax, Protozoan Proteins, Plasmepsin, Plasma protein binding, Crystallography, X-Ray, Cell Line, Substrate Specificity, Protein structure, Structural Biology, parasitic diseases, Animals, Aspartic Acid Endopeptidases, Humans, Protease Inhibitors, Amino Acid Sequence, Molecular Biology, Molecular Structure, Sequence Homology, Amino Acid, biology, Chemistry, Effector, Membrane Proteins, Surface Plasmon Resonance, biology.organism_classification, Protein Structure, Tertiary, Transport protein, Protein Transport, Membrane protein, Biochemistry, Carbamates, Peptides, Oligopeptides, Protein Binding

Abstract

Plasmepsin V, an essential aspartyl protease of malaria parasites, has a key role in the export of effector proteins to parasite-infected erythrocytes. Consequently, it is an important drug target for the two most virulent malaria parasites of humans, Plasmodium falciparum and Plasmodium vivax. We developed a potent inhibitor of plasmepsin V, called WEHI-842, which directly mimics the Plasmodium export element (PEXEL). WEHI-842 inhibits recombinant plasmepsin V with a half-maximal inhibitory concentration of 0.2 nM, efficiently blocks protein export and inhibits parasite growth. We obtained the structure of P. vivax plasmepsin V in complex with WEHI-842 to 2.4-Å resolution, which provides an explanation for the strict requirements for substrate and inhibitor binding. The structure characterizes both a plant-like fold and a malaria-specific helix-turn-helix motif that are likely to be important in cleavage of effector substrates for export.

Published

2015

12. The effect of N-methylation on transition state mimetic inhibitors of the Plasmodium protease, plasmepsin V

Author

Brian J. Smith, Brad E. Sleebs, Michelle Gazdik, Kym N Lowes, Matthew T. O'Neill, Justin A Boddey, Alan F. Cowman, and Sash Lopaticki

Subjects

Pharmacology, Protease, Transition (genetics), Stereochemistry, medicine.medical_treatment, Organic Chemistry, Plasmepsin, Plasmepsin V, Pharmaceutical Science, N methylation, Biology, biology.organism_classification, Biochemistry, Plasmodium, Drug Discovery, Lipophilicity, medicine, Molecular Medicine, Peptide bond

Abstract

N-Methylation of the N–Cα peptide bond is a known strategy to overcome the liabilities inherently associated with peptide-like molecules. Here, we apply this strategy to transition state mimetics that are potent inhibitors of the malarial protease, plasmepsin V, with the aim of enhancing their activity against Plasmodium parasites. We demonstrate that independent N-methylation of each N–Cα bond of the mimetics interferes with binding interactions to plasmepsin V, resulting in reduced affinity for the protease. We provide evidence that N-methylation improves proteolytic stability and slightly improves lipophilicity. However, the observed parasite activity of the N-methyl compounds had little correlation with on-target plasmepsin V activity, indicating non-specific activity. This study underscores the benefits and the drawbacks of the N-methylation strategy, and provides further evidence that plasmepsin V is highly sensitive to substrate modification.

Published

2015

13. Protein O-fucosylation in Plasmodium falciparum ensures efficient infection of mosquito and vertebrate hosts

Author

Ethan D. Goddard-Borger, Justin A Boddey, Norman M. Kneteman, Annie S. P. Yang, Sara M. Erickson, Lachlan Whitehead, Alan John, Matthew T. O'Neill, Nicole C. McKenzie, Nichollas E. Scott, Charlie Jennison, James P. Lingford, Sash Lopaticki, and Donna N. Douglas

Subjects

0301 basic medicine, animal structures, Glycosylation, Gliding motility, Science, Plasmodium falciparum, lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], Protozoan Proteins, General Physics and Astronomy, Plasmodium, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, parasitic diseases, medicine, Animals, Humans, Malaria, Falciparum, lcsh:Science, GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries), Fucosylation, Thrombospondin, Multidisciplinary, biology, Endoplasmic reticulum, fungi, General Chemistry, medicine.disease, biology.organism_classification, Fucosyltransferases, Virology, 3. Good health, Cell biology, Circumsporozoite protein, 030104 developmental biology, Culicidae, Sporozoites, lcsh:Q, Malaria

Abstract

O-glycosylation of the Plasmodium sporozoite surface proteins CSP and TRAP was recently identified, but the role of this modification in the parasite life cycle and its relevance to vaccine design remain unclear. Here, we identify the Plasmodium protein O-fucosyltransferase (POFUT2) responsible for O-glycosylating CSP and TRAP. Genetic disruption of POFUT2 in Plasmodium falciparum results in ookinetes that are attenuated for colonizing the mosquito midgut, an essential step in malaria transmission. Some POFUT2-deficient parasites mature into salivary gland sporozoites although they are impaired for gliding motility, cell traversal, hepatocyte invasion, and production of exoerythrocytic forms in humanized chimeric liver mice. These defects can be attributed to destabilization and incorrect trafficking of proteins bearing thrombospondin repeats (TSRs). Therefore, POFUT2 plays a similar role in malaria parasites to that in metazoans: it ensures the trafficking of Plasmodium TSR proteins as part of a non-canonical glycosylation-dependent endoplasmic reticulum protein quality control mechanism., The role of O-glycosylation in the malaria life cycle is largely unknown. Here, the authors identify a Plasmodium protein O-fucosyltransferase and show that it is important for normal trafficking of a subset of surface proteins, particularly CSP and TRAP, and efficient infection of mosquito and vertebrate hosts.

Published

2017

14. AMA1 and MAEBL are important for Plasmodium falciparum sporozoite infection of the liver

Author

Sara M. Erickson, Annie S. P. Yang, Donna N. Douglas, Justin A Boddey, Sash Lopaticki, Matthew T. O'Neill, and Norman M. Kneteman

Subjects

0301 basic medicine, Erythrocytes, Immunology, Cell, Plasmodium falciparum, Protozoan Proteins, Antigens, Protozoan, Receptors, Cell Surface, Mice, SCID, Biology, Microbiology, Cell Line, 03 medical and health sciences, Mice, Antigen, Virology, parasitic diseases, Anopheles, medicine, Animals, Humans, Malaria, Falciparum, Liver infection, 030102 biochemistry & molecular biology, Merozoites, Membrane Proteins, biology.organism_classification, Cell biology, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Liver, Cell culture, Sporozoites, Hepatocyte, Hepatocytes, Hepatocyte growth factor, medicine.drug

Abstract

The malaria sporozoite injected by a mosquito migrates to the liver by traversing host cells. The sporozoite also traverses hepatocytes before invading a terminal hepatocyte and developing into exoerythrocytic forms. Hepatocyte infection is critical for parasite development into merozoites that infect erythrocytes, and the sporozoite is thus an important target for antimalarial intervention. Here, we investigated two abundant sporozoite proteins of the most virulent malaria parasite Plasmodium falciparum and show that they play important roles during cell traversal and invasion of human hepatocytes. Incubation of P. falciparum sporozoites with R1 peptide, an inhibitor of apical merozoite antigen 1 (AMA1) that blocks merozoite invasion of erythrocytes, strongly reduced cell traversal activity. Consistent with its inhibitory effect on merozoites, R1 peptide also reduced sporozoite entry into human hepatocytes. The strong but incomplete inhibition prompted us to study the AMA-like protein, merozoite apical erythrocyte-binding ligand (MAEBL). MAEBL-deficient P. falciparum sporozoites were severely attenuated for cell traversal activity and hepatocyte entry in vitro and for liver infection in humanized chimeric liver mice. This study shows that AMA1 and MAEBL are important for P. falciparum sporozoites to perform typical functions necessary for infection of human hepatocytes. These two proteins therefore have important roles during infection at distinct points in the life cycle, including the blood, mosquito, and liver stages.

Published

2016

15. Cell Traversal Activity Is Important for Plasmodium falciparum Liver Infection in Humanized Mice

Author

Annie S. P. Yang, Sara M. Erickson, James C. Whisstock, Cody C. Allison, Donna N. Douglas, Charlie Jennison, Jennifer S. Armistead, Rhoel R. Dinglasan, Norman M. Kneteman, Matthew T. O'Neill, Sash Lopaticki, Kelly L. Rogers, Andrew M. Ellisdon, Rebecca E. Tweedell, and Justin A Boddey

Subjects

0301 basic medicine, 030106 microbiology, Cell, Plasmodium falciparum, malaria, Protozoan Proteins, Mice, SCID, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, Microneme, 03 medical and health sciences, Cell Movement, parasitic diseases, medicine, hepatocyte, sporozoite, Animals, Humans, genetics, Parasites, Malaria, Falciparum, lcsh:QH301-705.5, perforin, Mutation, Liver infection, biology, transmission, biology.organism_classification, invasion, Virology, 3. Good health, Cell biology, virulence, 030104 developmental biology, medicine.anatomical_structure, Perforin, motility, lcsh:Biology (General), Liver, Sporozoites, Hepatocyte, SPECT, biology.protein, Hepatocytes, Hepatocyte growth factor, medicine.drug

Abstract

Malaria sporozoites are deposited into the skin by mosquitoes and infect hepatocytes. The molecular basis of how Plasmodium falciparum sporozoites migrate through host cells is poorly understood, and direct evidence of its importance in vivo is lacking. Here, we generated traversal-deficient sporozoites by genetic disruption of sporozoite microneme protein essential for cell traversal (PfSPECT) or perforin-like protein 1 (PfPLP1). Loss of either gene did not affect P. falciparum growth in erythrocytes, in contrast with a previous report that PfPLP1 is essential for merozoite egress. However, although traversal-deficient sporozoites could invade hepatocytes in vitro, they could not establish normal liver infection in humanized mice. This is in contrast with NF54 sporozoites, which infected the humanized mice and developed into exoerythrocytic forms. This study demonstrates that SPECT and perforin-like protein 1 (PLP1) are critical for transcellular migration by P. falciparum sporozoites and demonstrates the importance of cell traversal for liver infection by this human pathogen.

Published

2016

16. Erythrocyte-binding antigens of Plasmodium falciparum are targets of human inhibitory antibodies and function to evade naturally acquired immunity

Author

Alan F. Cowman, Danny W. Wilson, James G. Beeson, Kristina E. M. Persson, Jack S. Richards, Sash Lopaticki, Nimmo Gicheru, Kevin Marsh, Fiona J. McCallum, Freya J. I. Fowkes, and Linda Reiling

Subjects

Adult, Male, Erythrocytes, Adolescent, Plasmodium falciparum, Immunology, Protozoan Proteins, Antibodies, Protozoan, Antigens, Protozoan, Article, Gene Knockout Techniques, Young Adult, Immune system, Antigen, Immunity, parasitic diseases, Humans, Immunology and Allergy, Malaria, Falciparum, Apical membrane antigen 1, Child, Aged, Immune Evasion, Aged, 80 and over, biology, Malaria vaccine, Genetic Variation, Membrane Proteins, Middle Aged, biology.organism_classification, Acquired immune system, Virology, Child, Preschool, biology.protein, Female, Antibody, Carrier Proteins

Abstract

Abs that inhibit Plasmodium falciparum invasion of erythrocytes form an important component of human immunity against malaria, but key target Ags are largely unknown. Phenotypic variation by P. falciparum mediates the evasion of inhibitory Abs, contributing to the capacity of P. falciparum to cause repeat and chronic infections. However, Ags involved in mediating immune evasion have not been defined, and studies of the function of human Abs are limited. In this study, we used novel approaches to determine the importance of P. falciparum erythrocyte-binding Ags (EBAs), which are important invasion ligands, as targets of human invasion-inhibitory Abs and define their role in contributing to immune evasion through variation in function. We evaluated the invasion-inhibitory activity of acquired Abs from malaria-exposed children and adults from Kenya, using P. falciparum with disruption of genes encoding EBA140, EBA175, and EBA181, either individually or combined as EBA140/EBA175 or EBA175/EBA181 double knockouts. Our findings provide important new evidence that variation in the expression and function of the EBAs plays an important role in evasion of acquired Abs and that a substantial amount of phenotypic diversity results from variation in expression of different EBAs that contributes to immune evasion by P. falciparum. All three EBAs were identified as important targets of naturally acquired inhibitory Abs demonstrated by differential inhibition of parental parasites greater than EBA knockout lines. This knowledge will help to advance malaria vaccine development and suggests that multiple invasion ligands need to be targeted to overcome the capacity of P. falciparum for immune evasion.

Published

2016

17. Plasmodium falciparum Adhesins Play an Essential Role in Signalling and Activation of Invasion into Human Erythrocytes

Author

Megan J. Bird, Sash Lopaticki, Paul R. Gilson, Isabelle S Lucet, Greta E. Weiss, Brendan S. Crabb, Alan F. Cowman, Wai-Hong Tham, Dominique Dorin-Semblat, Christian Doerig, Nicholas T.Y. Lim, and Brendan R E Ansell

Subjects

Erythrocytes, Protein family, QH301-705.5, Molecular Sequence Data, Plasmodium falciparum, Immunology, Protozoan Proteins, Microbiology, Plasmodium, 03 medical and health sciences, 0302 clinical medicine, Live cell imaging, Virology, parasitic diseases, Genetics, Humans, Amino Acid Sequence, Malaria, Falciparum, Phosphorylation, Biology (General), Receptor, Molecular Biology, 030304 developmental biology, 0303 health sciences, biology, Merozoites, Phosphotransferases, RC581-607, biology.organism_classification, 3. Good health, Cell biology, Bacterial adhesin, Membrane protein, Cytoplasm, Parasitology, Immunologic diseases. Allergy, 030217 neurology & neurosurgery, Research Article

Abstract

The most severe form of malaria in humans is caused by the protozoan parasite Plasmodium falciparum. The invasive form of malaria parasites is termed a merozoite and it employs an array of parasite proteins that bind to the host cell to mediate invasion. In Plasmodium falciparum, the erythrocyte binding-like (EBL) and reticulocyte binding-like (Rh) protein families are responsible for binding to specific erythrocyte receptors for invasion and mediating signalling events that initiate active entry of the malaria parasite. Here we have addressed the role of the cytoplasmic tails of these proteins in activating merozoite invasion after receptor engagement. We show that the cytoplasmic domains of these type 1 membrane proteins are phosphorylated in vitro. Depletion of PfCK2, a kinase implicated to phosphorylate these cytoplasmic tails, blocks P. falciparum invasion of red blood cells. We identify the crucial residues within the PfRh4 cytoplasmic domain that are required for successful parasite invasion. Live cell imaging of merozoites from these transgenic mutants show they attach but do not penetrate erythrocytes implying the PfRh4 cytoplasmic tail conveys signals important for the successful completion of the invasion process., Author Summary Malaria parasites must invade red blood cells to survive within the human host. Members of the erythrocyte binding-like (EBL) and reticulocyte binding-like (Rh) protein families, which are present at the apical tip of merozoites as single-pass transmembrane proteins, mediate recognition of red blood cells. Although extracellular domains of Plasmodium adhesins are required for binding red blood receptors, only the cytoplasmic region is in contact with the parasite’s cellular machinery to initiate invasion. Therefore any signal that is initiated upon binding must be communicated via the cytoplasmic domain to other targets within the malaria parasites. We investigate the role of adhesin phosphorylation in the P. falciparum invasion process. We show that the majority of adhesin cytoplasmic tails are phosphorylated in vitro. Mutational analyses provide identification of the important residues required for phosphorylation and suggest that PfCK2 may be responsible. Using a conditional knockdown line, we show that PfCK2 is essential for parasite growth and invasion. Using transgenic lines, we show that mutation of the PfRh4 cytoplasmic tail results in defects in parasite invasion. This work describes the critical residues important for signaling events and implicates PfCK2 as the essential kinase involved in P. falciparum invasion.

Published

2015

18. Plasmodium falciparum uses a key functional site in complement receptor type-1 for invasion of human erythrocytes

Author

Wai-Hong Tham, Sash Lopaticki, Alan F. Cowman, John P. Atkinson, Christoph Q. Schmidt, Richard E. Hauhart, Patience B. Tetteh-Quarcoo, Paul N. Barlow, and Mara Guariento

Subjects

Erythrocytes, Plasmodium falciparum, Immunology, Protozoan Proteins, chemical and pharmacologic phenomena, Complement receptor, Biochemistry, Host-Parasite Interactions, Red Cells, Iron, and Erythropoiesis, Complement Receptor Type 1, Humans, Malaria, Falciparum, biology, Complement component 2, CD46, Membrane Proteins, Cell Biology, Hematology, Recombinant Proteins, Receptors, Complement, Cell biology, Factor H, biology.protein, Alternative complement pathway, Complement membrane attack complex, Protein Binding, Complement control protein

Abstract

The Plasmodium falciparum adhesin PfRh4 binds to complement receptor type-1 (CR1) on human erythrocytes and mediates a glycophorin-independent invasion pathway. CR1 is a complement regulator and immune-adherence receptor on erythrocytes required for shuttling of C3b/C4b-opsonized particles to liver and spleen for phagocytosis. Using recombinant CR1 constructs, we mapped the recognition site for PfRh4 to complement control protein modules 1 to 3 (CCP1-3) at the membrane-distal amino terminus of CR1. This region of CR1 binds to C4b and C3b and accelerates decay of both classic pathway and alternative pathway C3 and C5 convertases. CCP1-3 competed for PfRh4 binding to erythroid CR1 and inhibited the PfRh4-CR1 invasion pathways across a wide range of P falciparum strains. PfRh4 did not bind significantly to other CR1 constructs, including CCP15-17, which is 85% identical to CCP1-3. PfRh4 binding to CR1 did not affect its C3b/C4b binding capability, and we show evidence for a ternary complex between CCP1-3, C4b, and PfRh4. PfRh4 binding specifically inhibited CR1's convertase decay-accelerating activity, whereas there was no effect on factor H-mediated decay-accelerating activity. These results increase our understanding of the functional implications of CR1 engagement with PfRh4 and highlight the interplay between complement regulation and infection.

Published

2011

19. Fine Mapping of Leishmania major Susceptibility Locus lmr2 and Evidence of a Role for Fli1 in Disease and Wound Healing

Author

Beena Kumar, Emanuela Handman, Sash Lopaticki, Anuratha Sakthianandeswaren, Tracey M. Baldwin, Simon J. Foote, Lukasz Kedzierski, Joan M Curtis, Gordon K. Smyth, and Colleen Elso

Subjects

Candidate gene, Immunology, Leishmaniasis, Cutaneous, Locus (genetics), Quantitative trait locus, Microbiology, Mice, Genetic linkage, Animals, Genetic Predisposition to Disease, Leishmania major, Allele, Promoter Regions, Genetic, Gene, Crosses, Genetic, Genetics, Mice, Inbred BALB C, Wound Healing, Host Response and Inflammation, Polymorphism, Genetic, biology, Proto-Oncogene Protein c-fli-1, Gene Expression Profiling, Chromosome Mapping, biology.organism_classification, Mice, Inbred C57BL, Gene expression profiling, Infectious Diseases, Genetic Loci, Female, Parasitology

Abstract

Genetic linkage studies of the host response to Leishmania major , the causative agent of cutaneous leishmaniasis, have identified significant genetic complexity in humans and mice. In the mouse model, multiple loci have been implicated in susceptibility to infection, but to date, the genes underlying these loci have not been identified. We now describe the contribution of a novel candidate gene, Fli1 , to both L. major resistance and enhanced wound healing. We have previously mapped the L. major response locus, lmr2 , to proximal chromosome 9 in a genetic cross between the resistant C57BL/6 strain and the susceptible BALB/c strain. We now show that the presence of the resistant C57BL/6 lmr2 allele in susceptible BALB/c mice confers an enhanced L. major resistance and wound healing phenotype. Fine mapping of the lmr2 locus permitted the localization of the lmr2 quantitative trait locus to a 5-Mb interval comprising 21 genes, of which microarray analysis was able to identify differential expression in 1 gene— Fli1 . Analysis of Fli1 expression in wounded and L. major -infected skin and naïve and infected lymph nodes validated the importance of Fli1 in lesion resolution and wound healing and identified 3 polymorphisms in the Fli1 promoter, among which a GA repeat element may be the important contributor.

Published

2010

20. Reticulocyte-binding protein homologue 5 – An essential adhesin involved in invasion of human erythrocytes by Plasmodium falciparum

Author

James G. Beeson, Lin Chen, Stuart A. Ralph, Alan F. Cowman, Michelle J. Boyle, Jake Baum, Sash Lopaticki, Julie Healer, Florian Ehlgen, and Tony Triglia

Subjects

Erythrocytes, Plasmodium falciparum, Antibodies, Protozoan, Receptors, Cell Surface, Biology, Host-Parasite Interactions, Tight Junctions, Apicomplexa, Mice, Microscopy, Electron, Transmission, Malaria Vaccines, Cell Adhesion, Animals, Humans, Apical membrane antigen 1, Receptor, Virulence, Rhoptry, Merozoites, Binding protein, biology.organism_classification, Virology, Transmembrane protein, Malaria, Protein Structure, Tertiary, Cell biology, Bacterial adhesin, Infectious Diseases, Parasitology, Rabbits, Carrier Proteins

Abstract

Invasion of erythrocytes is a prerequisite in the life history of the malaria parasite. Members of the reticulocyte-binding homologue family (PfRh) have been implicated in the invasion process and in some cases have been shown to act as adhesins, binding to specific receptors on the erythrocyte surface. We have identified a further, putatively essential, PfRh family member in the most virulent human malaria Plasmodium falciparum, called PfRh5, which binds to an unknown class of glycosylated receptors on the erythrocyte surface. This protein is an atypical PfRh family member, being much smaller than others and lacking a transmembrane and cytosolic region at the C-terminus. This suggests it may be part of a functional protein complex. PfRh5 localises to the rhoptries in merozoites and follows the tight junction during the process of erythrocyte invasion. Furthermore, rabbit immune serum raised against a portion of the ecto-domain, inhibits parasite invasion in vitro. We hypothesise an essential role for the PfRh5 adhesin in erythrocyte selection and commitment to invasion. Given its small size, we believe PfRh5 may prove to be a valuable candidate for inclusion in a multi-component anti-malarial vaccine.

Published

2009

21. An aspartyl protease defines a novel pathway for export of Toxoplasma proteins into the host cell

Author

Rebecca Stewart, Justin A Boddey, Magdalena Franco, Michael J Coffey, Alexandra L. Garnham, Michael W. Panas, Grant Dewson, David J. P. Ferguson, Brian J. Smith, John C. Boothroyd, Marta Enciso, Seth L. Masters, Matthew T. O'Neill, Brad E. Sleebs, Sash Lopaticki, Nicole D. Marino, Alessandro D. Uboldi, Christopher J. Tonkin, and Gordon K. Smyth

Subjects

Aspartic Acid Proteases, Virulence Factors, QH301-705.5, medicine.medical_treatment, Science, Protozoan Proteins, Virulence, Vacuole, General Biochemistry, Genetics and Molecular Biology, Gene expression, parasitic diseases, medicine, Humans, Biology (General), Cells, Cultured, Microbiology and Infectious Disease, Protease, General Immunology and Microbiology, biology, Effector, General Neuroscience, Toxoplasma gondii, Plasmodium falciparum, protease, General Medicine, Fibroblasts, biology.organism_classification, Cell biology, Transport protein, Protein Transport, effector, Medicine, Other, Protein Processing, Post-Translational, Toxoplasma, export, Gene Deletion, Research Article

Abstract

Infection by Toxoplasma gondii leads to massive changes to the host cell. Here, we identify a novel host cell effector export pathway that requires the Golgi-resident aspartyl protease 5 (ASP5). We demonstrate that ASP5 cleaves a highly constrained amino acid motif that has similarity to the PEXEL-motif of Plasmodium parasites. We show that ASP5 matures substrates at both the N- and C-terminal ends of proteins and also controls trafficking of effectors without this motif. Furthermore, ASP5 controls establishment of the nanotubular network and is required for the efficient recruitment of host mitochondria to the vacuole. Assessment of host gene expression reveals that the ASP5-dependent pathway influences thousands of the transcriptional changes that Toxoplasma imparts on its host cell. All these changes result in attenuation of virulence of Δasp5 tachyzoites in vivo. This work characterizes the first identified machinery required for export of Toxoplasma effectors into the infected host cell. DOI: http://dx.doi.org/10.7554/eLife.10809.001, eLife digest Toxoplasma gondii is a parasite that is thought to infect over two billion people worldwide. Often these infections cause no noticeable symptoms, but can cause serious illness in people with weakened immune systems. Toxoplasma parasites must enter human cells in order to survive. To dramatically increase their chances of survival, the parasites then deliver specialized proteins into the host cell that disarm the host’s immune defenses. Understanding how these specialized proteins are transported from inside the parasite into the host cell, and how this process can be blocked, may lead to new treatments for these and related parasitic infections. By genetically modifying Toxoplasma parasites to lack a parasite enzyme, Coffey et al. have now discovered that this molecule is required for correctly transporting parasite proteins. This enzyme is called aspartyl protease 5 (ASP5) and is found in the parasite in a structure called the Golgi apparatus, which acts as a main hub for protein transport. ASP5 cuts proteins at a ‘barcode’ that is found in many different types of proteins, priming them for transport out of the parasite and for export into the host cell in some cases. Coffey et al. show that in parasites that lack ASP5, these proteins are no longer cleaved and are not transported correctly, blocking the activities that parasites normally perform to ensure their survival. Therefore, ASP5 plays an important role in transporting a wide range of proteins associated with disease, including transporting certain proteins directly into the host cell. Future studies that compare parasites that lack ASP5 to normal parasites will aim to identify new proteins used by the parasites to defeat the host’s immune defenses. DOI: http://dx.doi.org/10.7554/eLife.10809.002

Published

2015

22. Author response: An aspartyl protease defines a novel pathway for export of Toxoplasma proteins into the host cell

Author

Rebecca Stewart, Brad E. Sleebs, Magdalena Franco, Seth L. Masters, Justin A Boddey, Marta Enciso, Michael W. Panas, Michael J Coffey, Grant Dewson, Brian J. Smith, Matthew T. O'Neill, Sash Lopaticki, Nicole D. Marino, Alessandro D. Uboldi, Christopher J. Tonkin, David J. P. Ferguson, Gordon K. Smyth, Alexandra L. Garnham, and John C. Boothroyd

Subjects

Aspartate protease, Biology, Cell biology

Published

2015

23. Persistence of recipient lymphocytes in NOD mice after irradiation and bone marrow transplantation

Author

Leonard C. Harrison, Raymond J. Steptoe, Grant Morahan, Sanda Stankovic, Lynelle K. Jones, and Sash Lopaticki

Subjects

Isoantigens, Adoptive cell transfer, Transplantation Conditioning, Myeloid, Immunology, Nod, Biology, Radiation Tolerance, Mice, Mice, Inbred NOD, medicine, Animals, Immunology and Allergy, Lymphocytes, Bone Marrow Transplantation, NOD mice, Protein Tyrosine Phosphatase, Non-Receptor Type 1, Graft Survival, medicine.disease, Hematopoiesis, Haematopoiesis, Diabetes Mellitus, Type 1, medicine.anatomical_structure, Radiation Chimera, Leukocyte Common Antigens, Bone marrow, Insulitis

Abstract

The non-obese diabetic (NOD) mouse is a unique and invaluable model of autoimmune disease, in particular type 1 diabetes. Bone marrow transplantation as a therapy for type 1 diabetes has been explored in NOD mice. NOD mice require higher doses of conditioning irradiation for successful allogeneic bone marrow transplantation, suggesting that NOD hematopoietic cells are radioresistant compared to those of other mouse strains. However, studies of hematopoietic reconstitution in NOD mice are hampered by the lack of mice bearing a suitable cell-surface marker that would allow transferred cells or their progeny to be distinguished. In order to monitor hematopoietic reconstitution in NOD mice we generated congenic NOD mice that carry the alternative allelic form of the pan-leukocyte alloantigen CD45. Following irradiation and congenic bone marrow transplantation, we found that the myeloid lineage was rapidly reconstituted by cells of donor origin but substantial numbers of recipient T lymphocytes persisted even after supra-lethal irradiation. This indicates that radiation resistance in the NOD hematopoietic compartment is a property primarily of mature T lymphocytes.

Published

2004

24. Genetic analysis of stress responsiveness in a mouse model

Author

Magdalena Kita, Mark Murphy, Yvette M. Wilson, Grant Morahan, Rebecca E. Newman, and Sash Lopaticki

Subjects

Genetics, Communication, business.industry, Genome Scan, Quantitative trait locus, Phenotype, Genetic analysis, Genome, Genotype, business, Psychology, Gene, General Psychology, Chromosome 12

Abstract

The purpose of the present paper was to look for genes that might be involved in anxiety-related behaviours by undertaking a genetic analysis of a simple mouse model of stress responsiveness. Two inbred mouse strains have been identified that show either high or low stress responsiveness. These strains were crossed to generate F1 progeny, which were then crossed to generate F2 progeny, and in which there is segregation of genotype within individual animals. DNA was isolated from these animals and a genome scan was conducted in order to find regions on the genome that correlate with the stress responsiveness. Several regions on the mouse genome show significant linkage with the stress phenotype. One region in particular, on chromosome 12, was further characterised and the most significant linkage was found between 32.8 and 44.8 cM. These chromosomal regions may contain genes encoding proteins that are involved in the underlying neural circuitry involved in stress responsiveness.

Published

2004

25. Transition state mimetics of the Plasmodium export element are potent inhibitors of Plasmepsin V from P. falciparum and P. vivax

Author

Brad E. Sleebs, Matthew T. O'Neill, Pravin Rajasekaran, Sash Lopaticki, Kym N Lowes, Brian J. Smith, Kurt Lackovic, Alan F. Cowman, Justin A Boddey, and Michelle Gazdik

Subjects

Models, Molecular, Erythrocytes, Protein Conformation, Proteolysis, Plasmodium vivax, Plasmodium falciparum, Plasmodium, Cell Line, Structure-Activity Relationship, Protein structure, Biomimetic Materials, parasitic diseases, Drug Discovery, medicine, Structure–activity relationship, Aspartic Acid Endopeptidases, Humans, Protease Inhibitors, chemistry.chemical_classification, medicine.diagnostic_test, biology, Endoplasmic reticulum, biology.organism_classification, Virology, Enzyme, Biochemistry, chemistry, Molecular Medicine

Abstract

Following erythrocyte invasion, malaria parasites export a catalogue of remodeling proteins into the infected cell that enable parasite development in the human host. Export is dependent on the activity of the aspartyl protease, plasmepsin V (PMV), which cleaves proteins within the Plasmodium export element (PEXEL; RxL↓xE/Q/D) in the parasite's endoplasmic reticulum. Here, we generated transition state mimetics of the native PEXEL substrate that potently inhibit PMV isolated from Plasmodium falciparum and Plasmodium vivax. Through optimization, we identified that the activity of the mimetics was completely dependent on the presence of P1 Leu and P3 Arg. Treatment of P. falciparum-infected erythrocytes with a set of optimized mimetics impaired PEXEL processing and killed the parasites. The striking effect of the compounds provides a clearer understanding of the accessibility of the PMV active site and reaffirms the enzyme as an attractive target for the design of future antimalarials.

Published

2014

26. Plasmodium falciparum is dependent on de novo myo-inositol biosynthesis for assembly of GPI glycolipids and infectivity

Author

James I, Macrae, Sash, Lopaticki, Alexander G, Maier, Thusitha, Rupasinghe, Amsha, Nahid, Alan F, Cowman, and Malcolm J, McConville

Subjects

Erythrocytes, Isotope Labeling, Plasmodium falciparum, Glucose-6-Phosphate, Humans, Glycolipids, GPI-Linked Proteins, Inositol

Abstract

Intra-erythrocytic stages of the malaria parasite, Plasmodium falciparum, are thought to be dependent on de novo synthesis of phosphatidylinositol, as red blood cells (RBC) lack the capacity to synthesize this phospholipid. The myo-inositol headgroup of PI can either be synthesized de novo or scavenged from the RBC. An untargeted metabolite profiling of P. falciparum infected RBC showed that trophozoite and schizont stages accumulate high levels of myo-inositol-3-phosphate, indicating increased de novo biosynthesis of myo-inositol from glucose 6-phosphate. Metabolic labelling studies with (13) C-U-glucose in the presence and absence of exogenous inositol confirmed that de novo myo-inositol synthesis occurs in parallel with myo-inositol salvage pathways. Unexpectedly, while both endogenous and scavenged myo-inositol was used to synthesize bulk PI, only de novo-synthesized myo-inositol was incorporated into GPI glycolipids. Moreover, gene disruption studies suggested that the INO1 gene, encoding myo-inositol 3-phosphate synthase, is essential in asexual parasite stages. Together these findings suggest that P. falciparum asexual stages are critically dependent on de novo myo-inositol biosynthesis for assembly of a sub-pool of PI species and GPI biosynthesis. These findings highlight unexpected complexity in phospholipid biosynthesis in P. falciparum and a lack of redundancy in some nutrient salvage versus endogenous biosynthesis pathways.

Published

2013

27. Characterization of pathotype-specific epitopes of Newcastle disease virus fusion glycoproteins by matrix-assisted laser desorption/ionization time-of-flight mass spectrometry and post-source decay sequencing

Author

Jeffrey J. Gorman, Christopher J. Morrow, and Sash Lopaticki

Subjects

chemistry.chemical_classification, Matrix-assisted laser desorption/ionization, chemistry.chemical_compound, Glycosylation, chemistry, Biochemistry, Protein primary structure, Glycoprotein, Mass spectrometry, Fusion protein, Peptide sequence, Spectroscopy, Amino acid

Abstract

Matrix-assisted laser desorption/ionization (MALDI) time-of-flight (TOF) mass spectrometry (MS) was used to characterize the F2 polypeptide of the fusion (F) protein of an avirulent isolate (VRI 82-6409) of Newcastle disease virus (NDV) that was previously identified by immunochemical screening as having a variant cleavage activation sequence in its fusion protein precursor (F0). The major glycoform of the intact F2 polypeptide of the VRI 82-6409 isolate was 89 Da smaller than the F2 polypeptide of the avirulent V4 isolate of the Queensland strain of NDV. Analysis of AspN protease digests of the F2 polypeptides by MALDI/TOF-MS, with and without high-performance liquid chromatographic (HPLC) separation, showed this mass difference to be due to a combination of differences in the extents of glycosylation and an amino acid difference in the AspN peptides derived from the C-termini of the F2 polypeptides. Accuracies achieved in analysis of the AspN peptides allowed the identification of this amino acid difference as glutamic acid in the VRI 82-6409 isolate compared with glycine in the V4 isolate. Analysis of fragments formed by post-source decay (PSD) of ions of the C-terminal AspN peptides localized the difference to the C-terminal residues of the respective F2 polypeptides. The present study demonstrated that MALDI/TOF-MS is a highly effective technique for the characterization of NDV variants identified by immunochemical screening of pathotype-specific epitopes at the C-termini of their F2 polypeptides.

Published

1998

28. The stretcher spontaneous neurodegenerative mutation models Charcot-Marie-Tooth disease type 4D

Author

Dexing Huang, Trevor J. Kilpatrick, Dora Angelicheva, Rosalind Hm King, Luba Kalaydjieva, David Chandler, Grant Morahan, Michael Hunter, and Sash Lopaticki

Subjects

Candidate gene, Mutant, Biology, medicine.disease_cause, Peripheral Neuropathies, General Biochemistry, Genetics and Molecular Biology, Neurobiology of Disease & Regeneration, 03 medical and health sciences, Chromosome 15, Exon, 0302 clinical medicine, Gene mapping, medicine, General Pharmacology, Toxicology and Pharmaceutics, Neurogenetics, Gene, NDRG1 Gene, 030304 developmental biology, Genetics, 0303 health sciences, Mutation, General Immunology and Microbiology, General Medicine, Articles, 030217 neurology & neurosurgery, Research Article

Abstract

Mice affected by a spontaneous mutation which arose within our colony exhibited a neuromuscular phenotype involving tremor and characteristic stretching of the rear limbs. The mutant, namedstretcher, was used to breed a backcross cohort for genetic mapping studies. The gene responsible for the mutant phenotype was mapped to a small region on mouse chromosome 15, with a LOD score above 20. Candidate genes within the region included theNdrg1gene. Examination of this gene in the mutant mouse strain revealed that exons 10 to 14 had been deleted. Mutations in the human orthologue are known to result in Charcot-Marie-Tooth disease type 4D (CMT4D) a severe early-onset disorder involving Schwann cell dysfunction and extensive demyelination. Thestretchermutant mouse is more severely affected than mice in which theNdrg1gene had been knocked out by homologous recombination. Our results demonstrate that theNdrg1strmutation provides a new model for CMT4D, and demonstrate that exons 10 to 14 ofNdrg1encode amino acids crucial to the appropriate function of Ndrg1 in the central nervous system.

Published

2013

29. The stretcher spontaneous neurodegenerative mutation models Charcot-Marie-Tooth disease type 4D [v1; ref status: indexed, http://f1000r.es/8c]

Author

David Chandler, Sash Lopaticki, Dexing Huang, Michael Hunter, Dora Angelicheva, Trevor Kilpatrick, Rosalind HM King, Luba Kalaydjieva, and Grant Morahan

Subjects

lcsh:R, lcsh:Medicine, lcsh:Q, Neurogenetics, Peripheral Neuropathies, lcsh:Science, Neurobiology of Disease & Regeneration

Abstract

Mice affected by a spontaneous mutation which arose within our colony exhibited a neuromuscular phenotype involving tremor and characteristic stretching of the rear limbs. The mutant, named stretcher, was used to breed a backcross cohort for genetic mapping studies. The gene responsible for the mutant phenotype was mapped to a small region on mouse chromosome 15, with a LOD score above 20. Candidate genes within the region included the Ndrg1 gene. Examination of this gene in the mutant mouse strain revealed that exons 10 to 14 had been deleted. Mutations in the human orthologue are known to result in Charcot-Marie-Tooth disease type 4D (CMT4D) a severe early-onset disorder involving Schwann cell dysfunction and extensive demyelination. The stretcher mutant mouse is more severely affected than mice in which the Ndrg1 gene had been knocked out by homologous recombination. Our results demonstrate that the Ndrg1str mutation provides a new model for CMT4D, and demonstrate that exons 10 to 14 of Ndrg1 encode amino acids crucial to the appropriate function of Ndrg1 in the central nervous system.

Published

2013

30. Role of plasmepsin V in export of diverse protein families from the Plasmodium falciparum exportome

Author

Teresa Carvalho, Anthony N. Hodder, Alan F. Cowman, Justin A Boddey, Danushka S. Marapana, Thomas Nebl, Brad E. Sleebs, Sash Lopaticki, and Tobias Sargeant

Subjects

Erythrocytes, Protein family, Virulence Factors, Amino Acid Motifs, Plasmodium falciparum, Plasmepsin, Protozoan Proteins, Antigens, Protozoan, Endoplasmic Reticulum, Biochemistry, Plasmodium, Protein structure, Structural Biology, parasitic diseases, Genetics, Aspartic Acid Endopeptidases, Humans, Molecular Biology, Chromatography, High Pressure Liquid, biology, Effector, Endoplasmic reticulum, Computational Biology, Membrane Proteins, Cell Biology, biology.organism_classification, Protein Structure, Tertiary, Membrane protein, Carrier Proteins, Software, Subcellular Fractions

Abstract

Plasmodium falciparum exports several hundred effector proteins that remodel the host erythrocyte and enable parasites to acquire nutrients, sequester in the circulation and evade immune responses. The majority of exported proteins contain the Plasmodium export element (PEXEL; RxLxE/Q/D) in their N-terminus, which is proteolytically cleaved in the parasite endoplasmic reticulum by Plasmepsin V, and is necessary for export. Several exported proteins lack a PEXEL or contain noncanonical motifs. Here, we assessed whether Plasmepsin V could process the N-termini of diverse protein families in P. falciparum. We show that Plasmepsin V cleaves N-terminal sequences from RIFIN, STEVOR and RESA multigene families, the latter of which contain a relaxed PEXEL (RxLxxE). However, Plasmepsin V does not cleave the N-terminal sequence of the major exported virulence factor erythrocyte membrane protein 1 (PfEMP1) or the PEXEL-negative exported proteins SBP-1 or REX-2. We probed the substrate specificity of Plasmepsin V and determined that lysine at the PEXEL P3 position, which is present in PfEMP1 and other putatively exported proteins, blocks Plasmepsin V activity. Furthermore, isoleucine at position P1 also blocked Plasmepsin V activity. The specificity of Plasmepsin V is therefore exquisitely confined and we have used this novel information to redefine the predicted P. falciparum PEXEL exportome.

Published

2012

31. Reticulocyte and Erythrocyte Binding-Like Proteins Function Cooperatively in Invasion of Human Erythrocytes by Malaria Parasites▿ ‡

Author

Wai-Hong Tham, Jennifer K. Thompson, Sash Lopaticki, James G. Beeson, Alex Gout, Tony Triglia, Alan F. Cowman, Terence P. Speed, Danny W. Wilson, Julie Healer, and Alexander G. Maier

Subjects

Erythrocytes, Reticulocytes, Protein family, Immunology, Immunoblotting, Plasmodium falciparum, Protozoan Proteins, Antibodies, Protozoan, Enzyme-Linked Immunosorbent Assay, Biology, Transfection, Microbiology, law.invention, Gene Knockout Techniques, Antigen, law, parasitic diseases, Malaria Vaccines, Animals, Humans, Malaria vaccine, Reverse Transcriptase Polymerase Chain Reaction, Binding protein, Glycophorin C, biology.organism_classification, Molecular biology, Coculture Techniques, Malaria, Infectious Diseases, Microbial Immunity and Vaccines, biology.protein, Recombinant DNA, Parasitology, Rabbits, Antibody

Abstract

Plasmodium falciparum causes the most severe form of malaria in humans and invades erythrocytes using multiple ligand-receptor interactions. Two important protein families involved in erythrocyte binding are the erythrocyte binding-like (EBL) and the reticulocyte binding-like (RBL or P. falciparum Rh [PfRh]) proteins. We constructed P. falciparum lines lacking expression of EBL proteins by creating single and double knockouts of the corresponding genes for eba-175 , eba-181 , and eba-140 and show that the EBL and PfRh proteins function cooperatively, consistent with them playing a similar role in merozoite invasion. We provide evidence that PfRh and EBL proteins functionally interact, as loss of function of EBA-181 ablates the ability of PfRh2a/b protein antibodies to inhibit merozoite invasion. Additionally, loss of function of some ebl genes results in selection for increased transcription of the PfRh family. This provides a rational basis for considering PfRh and EBL proteins for use as a combination vaccine against P. falciparum . We immunized rabbits with combinations of PfRh and EBL proteins to test the ability of antibodies to block merozoite invasion in growth inhibition assays. A combination of EBA-175, PfRh2a/b, and PfRh4 recombinant proteins induced antibodies that potently blocked merozoite invasion. This validates the use of a combination of these ligands as a potential vaccine that would have broad activity against P. falciparum .

Published

2010

32. Ndrg1 in development and maintenance of the myelin sheath

Author

Tomohiko Okuda, Dexing Huang, Rosalind H.M. King, Trevor J. Kilpatrick, Julian Blake, Kim W. Carter, David Chandler, Luba Kalaydjieva, Grant Morahan, Michael Hunter, J. R. Muddle, Sash Lopaticki, Dora Angelicheva, Toshiyuki Miyata, and Michelle Nourallah

Subjects

Mouse, Blotting, Western, Axonal loss, Schwann cell, Gene Expression, Cell Cycle Proteins, Biology, lcsh:RC321-571, Myelin, Mice, Peripheral nerve, CMT4D, Charcot-Marie-Tooth Disease, medicine, Animals, Axon, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Myelin Sheath, Regulation of gene expression, Mice, Knockout, Intracellular Signaling Peptides and Proteins, Phenotype, Sciatic Nerve, Cell biology, Gene expression profiling, Electrophysiology, Disease Models, Animal, medicine.anatomical_structure, Neurology, Refsum Disease, Sciatic nerve, Schwann Cells, Demyelination, Neuroscience, Demyelinating Diseases

Abstract

CMT4D disease is a severe autosomal recessive demyelinating neuropathy with extensive axonal loss leading to early disability, caused by mutations in the N-myc downstream regulated gene 1 (NDRG1). NDRG1 is expressed at particularly high levels in the Schwann cell (SC), but its physiological function(s) are unknown. To help with their understanding, we characterise the phenotype of a new mouse model, stretcher (str), with total Ndrg1 deficiency, in comparison with the hypomorphic Ndrg1 knock-out (KO) mouse. While both models display normal initial myelination and a transition to overt pathology between weeks 3 and 5, the markedly more severe str phenotype suggests that even low Ndrg1 expression results in significant phenotype rescue. Neither model replicates fully the features of CMT4D: although axon damage is present, regenerative capacity is unimpaired and the mice do not display the early severe axonal loss typical of the human disease. The widespread large fibre demyelination coincides precisely with the period of rapid growth of the animals and the dramatic (160–500-fold) increase in myelin volume and length in large fibres. This is followed by stabilisation after week 10, while small fibres remain unaffected. Gene expression profiling of str peripheral nerve reveals non-specific secondary changes at weeks 5 and 10 and preliminary data point to normal proteasomal function. Our findings do not support the proposed roles of NDRG1 in growth arrest, terminal differentiation, gene expression regulation and proteasomal degradation. Impaired SC trafficking failing to meet the considerable demands of nerve growth, emerges as the likely pathogenetic mechanism in NDRG1 deficiency.

Published

2010

33. Complement receptor 1 is the host erythrocyte receptor for Plasmodium falciparum PfRh4 invasion ligand

Author

Paul N. Barlow, Alan F. Cowman, Christoph Q. Schmidt, Sash Lopaticki, Dave Richard, Wai-Hong Tham, Danny W. Wilson, James G. Beeson, Patience B. Tetteh-Quarcoo, and Jason Corbin

Subjects

Erythrocytes, Complement receptor 1, Plasmodium falciparum, Protozoan Proteins, malaria, Plasma protein binding, red blood cell, chemistry.chemical_compound, parasitic diseases, medicine, Animals, Humans, Parasite hosting, Receptor, General, Multidisciplinary, biology, Intracellular parasite, Membrane Proteins, Biological Sciences, biology.organism_classification, N-Acetylneuraminic Acid, Recombinant Proteins, merozoite, Receptors, Complement, Cell biology, Red blood cell, reticulocyte-binding-like homologue, medicine.anatomical_structure, chemistry, biology.gene, N-Acetylneuraminic acid, Protein Binding

Abstract

Plasmodium falciparum is responsible for the most severe form of malaria disease in humans, causing more than 1 million deaths each year. As an obligate intracellular parasite, P. falciparum ’s ability to invade erythrocytes is essential for its survival within the human host. P. falciparum invades erythrocytes using multiple host receptor–parasite ligand interactions known as invasion pathways. Here we show that CR1 is the host erythrocyte receptor for PfRh4, a major P. falciparum ligand essential for sialic acid–independent invasion. PfRh4 and CR1 interact directly, with a K d of 2.9 μM. PfRh4 binding is strongly correlated with the CR1 level on the erythrocyte surface. Parasite invasion via sialic acid–independent pathways is reduced in low-CR1 erythrocytes due to limited availability of this receptor on the surface. Furthermore, soluble CR1 can competitively block binding of PfRh4 to the erythrocyte surface and specifically inhibit sialic acid–independent parasite invasion. These results demonstrate that CR1 is an erythrocyte receptor used by the parasite ligand PfRh4 for P. falciparum invasion.

Published

2010

34. Plasmepsin V, a Secret Weapon Against Malaria

Author

Kym N Lowes, Lea Barfod, Danushka S. Marapana, Brad E. Sleebs, Michelle Gazdik, Alan F. Cowman, Anthony N. Hodder, Pravin Rajasekaran, Sash Lopaticki, Brian J. Smith, Lars Hviid, Matthew T. O'Neill, Justin A Boddey, Svenja Günther, Philip J. Shaw, and Lachlan Whitehead

Subjects

Erythrocytes, Plasmodium vivax, Gene Identification and Analysis, Protozoan Proteins, Plasmepsin, Pathogenesis, Endoplasmic Reticulum, Pathology and Laboratory Medicine, Biochemistry, Molecular Cell Biology, Drug Discovery, Medicine and Health Sciences, Aspartic Acid Endopeptidases, Plasmodium Vivax, Biology (General), Mathematical Computing, Protozoans, Sulfonamides, biology, General Neuroscience, Malarial Parasites, Enzymes, 3. Good health, Transport protein, Plasmodium Falciparum, Protein Transport, Chemistry, Infectious Diseases, Medical Microbiology, Host-Pathogen Interactions, Physical Sciences, Synopsis, General Agricultural and Biological Sciences, Oligopeptides, Research Article, Signal peptide, Cell Physiology, Computer and Information Sciences, Proteases, Drug Research and Development, Aspartic Acid Proteases, Infectious Disease Control, QH301-705.5, Virulence, Microbiology, General Biochemistry, Genetics and Molecular Biology, Molecular Genetics, Chemical Biology, parasitic diseases, Genetics, Parasitic Diseases, Humans, Enzyme Kinetics, Pharmacology, General Immunology and Microbiology, Organisms, Biology and Life Sciences, Plasmodium falciparum, Cell Biology, biology.organism_classification, Computing Methods, Virology, Parasitic Protozoans, Malaria, Bacterial adhesin, Membrane Trafficking, Mutagenesis, Mutation, Enzymology, Parasitology, Gene Function, Mathematics

Abstract

A small molecule inhibitor of the malarial protease Plasmepsin V impairs protein export and cellular remodeling, reducing parasite survival in human erythrocytes., The malaria parasite Plasmodium falciparum exports several hundred proteins into the infected erythrocyte that are involved in cellular remodeling and severe virulence. The export mechanism involves the Plasmodium export element (PEXEL), which is a cleavage site for the parasite protease, Plasmepsin V (PMV). The PMV gene is refractory to deletion, suggesting it is essential, but definitive proof is lacking. Here, we generated a PEXEL-mimetic inhibitor that potently blocks the activity of PMV isolated from P. falciparum and Plasmodium vivax. Assessment of PMV activity in P. falciparum revealed PEXEL cleavage occurs cotranslationaly, similar to signal peptidase. Treatment of P. falciparum–infected erythrocytes with the inhibitor caused dose-dependent inhibition of PEXEL processing as well as protein export, including impaired display of the major virulence adhesin, PfEMP1, on the erythrocyte surface, and cytoadherence. The inhibitor killed parasites at the trophozoite stage and knockdown of PMV enhanced sensitivity to the inhibitor, while overexpression of PMV increased resistance. This provides the first direct evidence that PMV activity is essential for protein export in Plasmodium spp. and for parasite survival in human erythrocytes and validates PMV as an antimalarial drug target., Author Summary To survive within human red blood cells, malaria parasites must export a catalog of proteins that remodel the host cell and its surface. This enables parasites to acquire nutrients from outside the cell and to modify the cell surface in order to evade host defenses. Protein export involves proteolytic cleavage of the Plasmodium Export Element (PEXEL) by the aspartyl protease Plasmepsin V. We report here the development of a small molecule inhibitor that closely mimics the natural PEXEL substrate and blocks the activity of Plasmepsin V from the malarial parasites Plasmodium falciparum and Plasmodium vivax. The inhibitor impairs export and cellular remodeling and kills P. falciparum at the ring-trophozoite transition, providing direct evidence that Plasmepsin V activity is essential for export of PEXEL proteins and parasite survival within the host. These findings validate Plasmepsin V as a highly conserved antimalarial drug target.

Published

2014

35. An EGF-like Protein Forms a Complex with PfRh5 and Is Required for Invasion of Human Erythrocytes by Plasmodium falciparum

Author

Stuart A. Ralph, Sash Lopaticki, Alex D. Uboldi, Chaitali Dekiwadia, Alan F. Cowman, Matthew T. O'Neill, Dave Richard, David T. Riglar, Lin Chen, Wai-Hong Tham, and Jake Baum

Subjects

Erythrocytes, Protein family, QH301-705.5, Immunoprecipitation, Plasmodium falciparum, Immunology, Protozoan Proteins, Microbiology, Reticulocyte, Epidermal growth factor, Virology, Genetics, medicine, Animals, Humans, Biology (General), Receptor, Biology, Molecular Biology, Epidermal Growth Factor, biology, Rhoptry, Merozoites, RC581-607, biology.organism_classification, Cell biology, medicine.anatomical_structure, biology.protein, Parasitology, Immunologic diseases. Allergy, Antibody, Carrier Proteins, Research Article

Abstract

Invasion of erythrocytes by Plasmodium falciparum involves a complex cascade of protein-protein interactions between parasite ligands and host receptors. The reticulocyte binding-like homologue (PfRh) protein family is involved in binding to and initiating entry of the invasive merozoite into erythrocytes. An important member of this family is PfRh5. Using ion-exchange chromatography, immunoprecipitation and mass spectroscopy, we have identified a novel cysteine-rich protein we have called P. falciparum Rh5 interacting protein (PfRipr) (PFC1045c), which forms a complex with PfRh5 in merozoites. Mature PfRipr has a molecular weight of 123 kDa with 10 epidermal growth factor-like domains and 87 cysteine residues distributed along the protein. In mature schizont stages this protein is processed into two polypeptides that associate and form a complex with PfRh5. The PfRipr protein localises to the apical end of the merozoites in micronemes whilst PfRh5 is contained within rhoptries and both are released during invasion when they form a complex that is shed into the culture supernatant. Antibodies to PfRipr1 potently inhibit merozoite attachment and invasion into human red blood cells consistent with this complex playing an essential role in this process., Author Summary The malaria parasite invades red blood cells by binding to proteins on the surface of this host cell. A family of proteins called P. falciparum reticulocyte binding-like homologue (PfRh) proteins are important for recognition of the red blood cell and activation of the invasion process. An important member of the PfRh family is PfRh5. We have identified a novel cysteine-rich protein we have called P. falciparum Rh5 interacting protein (PfRipr), which forms a complex with PfRh5 in merozoites. PfRipr has 10 epidermal growth factor-like domains and is expressed in mature schizont stages where it is processed into two polypeptides that associate and form a complex with PfRh5. The PfRipr protein localises to the apical end of the merozoites in micronemes whilst PfRh5 is contained within rhoptries and both are released during invasion when they form a complex that is released into the culture supernatant. Antibodies to PfRipr1 can potently inhibit merozoite attachment and invasion into human red blood cells consistent with this complex playing an essential role in this process.

Published

2011

36. Plasmodium falciparum Merozoite Invasion Is Inhibited by Antibodies that Target the PfRh2a and b Binding Domains

Author

David T. Riglar, Chaitali Dekiwadia, Sash Lopaticki, Stuart A. Ralph, Anthony N. Hodder, Jake Baum, Lin Chen, Tony Triglia, and Alan F. Cowman

Subjects

lcsh:Immunologic diseases. Allergy, Erythrocytes, medicine.drug_class, Molecular Sequence Data, Plasmodium falciparum, Immunology, Protein domain, Protozoan Proteins, Antibodies, Protozoan, Plasma protein binding, Monoclonal antibody, Microbiology, Mice, 03 medical and health sciences, Reticulocyte, Virology, Genetics, medicine, Animals, Humans, Protein Interaction Domains and Motifs, lcsh:QH301-705.5, Biology, Molecular Biology, Cells, Cultured, 030304 developmental biology, 0303 health sciences, biology, Merozoites, 030306 microbiology, Glycophorin C, biology.organism_classification, Molecular biology, Endocytosis, 3. Good health, medicine.anatomical_structure, lcsh:Biology (General), Ectodomain, biology.protein, Medicine, Parasitology, Rabbits, Antibody, lcsh:RC581-607, Protein Binding, Research Article

Abstract

Plasmodium falciparum, the causative agent of the most severe form of malaria in humans invades erythrocytes using multiple ligand-receptor interactions. The P. falciparum reticulocyte binding-like homologue proteins (PfRh or PfRBL) are important for entry of the invasive merozoite form of the parasite into red blood cells. We have analysed two members of this protein family, PfRh2a and PfRh2b, and show they undergo a complex series of proteolytic cleavage events before and during merozoite invasion. We show that PfRh2a undergoes a cleavage event in the transmembrane region during invasion consistent with activity of the membrane associated PfROM4 protease that would result in release of the ectodomain into the supernatant. We also show that PfRh2a and PfRh2b bind to red blood cells and have defined the erythrocyte-binding domain to a 15 kDa region at the N-terminus of each protein. Antibodies to this receptor-binding region block merozoite invasion demonstrating the important function of this domain. This region of PfRh2a and PfRh2b has potential in a combination vaccine with other erythrocyte binding ligands for induction of antibodies that would block a broad range of invasion pathways for P. falciparum into human erythrocytes., Author Summary The causative agent of the most severe form of malaria in humans is the protozoan parasite Plasmodium falciparum. These parasites are carried by a mosquito that infects humans during feeding resulting in injection of sporozoite forms that infect and develop in the liver into the merozoite stage. The merozoites are released into the blood stream where they invade erythrocytes in which they can grow and divide. Invasion of the red blood cell by P. falciparum merozoites involves a cascade of protein-protein interactions. The P. falciparum reticulocyte binding-like homologue proteins (PfRh or PfRBL) are an important protein family involved in binding to specific receptors on the red blood cell. We have analysed two members of this protein family, PfRh2a and PfRh2b, and show that they undergo a complex series of cleavage events before and during merozoite invasion. We have defined the region of these ligands that bind red blood cells and show that antibodies to this receptor-binding region block merozoite invasion demonstrating the important function of this domain.

Published

2011