Your search keyword '"Tony Triglia"' showing total 23 results

1. Plasmepsin X activates the PCRCR complex of Plasmodium falciparum by processing PfRh5 for erythrocyte invasion

Author

Tony Triglia, Stephen W. Scally, Benjamin A. Seager, Michał Pasternak, Laura F. Dagley, and Alan F. Cowman

Subjects

Science

Abstract

Abstract Plasmodium falciparum causes the most severe form of malaria in humans. The protozoan parasite develops within erythrocytes to mature schizonts, that contain more than 16 merozoites, which egress and invade fresh erythrocytes. The aspartic protease plasmepsin X (PMX), processes proteins and proteases essential for merozoite egress from the schizont and invasion of the host erythrocyte, including the leading vaccine candidate PfRh5. PfRh5 is anchored to the merozoite surface through a 5-membered complex (PCRCR), consisting of Plasmodium thrombospondin-related apical merozoite protein, cysteine-rich small secreted protein, Rh5-interacting protein and cysteine-rich protective antigen. Here, we show that PCRCR is processed by PMX in micronemes to remove the N-terminal prodomain of PhRh5 and this activates the function of the complex unmasking a form that can bind basigin on the erythrocyte membrane and mediate merozoite invasion. The ability to activate PCRCR at a specific time in merozoite invasion most likely masks potential deleterious effects of its function until they are required. These results provide an important understanding of the essential role of PMX and the fine regulation of PCRCR function in P. falciparum biology.

Published

2023

2. RhopH2 and RhopH3 export enables assembly of the RhopH complex on P. falciparum-infected erythrocyte membranes

Author

Michał Pasternak, Julie M. J. Verhoef, Wilson Wong, Tony Triglia, Michael J. Mlodzianoski, Niall Geoghegan, Cindy Evelyn, Ahmad Z. Wardak, Kelly Rogers, and Alan F. Cowman

Subjects

Biology (General), QH301-705.5

Abstract

While RhopH3 is necessary for host invasion by Plasmodium falciparum parasites, the complete RhopH complex involved in parasite nutrient uptake only incorporates into the host membrane after merozoite invasion.

Published

2022

3. 4D analysis of malaria parasite invasion offers insights into erythrocyte membrane remodeling and parasitophorous vacuole formation

Author

Niall D. Geoghegan, Cindy Evelyn, Lachlan W. Whitehead, Michal Pasternak, Phoebe McDonald, Tony Triglia, Danushka S. Marapana, Daryan Kempe, Jennifer K. Thompson, Michael J. Mlodzianoski, Julie Healer, Maté Biro, Alan F. Cowman, and Kelly L. Rogers

Subjects

Science

Abstract

Here, Geoghegan, Evelyn et al. provide a lattice light-sheet microscopy based 4D imaging pipeline to quantitatively investigate Plasmodium spp. invasion and show that the nascent parasitophorous vacuole is predominantly formed from host’s erythrocyte membrane and undergoes continuous remodeling throughout invasion.

Published

2021

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

Author

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

Subjects

CRISPR, Plasmodium falciparum, antimalarial, fosmidomycin, glycolysis, isoprenoid, Microbiology, QR1-502

Abstract

ABSTRACT 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. IMPORTANCE 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.

Published

2019

5. Transcription Factor T-bet in B Cells Modulates Germinal Center Polarization and Antibody Affinity Maturation in Response to Malaria

Author

Ann Ly, Yang Liao, Halina Pietrzak, Lisa J. Ioannidis, Tom Sidwell, Renee Gloury, Marcel Doerflinger, Tony Triglia, Raymond Z. Qin, Joanna R. Groom, Gabrielle T. Belz, Kim L. Good-Jacobson, Wei Shi, Axel Kallies, and Diana S. Hansen

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Despite the key role that antibodies play in protection, the cellular processes mediating the acquisition of humoral immunity against malaria are not fully understood. Using an infection model of severe malaria, we find that germinal center (GC) B cells upregulate the transcription factor T-bet during infection. Molecular and cellular analyses reveal that T-bet in B cells is required not only for IgG2c switching but also favors commitment of B cells to the dark zone of the GC. T-bet was found to regulate the expression of Rgs13 and CXCR3, both of which contribute to the impaired GC polarization observed in the absence of T-bet, resulting in reduced IghV gene mutations and lower antibody avidity. These results demonstrate that T-bet modulates GC dynamics, thereby promoting the differentiation of B cells with increased affinity for antigen. : Antibody responses play a pivotal role in clinical immunity to malaria. Ly et al. report that that germinal center (GC) B cells upregulate the transcription factor T-bet during infection. T-bet favors commitment of B cells to the GC dark zone, thereby augmenting immunoglobulin gene mutation rates and antibody affinity maturation. Keywords: malaria, T-bet, B cells, germinal center, antibodies, affinity maturation

Published

2019

6. Protein Kinase A Is Essential for Invasion of Plasmodium falciparum into Human Erythrocytes

Author

Mary-Louise Wilde, Tony Triglia, Danushka Marapana, Jennifer K. Thompson, Alexei A. Kouzmitchev, Hayley E. Bullen, Paul R. Gilson, Alan F. Cowman, and Christopher J. Tonkin

Subjects

AMP-activated kinases, Plasmodium falciparum, host cell invasion, malaria, Microbiology, QR1-502

Abstract

ABSTRACT Understanding the mechanisms behind host cell invasion by Plasmodium falciparum remains a major hurdle to developing antimalarial therapeutics that target the asexual cycle and the symptomatic stage of malaria. Host cell entry is enabled by a multitude of precisely timed and tightly regulated receptor-ligand interactions. Cyclic nucleotide signaling has been implicated in regulating parasite invasion, and an important downstream effector of the cAMP-signaling pathway is protein kinase A (PKA), a cAMP-dependent protein kinase. There is increasing evidence that P. falciparum PKA (PfPKA) is responsible for phosphorylation of the cytoplasmic domain of P. falciparum apical membrane antigen 1 (PfAMA1) at Ser610, a cAMP-dependent event that is crucial for successful parasite invasion. In the present study, CRISPR-Cas9 and conditional gene deletion (dimerizable cre) technologies were implemented to generate a P. falciparum parasite line in which expression of the catalytic subunit of PfPKA (PfPKAc) is under conditional control, demonstrating highly efficient dimerizable Cre recombinase (DiCre)-mediated gene excision and complete knockdown of protein expression. Parasites lacking PfPKAc show severely reduced growth after one intraerythrocytic growth cycle and are deficient in host cell invasion, as highlighted by live-imaging experiments. Furthermore, PfPKAc-deficient parasites are unable to phosphorylate PfAMA1 at Ser610. This work not only identifies an essential role for PfPKAc in the P. falciparum asexual life cycle but also confirms that PfPKAc is the kinase responsible for phosphorylating PfAMA1 Ser610. IMPORTANCE Malaria continues to present a major global health burden, particularly in low-resource countries. Plasmodium falciparum, the parasite responsible for the most severe form of malaria, causes disease through rapid and repeated rounds of invasion and replication within red blood cells. Invasion into red blood cells is essential for P. falciparum survival, and the molecular events mediating this process have gained much attention as potential therapeutic targets. With no effective vaccine available, and with the emergence of resistance to antimalarials, there is an urgent need for the development of new therapeutics. Our research has used genetic techniques to provide evidence of an essential protein kinase involved in P. falciparum invasion. Our work adds to the current understanding of parasite signaling processes required for invasion, highlighting PKA as a potential drug target to inhibit invasion for the treatment of malaria.

Published

2019

7. PCRCR complex is essential for invasion of human erythrocytes by Plasmodium falciparum

Author

Stephen W. Scally, Tony Triglia, Cindy Evelyn, Benjamin A. Seager, Michał Pasternak, Pailene S. Lim, Julie Healer, Niall D. Geoghegan, Amy Adair, Wai-Hong Tham, Laura F. Dagley, Kelly L. Rogers, and Alan F. Cowman

Subjects

Microbiology (medical), Immunology, Genetics, Cell Biology, Applied Microbiology and Biotechnology, Microbiology

Abstract

The most severe form of malaria is caused by Plasmodium falciparum. These parasites invade human erythrocytes, and an essential step in this process involves the ligand PfRh5, which forms a complex with cysteine-rich protective antigen (CyRPA) and PfRh5-interacting protein (PfRipr) (RCR complex) and binds basigin on the host cell. We identified a heteromeric disulfide-linked complex consisting of P. falciparum Plasmodium thrombospondin-related apical merozoite protein (PfPTRAMP) and P. falciparum cysteine-rich small secreted protein (PfCSS) and have shown that it binds RCR to form a pentameric complex, PCRCR. Using P. falciparum lines with conditional knockouts, invasion inhibitory nanobodies to both PfPTRAMP and PfCSS, and lattice light-sheet microscopy, we show that they are essential for merozoite invasion. The PCRCR complex functions to anchor the contact between merozoite and erythrocyte membranes brought together by strong parasite deformations. We solved the structure of nanobody–PfCSS complexes to identify an inhibitory epitope. Our results define the function of the PCRCR complex and identify invasion neutralizing epitopes providing a roadmap for structure-guided development of these proteins for a blood stage malaria vaccine.

Published

2022

8. The Plasmodium falciparum parasitophorous vacuole protein <scp>P113</scp> interacts with the parasite protein export machinery and maintains normal vacuole architecture

Author

Hayley E. Bullen, Paul R. Sanders, Madeline G. Dans, Thorey K. Jonsdottir, David T. Riglar, Oliver Looker, Catherine S. Palmer, Betty Kouskousis, Sarah C. Charnaud, Tony Triglia, Mikha Gabriela, Molly Parkyn Schneider, Jo‐Anne Chan, Tania F. de Koning‐Ward, Jake Baum, James W. Kazura, James G. Beeson, Alan F. Cowman, Paul R. Gilson, and Brendan S. Crabb

Subjects

Protein Transport, Erythrocytes, Plasmodium falciparum, Vacuoles, Protozoan Proteins, Animals, Humans, Parasites, Malaria, Falciparum, Molecular Biology, Microbiology

Abstract

Infection with Plasmodium falciparum parasites results in approximately 627,000 deaths from malaria annually. Key to the parasite's success is their ability to invade and subsequently grow within human erythrocytes. Parasite proteins involved in parasite invasion and proliferation are therefore intrinsically of great interest, as targeting these proteins could provide novel means of therapeutic intervention. One such protein is P113 which has been reported to be both an invasion protein and an intracellular protein located within the parasitophorous vacuole (PV). The PV is delimited by a membrane (PVM) across which a plethora of parasite-specific proteins are exported via the Plasmodium Translocon of Exported proteins (PTEX) into the erythrocyte to enact various immune evasion functions. To better understand the role of P113 we isolated its binding partners from in vitro cultures of P. falciparum. We detected interactions with the protein export machinery (PTEX and exported protein-interacting complex) and a variety of proteins that either transit through the PV or reside on the parasite plasma membrane. Genetic knockdown or partial deletion of P113 did not significantly reduce parasite growth or protein export but did disrupt the morphology of the PVM, suggesting that P113 may play a role in maintaining normal PVM architecture.

Published

2022

9. Plasmepsin X activates function of the PCRCR complex in P. falciparum by processing PfRh5 for binding to basigin and invasion of human erythrocytes

Author

Tony Triglia, Stephen Scally, Benjamin Seager, Michal Pasternak, Laura Dagley, and Alan Cowman

Abstract

Plasmodium falciparum causes the most severe form of malaria in humans. The protozoan parasite develops within erythrocytes to mature schizonts, that contain more than 16 merozoites, which egress and invade fresh erythrocytes. The aspartic protease plasmepsin X (PMX), processes proteins and proteases essential for merozoite egress from the schizont and invasion of the host erythrocyte, including the leading vaccine candidate PfRh5. PfRh5 is anchored to the merozoite surface through a 5-membered complex (PCRCR), consisting of Plasmodium thrombospondin-related apical merozoite protein (PTRAMP), cysteine-rich small secreted protein (CSS), Rh5-interacting protein (PfRipr) and cysteine-rich protective antigen (CyRPA). We show that PCRCR is processed by PMX in micronemes to remove the N-terminal prodomain of PhRh5 and this activates the function of the complex unmasking a form that can bind basigin on the erythrocyte membrane and mediate merozoite invasion. The ability to activate PCRCR at a specific time in merozoite invasion most likely masks potential deleterious effects of its function until they are required. These results provide an important understanding of the essential role of PMX and the fine regulation of PCRCR function in P. falciparum biology.

Published

2023

10. Substrate Peptidomimetic Inhibitors of P. falciparum Plasmepsin X with Potent Antimalarial Activity

Author

Lachlan W. Richardson, Trent D. Ashton, Madeline G. Dans, Nghi Nguyen, Paola Favuzza, Tony Triglia, Anthony N. Hodder, Anna Ngo, Kate E. Jarman, Alan F. Cowman, and Brad E. Sleebs

Subjects

Pharmacology, Organic Chemistry, Plasmodium falciparum, Protozoan Proteins, Biochemistry, Carbon, Antimalarials, Drug Discovery, Molecular Medicine, Aspartic Acid Endopeptidases, Folic Acid Antagonists, Humans, Protease Inhibitors, Peptidomimetics, General Pharmacology, Toxicology and Pharmaceutics, Amino Acids, Malaria, Falciparum

Abstract

Plasmepsin X (PMX) is an aspartyl protease that processes proteins essential for Plasmodium parasites to invade and egress from host erythrocytes during the symptomatic asexual stage of malaria. PMX substrates possess a conserved cleavage region denoted by the consensus motif, SFhE (h=hydrophobic amino acid). Peptidomimetics reflecting the P

Published

2022

11. Basis for drug selectivity of plasmepsin IX and X inhibition in Plasmodium falciparum and vivax

Author

Anthony N. Hodder, Janni Christensen, Stephen Scally, Tony Triglia, Anna Ngo, Richard W. Birkinshaw, Brodie Bailey, Paola Favuzza, Melanie H. Dietrich, Wai-Hong Tham, Peter E. Czabotar, Kym Lowes, Zhuyan Guo, Nicholas Murgolo, Manuel de Lera Ruiz, John A. McCauley, Brad E. Sleebs, David Olsen, and Alan F. Cowman

Subjects

Kinetics, Structural Biology, Plasmodium falciparum, Protozoan Proteins, Aspartic Acid Endopeptidases, Molecular Biology, Substrate Specificity

Abstract

Plasmepsins IX (PMIX) and X (PMX) are essential aspartyl proteases for Plasmodium spp. egress, invasion, and development. WM4 and WM382 inhibit PMIX and PMX in Plasmodium falciparum and P. vivax. WM4 inhibits PMX, while WM382 is a dual inhibitor of PMIX and PMX. To understand their function, we identified protein substrates. Enzyme kinetic and structural analyses identified interactions responsible for drug specificity. PMIX and PMX have similar substrate specificity; however, there are distinct differences for peptide and protein substrates. Differences in WM4 and WM382 binding for PMIX and PMX map to variations in the S' region and engagement of the active site S3 pocket. Structures of PMX reveal interactions and mechanistic detail of drug binding important for development of clinical candidates against these targets.

Published

2021

12. Basis for drug selectivity of plasmepsin IX and X inhibition for Plasmodium falciparum and vivax

Author

Alan Cowman, Anthony Hodder, Janni Christensen, Stephen Scally, Tony Triglia, Anna Ngo, Richard Birkinshaw, Brodie Bailey, Paola Favuzza, Melanie Dietrich, Wai-Hong Tham, Peter Czabotar, Kym Lowes, Zhuyan Guo, Nicholas Murgolo, Manuel Ruiz, John McCauley, Brad Sleebs, and David Olsen

Subjects

parasitic diseases

Abstract

Plasmepsin IX (PMIX) and X (PMX) are aspartyl proteases of Plasmodium spp. that play essential roles in parasite egress, invasion and development. Consequently, they are important drug targets for Plasmodium falciparum and P. vivax. WM4 and WM382 are potent inhibitors of PMIX and PMX that block invasion of liver and blood stages and transmission to mosquitoes. WM4 specifically inhibits PMX whilst WM382 is a dual inhibitor of PMIX and PMX. To understand the function of PMIX and PMX proteases we identified new protein substrates in P. falciparum and together with detailed kinetic analyses and structural analyses identified key molecular interactions in the active site responsible for the specificity of WM4 and WM382 inhibition. The crystal structures of PMX apo enzyme and the protease/drug complexes of PMX/WM382 and PMX/WM4 for P. falciparum and P. vivax have been solved. We show PMIX and PMX have similar substrate selectivity, however, there are distinct differences for both peptide and full-length protein substrates through differences in localised 3-dimensional structures for the enzyme substrate-binding cleft and substrate interface. The differences in affinities of WM4 and WM382 binding for PMIX and PMX map to variations in surface interactions with each protease in the S' region of the active sites. Crystal structures of PMX reveal interactions and mechanistic detail on the selectivity of drug binding which will be important for further development of clinical candidates against these important molecular targets.

Published

2021

13. Basis for drug selectivity of plasmepsin IX and X inhibition for Plasmodium falciparum and vivax

Author

Janni Christensen, Wai-Hong Tham, David B. Olsen, Alan F. Cowman, Anthony N. Hodder, Brodie L Bailey, Peter E. Czabotar, Brad E. Sleebs, Zhuyan Guo, Tony Triglia, Stephen Scally, Nicholas Murgolo, John A. Mccauley, Anna Ngo, Richard W Birkinshaw, Paola Favuzza, Kym N Lowes, Melanie H. Dietrich, and Manuel de Lera Ruiz

Subjects

Drug, biology, Biochemistry, Chemistry, media_common.quotation_subject, Plasmepsin, Plasmodium falciparum, Selectivity, biology.organism_classification, media_common

Abstract

Plasmepsin IX (PMIX) and X (PMX) are aspartyl proteases of Plasmodium spp. that play essential roles in parasite egress, invasion and development. Consequently, they are important drug targets for Plasmodium falciparum and P. vivax. WM4 and WM382 are potent inhibitors of PMIX and PMX that block invasion of liver and blood stages and transmission to mosquitoes. WM4 specifically inhibits PMX whilst WM382 is a dual inhibitor of PMIX and PMX. To understand the function of PMIX and PMX proteases we identified new protein substrates in P. falciparum and together with detailed kinetic analyses and structural analyses identified key molecular interactions in the active site responsible for the specificity of WM4 and WM382 inhibition. The crystal structures of PMX apo enzyme and the protease/drug complexes of PMX/WM382 and PMX/WM4 for P. falciparum and P. vivax have been solved. We show PMIX and PMX have similar substrate selectivity, however, there are distinct differences for both peptide and full-length protein substrates through differences in localised 3-dimensional structures for the enzyme substrate-binding cleft and substrate interface. The differences in affinities of WM4 and WM382 binding for PMIX and PMX map to variations in surface interactions with each protease in the S' region of the active sites. Crystal structures of PMX reveal interactions and mechanistic detail on the selectivity of drug binding which will be important for further development of clinical candidates against these important molecular targets.

Published

2021

14. 4D analysis of malaria parasite invasion offers insights into erythrocyte membrane remodeling and parasitophorous vacuole formation

Author

Phoebe McDonald, Michael J. Mlodzianoski, Niall D. Geoghegan, Julie Healer, Alan F. Cowman, Cindy Evelyn, Kelly L. Rogers, Danushka S. Marapana, Michal Pasternak, Daryan Kempe, Tony Triglia, Maté Biro, Lachlan Whitehead, and Jennifer K. Thompson

Subjects

0301 basic medicine, Plasmodium, Erythrocytes, Science, Plasmodium falciparum, Protozoan Proteins, General Physics and Astronomy, General Biochemistry, Genetics and Molecular Biology, Article, Host-Parasite Interactions, 03 medical and health sciences, Membrane biophysics, 0302 clinical medicine, Organelle, parasitic diseases, Humans, Animals, Secretion, Parasites, Four-Dimensional Computed Tomography, Host cell membrane, Microscopy, Multidisciplinary, biology, Plasmodium (life cycle), Chemistry, Merozoites, Intracellular parasite, Time-lapse imaging, Erythrocyte Membrane, General Chemistry, biology.organism_classification, Cell biology, Malaria, Parasite biology, 030104 developmental biology, Vacuoles, 030217 neurology & neurosurgery, Biogenesis

Abstract

Host membrane remodeling is indispensable for viruses, bacteria, and parasites, to subvert the membrane barrier and obtain entry into cells. The malaria parasite Plasmodium spp. induces biophysical and molecular changes to the erythrocyte membrane through the ordered secretion of its apical organelles. To understand this process and address the debate regarding how the parasitophorous vacuole membrane (PVM) is formed, we developed an approach using lattice light-sheet microscopy, which enables the parasite interaction with the host cell membrane to be tracked and characterized during invasion. Our results show that the PVM is predominantly formed from the erythrocyte membrane, which undergoes biophysical changes as it is remodeled across all stages of invasion, from pre-invasion through to PVM sealing. This approach enables a functional interrogation of parasite-derived lipids and proteins in PVM biogenesis and echinocytosis during Plasmodium falciparum invasion and promises to yield mechanistic insights regarding how this is more generally orchestrated by other intracellular pathogens., Here, Geoghegan, Evelyn et al. provide a lattice light-sheet microscopy based 4D imaging pipeline to quantitatively investigate Plasmodium spp. invasion and show that the nascent parasitophorous vacuole is predominantly formed from host’s erythrocyte membrane and undergoes continuous remodeling throughout invasion.

Published

2021

15. Transcription Factor T-bet in B Cells Modulates Germinal Center Polarization and Antibody Affinity Maturation in Response to Malaria

Author

Raymond Z. Qin, Joanna R Groom, Halina M. Pietrzak, Kim L. Good-Jacobson, Lisa J Ioannidis, Tom Sidwell, Ann Ly, Diana S. Hansen, Marcel Doerflinger, Axel Kallies, Wei Shi, Gabrielle T. Belz, Renee Gloury, Tony Triglia, and Yang Liao

Subjects

0301 basic medicine, Receptors, CXCR3, Antibody Affinity, chemical and pharmacologic phenomena, Gene mutation, General Biochemistry, Genetics and Molecular Biology, Affinity maturation, Mice, 03 medical and health sciences, 0302 clinical medicine, Antigen, Animals, Avidity, Transcription factor, lcsh:QH301-705.5, B-Lymphocytes, biology, Chemistry, Germinal center, hemic and immune systems, Germinal Center, Malaria, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, lcsh:Biology (General), Mutation, Humoral immunity, biology.protein, Antibody, T-Box Domain Proteins, RGS Proteins, 030217 neurology & neurosurgery

Abstract

Summary: Despite the key role that antibodies play in protection, the cellular processes mediating the acquisition of humoral immunity against malaria are not fully understood. Using an infection model of severe malaria, we find that germinal center (GC) B cells upregulate the transcription factor T-bet during infection. Molecular and cellular analyses reveal that T-bet in B cells is required not only for IgG2c switching but also favors commitment of B cells to the dark zone of the GC. T-bet was found to regulate the expression of Rgs13 and CXCR3, both of which contribute to the impaired GC polarization observed in the absence of T-bet, resulting in reduced IghV gene mutations and lower antibody avidity. These results demonstrate that T-bet modulates GC dynamics, thereby promoting the differentiation of B cells with increased affinity for antigen. : Antibody responses play a pivotal role in clinical immunity to malaria. Ly et al. report that that germinal center (GC) B cells upregulate the transcription factor T-bet during infection. T-bet favors commitment of B cells to the GC dark zone, thereby augmenting immunoglobulin gene mutation rates and antibody affinity maturation. Keywords: malaria, T-bet, B cells, germinal center, antibodies, affinity maturation

Published

2019

16. Basis for Drug Selectivity of Plasmepsin IX and X Inhibition for Plasmodium falciparum and vivax

Author

Anthony Hodder, Janni Christensen, Stephen Scally, Tony Triglia, Anna Ngo, Richard Birkinshaw, Brodie L Bailey, Paola Favuzza, Melanie Dietrich, Wai-Hong Tham, Peter Czabotar, Kym Lowes, Zhuyan Guo, Nicholas Murgolo, Manuel de Lera Ruiz, John McCauley, Brad Sleebs, David Olsen, and Alan Cowman

Published

2021

17. 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

18. Plasmepsin V cleaves malaria effector proteins in a distinct endoplasmic reticulum translocation interactome for export to the erythrocyte

Author

Paul R. Gilson, Danushka S. Marapana, Andrew I. Webb, Benjamin K. Dickerman, Jarrod J. Sandow, Thomas Nebl, Tony Triglia, Alan F. Cowman, Justin A Boddey, Michał Pasternak, Laura F. Dagley, and Brendan S. Crabb

Subjects

0301 basic medicine, Microbiology (medical), Erythrocytes, Virulence Factors, Plasmodium falciparum, Immunology, Plasmepsin, Endoplasmic Reticulum, Applied Microbiology and Biotechnology, Microbiology, 03 medical and health sciences, Genetics, Aspartic Acid Endopeptidases, Malaria, Falciparum, Secretory pathway, Signal peptidase, Chemistry, Effector, Endoplasmic reticulum, Cell Membrane, Peptidase complex, Biological Transport, Cell Biology, Translocon, Cell biology, 030104 developmental biology, Vacuolar transport, SEC Translocation Channels

Abstract

Plasmodium falciparum exports hundreds of virulence proteins within infected erythrocytes, a process that requires cleavage of a pentameric motif called Plasmodium export element or vacuolar transport signal by the endoplasmic reticulum (ER)-resident protease plasmepsin V. We identified plasmepsin V-binding proteins that form a unique interactome required for the translocation of effector cargo into the parasite ER. These interactions are functionally distinct from the Sec61-signal peptidase complex required for the translocation of proteins destined for the classical secretory pathway. This interactome does not involve the signal peptidase (SPC21) and consists of PfSec61, PfSPC25, plasmepsin V and PfSec62, which is an essential component of the post-translational ER translocon. Together, they form a distinct portal for the recognition and translocation of a large subset of Plasmodium export element effector proteins into the ER, thereby remodelling the infected erythrocyte that is required for parasite survival and pathogenesis.

Published

2018

19. 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

20. Protein Kinase A Is Essential for Invasion of Plasmodium falciparum into Human Erythrocytes

Author

Paul R. Gilson, Mary-Louise Wilde, Jennifer K. Thompson, Alan F. Cowman, Christopher J. Tonkin, Hayley E Bullen, Danushka S. Marapana, Alexei A Kouzmitchev, and Tony Triglia

Subjects

Erythrocytes, plasmodium falciparum, Protozoan Proteins, malaria, Cre recombinase, Antigens, Protozoan, Microbiology, Host-Microbe Biology, 03 medical and health sciences, Catalytic Domain, Virology, parasitic diseases, Humans, Phosphorylation, Apical membrane antigen 1, Protein kinase A, Gene, host cell invasion, 030304 developmental biology, amp-activated kinases, 0303 health sciences, Gene knockdown, biology, 030306 microbiology, Kinase, Effector, Membrane Proteins, Plasmodium falciparum, biology.organism_classification, Cyclic AMP-Dependent Protein Kinases, Endocytosis, QR1-502, Cell biology, Protein Processing, Post-Translational, Research Article

Abstract

Malaria continues to present a major global health burden, particularly in low-resource countries. Plasmodium falciparum, the parasite responsible for the most severe form of malaria, causes disease through rapid and repeated rounds of invasion and replication within red blood cells. Invasion into red blood cells is essential for P. falciparum survival, and the molecular events mediating this process have gained much attention as potential therapeutic targets. With no effective vaccine available, and with the emergence of resistance to antimalarials, there is an urgent need for the development of new therapeutics. Our research has used genetic techniques to provide evidence of an essential protein kinase involved in P. falciparum invasion. Our work adds to the current understanding of parasite signaling processes required for invasion, highlighting PKA as a potential drug target to inhibit invasion for the treatment of malaria., Understanding the mechanisms behind host cell invasion by Plasmodium falciparum remains a major hurdle to developing antimalarial therapeutics that target the asexual cycle and the symptomatic stage of malaria. Host cell entry is enabled by a multitude of precisely timed and tightly regulated receptor-ligand interactions. Cyclic nucleotide signaling has been implicated in regulating parasite invasion, and an important downstream effector of the cAMP-signaling pathway is protein kinase A (PKA), a cAMP-dependent protein kinase. There is increasing evidence that P. falciparum PKA (PfPKA) is responsible for phosphorylation of the cytoplasmic domain of P. falciparum apical membrane antigen 1 (PfAMA1) at Ser610, a cAMP-dependent event that is crucial for successful parasite invasion. In the present study, CRISPR-Cas9 and conditional gene deletion (dimerizable cre) technologies were implemented to generate a P. falciparum parasite line in which expression of the catalytic subunit of PfPKA (PfPKAc) is under conditional control, demonstrating highly efficient dimerizable Cre recombinase (DiCre)-mediated gene excision and complete knockdown of protein expression. Parasites lacking PfPKAc show severely reduced growth after one intraerythrocytic growth cycle and are deficient in host cell invasion, as highlighted by live-imaging experiments. Furthermore, PfPKAc-deficient parasites are unable to phosphorylate PfAMA1 at Ser610. This work not only identifies an essential role for PfPKAc in the P. falciparum asexual life cycle but also confirms that PfPKAc is the kinase responsible for phosphorylating PfAMA1 Ser610.

Published

2019

21. Essential Role of the PfRh5/PfRipr/CyRPA Complex during Plasmodium falciparum Invasion of Erythrocytes

Author

Jennifer Volz, Danushka S. Marapana, Alan Yap, Alan F. Cowman, Wai-Hong Tham, Jenn K. Thompson, Kelly L. Rogers, Marko Lampe, Lachlan Whitehead, Wilson Wong, Tony Triglia, Thomas Nebl, Lin Chen, Nicholas T.Y. Lim, Danny W. Wilson, and Xavier Sisquella

Subjects

0301 basic medicine, Erythrocytes, Cations, Divalent, Plasmodium falciparum, Protozoan Proteins, Antigens, Protozoan, Plasma protein binding, Biology, Endocytosis, Models, Biological, Microbiology, 03 medical and health sciences, 0302 clinical medicine, Antigen, Virology, parasitic diseases, Humans, Receptor, Microscopy, Tight junction, biology.organism_classification, Cell biology, 030104 developmental biology, Gene Knockdown Techniques, Basigin, Host-Pathogen Interactions, biology.protein, Calcium, Parasitology, Protein Multimerization, Antibody, Carrier Proteins, 030217 neurology & neurosurgery, Protein Binding

Abstract

Plasmodium falciparum parasites in the merozoite stage invade human erythrocytes and cause malaria. Invasion requires multiple interactions between merozoite ligands and erythrocyte receptors. P. falciparum reticulocyte binding homolog 5 (PfRh5) forms a complex with the PfRh5-interacting protein (PfRipr) and Cysteine-rich protective antigen (CyRPA) and binds erythrocytes via the host receptor basigin. However, the specific role that PfRipr and CyRPA play during invasion is unclear. Using P. falciparum lines conditionally expressing PfRipr and CyRPA, we show that loss of PfRipr or CyRPA function blocks growth due to the inability of merozoites to invade erythrocytes. Super-resolution microscopy revealed that PfRipr, CyRPA, and PfRh5 colocalize at the junction between merozoites and erythrocytes during invasion. PfRipr, CyRPA, and PfRipr/CyRPA/PfRh5-basigin complex is required for triggering the Ca(2+) release and establishing the tight junction. Together, these results establish that the PfRh5/PfRipr/CyRPA complex is essential in the sequential molecular events leading to parasite invasion of human erythrocytes.

Published

2016

22. 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

23. Mefloquine targets the Plasmodium falciparum 80S ribosome to inhibit protein synthesis

Author

Brad E. Sleebs, Xiao Chen Bai, Alan F. Cowman, Jake Baum, Israel S. Fernández, Danushka S. Marapana, Alan Brown, Jennifer K. Thompson, Eric Hanssen, Tony Triglia, Wilson Wong, Sjors H.W. Scheres, Katherine E. Jackson, Stuart A. Ralph, and Wellcome Trust

Subjects

0301 basic medicine, Microbiology (medical), FEATURES, INVASION, Plasmodium falciparum, 030106 microbiology, Immunology, SUSCEPTIBILITY, Pharmacology, Applied Microbiology and Biotechnology, Microbiology, Ribosome, Article, Antimalarials, 03 medical and health sciences, 1108 Medical Microbiology, Genetics, medicine, Animals, Parasites, COMBINATION, Mode of action, Protein Synthesis Inhibitors, Science & Technology, Protein synthesis inhibitor, IDENTIFICATION, REFINEMENT, biology, Chemistry, Mefloquine, Mutagenesis, Cell Biology, biology.organism_classification, GENE, 030104 developmental biology, RESOLUTION, Mechanism of action, Protein Biosynthesis, medicine.symptom, Eukaryotic Ribosome, Life Sciences & Biomedicine, Ribosomes, RESISTANCE, 0605 Microbiology, medicine.drug

Abstract

Malaria control is heavily dependent on chemotherapeutic agents for disease prevention and drug treatment. Defining the mechanism of action for licensed drugs, for which no target is characterized, is critical to the development of their second-generation derivatives to improve drug potency towards inhibition of their molecular targets. Mefloquine is a widely used antimalarial without a known mode of action. Here, we demonstrate that mefloquine is a protein synthesis inhibitor. We solved a 3.2 Å cryo-electron microscopy structure of the Plasmodium falciparum 80S ribosome with the (+)-mefloquine enantiomer bound to the ribosome GTPase-associated centre. Mutagenesis of mefloquine-binding residues generates parasites with increased resistance, confirming the parasite-killing mechanism. Furthermore, structure-guided derivatives with an altered piperidine group, predicted to improve binding, show enhanced parasiticidal effect. These data reveal one possible mode of action for mefloquine and demonstrate the vast potential of cryo-electron microscopy to guide the development of mefloquine derivatives to inhibit parasite protein synthesis.

Published

2017