Your search keyword '"Hans B. Liu"' showing total 8 results

1. Dephospho‐CoA kinase, a nuclear‐encoded apicoplast protein, remains active and essential after Plasmodium falciparum apicoplast disruption

Author

Sean T. Prigge, Russell P. Swift, Hans B. Liu, and Krithika Rajaram

Subjects

Coenzyme A, Plasmodium falciparum, Isopentenyl pyrophosphate, malaria, Protozoan Proteins, coenzyme A, Apicoplasts, General Biochemistry, Genetics and Molecular Biology, Article, Pantothenic Acid, DPCK, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Organelle, Molecular Biology, Heme, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Apicoplast, apicoplast, General Immunology and Microbiology, biology, General Neuroscience, Articles, biology.organism_classification, Microbiology, Virology & Host Pathogen Interaction, Cell biology, Metabolic pathway, Phosphotransferases (Alcohol Group Acceptor), Enzyme, Metabolism, chemistry, 030217 neurology & neurosurgery

Abstract

Malaria parasites contain an essential organelle called the apicoplast that houses metabolic pathways for fatty acid, heme, isoprenoid, and iron–sulfur cluster synthesis. Surprisingly, malaria parasites can survive without the apicoplast as long as the isoprenoid precursor isopentenyl pyrophosphate (IPP) is supplemented in the growth medium, making it appear that isoprenoid synthesis is the only essential function of the organelle in blood‐stage parasites. In the work described here, we localized an enzyme responsible for coenzyme A synthesis, DPCK, to the apicoplast, but we were unable to delete DPCK, even in the presence of IPP. However, once the endogenous DPCK was complemented with the E. coli DPCK (EcDPCK), we were successful in deleting it. We were then able to show that DPCK activity is required for parasite survival through knockdown of the complemented EcDPCK. Additionally, we showed that DPCK enzyme activity remains functional and essential within the vesicles present after apicoplast disruption. These results demonstrate that while the apicoplast of blood‐stage P. falciparum parasites can be disrupted, the resulting vesicles remain biochemically active and are capable of fulfilling essential functions., Production of coenzyme A is an indispensable function of the apicoplast organelle in blood‐stage malaria parasites.

Published

2021

2. Redesigned TetR-Aptamer System To Control Gene Expression in Plasmodium falciparum

Author

Hans B. Liu, Sean T. Prigge, and Krithika Rajaram

Subjects

Untranslated region, Molecular Biology and Physiology, Aptamer, Plasmodium falciparum, lcsh:QR1-502, malaria, Computational biology, Biology, Proof of Concept Study, Microbiology, lcsh:Microbiology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Gene expression, TetR, RNA, Messenger, RNA aptamers, Molecular Biology, Gene, Gene knockout, Oligonucleotide Array Sequence Analysis, tetracycline, 030304 developmental biology, 0303 health sciences, Gene knockdown, Apicoplast, Genes, Essential, tetracycline repressor, Aptamers, Nucleotide, QR1-502, Gene Expression Regulation, chemistry, TetR-DOZI, Trans-Activators, protein knockdown, 030217 neurology & neurosurgery, Research Article

Abstract

Malaria elimination efforts have been repeatedly hindered by the evolution and spread of multidrug-resistant strains of Plasmodium falciparum. The absence of a commercially available vaccine emphasizes the need for a better understanding of Plasmodium biology in order to further translational research. This has been partly facilitated by targeted gene deletion strategies for the functional analysis of parasite genes. However, genes that are essential for parasite replication in erythrocytes are refractory to such methods, and require conditional knockdown or knockout approaches to dissect their function. One such approach is the TetR-DOZI system that employs multiple synthetic aptamers in the untranslated regions of target genes to control their expression in a tetracycline-dependent manner. Maintaining modified parasites with intact aptamer copies has been challenging since these repeats can be lost by recombination. By interspacing the aptamers with unique sequences, we created a stable genetic system that remains effective at controlling target gene expression., One of the most powerful approaches to understanding gene function involves turning genes on and off at will and measuring the impact at the cellular or organismal level. This particularly applies to the cohort of essential genes where traditional gene knockouts are inviable. In Plasmodium falciparum, conditional control of gene expression has been achieved by using multicomponent systems in which individual modules interact with each other to regulate DNA recombination, transcription, or posttranscriptional processes. The recently devised TetR-DOZI aptamer system relies on the ligand-regulatable interaction of a protein module with synthetic RNA aptamers to control the translation of a target gene. This technique has been successfully employed to study essential genes in P. falciparum and involves the insertion of several aptamer copies into the 3′ untranslated regions (UTRs), which provide control over mRNA fate. However, aptamer repeats are prone to recombination and one or more copies can be lost from the system, resulting in a loss of control over target gene expression. We rectified this issue by redesigning the aptamer array to minimize recombination while preserving the control elements. As proof of concept, we compared the original and modified arrays for their ability to knock down the levels of a putative essential apicoplast protein (PF3D7_0815700) and demonstrated that the modified array is highly stable and efficient. This redesign will enhance the utility of a tool that is quickly becoming a favored strategy for genetic studies in P. falciparum. IMPORTANCE Malaria elimination efforts have been repeatedly hindered by the evolution and spread of multidrug-resistant strains of Plasmodium falciparum. The absence of a commercially available vaccine emphasizes the need for a better understanding of Plasmodium biology in order to further translational research. This has been partly facilitated by targeted gene deletion strategies for the functional analysis of parasite genes. However, genes that are essential for parasite replication in erythrocytes are refractory to such methods, and require conditional knockdown or knockout approaches to dissect their function. One such approach is the TetR-DOZI system that employs multiple synthetic aptamers in the untranslated regions of target genes to control their expression in a tetracycline-dependent manner. Maintaining modified parasites with intact aptamer copies has been challenging since these repeats can be lost by recombination. By interspacing the aptamers with unique sequences, we created a stable genetic system that remains effective at controlling target gene expression.

Published

2020

3. The NTP generating activity of pyruvate kinase II is critical for apicoplast maintenance in Plasmodium falciparum

Author

Cyrianne Keutcha, Amanda Dziedzic, Sean T. Prigge, Hans B. Liu, Bobby Kwan, Krithika Rajaram, Russell P. Swift, and Anne E. Jedlicka

Subjects

carbon metabolism, QH301-705.5, Science, Pyruvate Kinase, malaria, Chemical biology, Biology, General Biochemistry, Genetics and Molecular Biology, Organelle, Nucleotide, Biology (General), Gene, chemistry.chemical_classification, Apicoplast, apicoplast, General Immunology and Microbiology, General Neuroscience, Plasmodium falciparum, General Medicine, biology.organism_classification, Cell biology, Enzyme, plasmodium, chemistry, Medicine, microarray, Pyruvate kinase

Abstract

The apicoplast of Plasmodium falciparum parasites is believed to rely on the import of three-carbon phosphate compounds for use in organelle anabolic pathways, in addition to the generation of energy and reducing power within the organelle. We generated a series of genetic deletions in an apicoplast metabolic bypass line to determine which genes involved in apicoplast carbon metabolism are required for blood-stage parasite survival and organelle maintenance. We found that pyruvate kinase II (PyrKII) is essential for organelle maintenance, but that production of pyruvate by PyrKII is not responsible for this phenomenon. Enzymatic characterization of PyrKII revealed activity against all NDPs and dNDPs tested, suggesting that it may be capable of generating a broad range of nucleotide triphosphates. Conditional mislocalization of PyrKII resulted in decreased transcript levels within the apicoplast that preceded organelle disruption, suggesting that PyrKII is required for organelle maintenance due to its role in nucleotide triphosphate generation.

Published

2020

4. Author response: The NTP generating activity of pyruvate kinase II is critical for apicoplast maintenance in Plasmodium falciparum

Author

Russell P. Swift, Cyrianne Keutcha, Krithika Rajaram, Bobby Kwan, Anne E. Jedlicka, Sean T. Prigge, Hans B. Liu, and Amanda Dziedzic

Subjects

Apicoplast, Biochemistry, Plasmodium falciparum, Biology, biology.organism_classification, Pyruvate kinase

Published

2020

5. A redesigned TetR-aptamer system to control gene expression in Plasmodium falciparum

Author

Krithika Rajaram, Hans B. Liu, and Sean T. Prigge

Subjects

Untranslated region, Apicoplast, chemistry.chemical_compound, chemistry, Transcription (biology), Aptamer, Gene expression, TetR, Computational biology, Biology, Gene, Gene knockout

Abstract

One of the most powerful approaches to understanding gene function involves turning genes on and off at will and measuring the impact at the cellular or organismal level. This particularly applies to the cohort of essential genes where traditional gene knockouts are inviable. In Plasmodium falciparum, conditional control of gene expression has been achieved by using multi-component systems in which individual modules interact with each other to regulate DNA recombination, transcription or posttranscriptional processes. The recently devised TetR-DOZI aptamer system relies on the ligand-regulatable interaction of a protein module with synthetic RNA aptamers to control the translation of a target gene. This technique has been successfully employed to study essential genes in P. falciparum and involves the insertion of several aptamer copies into their 3’ untranslated regions (UTRs) which provide control over mRNA fate. However, aptamer repeats are prone to recombination and one or more copies can be lost from the system, resulting in a loss of control over target gene expression. We rectified this issue by redesigning the aptamer array to minimize recombination while preserving the control elements. As proof of concept, we compared the original and modified arrays for their ability to knock down the levels of a putative essential apicoplast protein (PF3D7_0815700) and demonstrated that the modified array is highly stable and efficient. This redesign will enhance the utility of a tool that is quickly becoming a favored strategy for genetic studies in P. falciparum.ImportanceMalaria elimination efforts have been repeatedly hindered by the evolution and spread of multidrug-resistant strains of Plasmodium falciparum. The absence of a commercially available vaccine emphasizes the need for a better understanding of Plasmodium biology in order to further translational research. This has been partly facilitated by targeted gene deletion strategies for the functional analysis of parasite genes. However, genes that are essential for parasite replication in erythrocytes are refractory to such methods, and require conditional knockdown or knockout approaches to dissect their function. One such approach is the TetR-DOZI system that employs multiple synthetic aptamers in the untranslated regions of target genes to control their expression in a tetracycline-dependent manner. Maintaining modified parasites with intact aptamer copies has been challenging since these repeats are frequently lost by recombination. By interspacing the aptamers with unique sequences, we created a stable genetic system that remains effective at controlling target gene expression.

Published

2020

6. A mevalonate bypass system facilitates elucidation of plastid biology in malaria parasites

Author

Krista Ann Matthews, Namandjé N. Bumpus, Hugo Jhun, Hans B. Liu, Krithika Rajaram, Sean T. Prigge, Aleah D. Roberts, Anne E. Jedlicka, Russell P. Swift, Amanda Dziedzic, Shivendra G. Tewari, and Anders Wallqvist

Subjects

Plasmodium, Protozoan Proteins, Isopentenyl pyrophosphate, Azithromycin, Biochemistry, Transcriptome, chemistry.chemical_compound, Drug Metabolism, Medicine and Health Sciences, Metabolites, Plastids, Biology (General), Protein Metabolism, Protozoans, 0303 health sciences, 030302 biochemistry & molecular biology, Malarial Parasites, Eukaryota, Isoprenoids, Lipids, Anti-Bacterial Agents, 3. Good health, Cell biology, Cellular Structures and Organelles, Research Article, medicine.drug, QH301-705.5, Plasmodium falciparum, Immunology, Mevalonic Acid, Apicoplasts, Biology, Microbiology, 03 medical and health sciences, Hemiterpenes, Organophosphorus Compounds, Metabolomics, Fosfomycin, Virology, Parasite Groups, Organelle, Parasitic Diseases, Genetics, medicine, Animals, Humans, Parasites, Pharmacokinetics, Plastid, Molecular Biology, 030304 developmental biology, Pharmacology, Apicoplast, Organisms, Biology and Life Sciences, Cell Biology, RC581-607, medicine.disease, Parasitic Protozoans, Fosmidomycin, Malaria, Metabolism, chemistry, Parasitology, Immunologic diseases. Allergy, Apicomplexa

Abstract

Malaria parasites rely on a plastid organelle for survival during the blood stages of infection. However, the entire organelle is dispensable as long as the isoprenoid precursor, isopentenyl pyrophosphate (IPP), is supplemented in the culture medium. We engineered parasites to produce isoprenoid precursors from a mevalonate-dependent pathway, creating a parasite line that replicates normally after the loss of the apicoplast organelle. We show that carbon-labeled mevalonate is specifically incorporated into isoprenoid products, opening new avenues for researching this essential class of metabolites in malaria parasites. We also show that essential apicoplast proteins, such as the enzyme target of the drug fosmidomycin, can be deleted in this mevalonate bypass parasite line, providing a new method to determine the roles of other important apicoplast-resident proteins. Several antibacterial drugs kill malaria parasites by targeting basic processes, such as transcription, in the organelle. We used metabolomic and transcriptomic methods to characterize parasite metabolism after azithromycin treatment triggered loss of the apicoplast and found that parasite metabolism and the production of apicoplast proteins is largely unaltered. These results provide insight into the effects of apicoplast-disrupting drugs, several of which have been used to treat malaria infections in humans. Overall, the mevalonate bypass system provides a way to probe essential aspects of apicoplast biology and study the effects of drugs that target apicoplast processes., Author summary Malaria parasites rely on an organelle called the apicoplast for growth and survival. Antimalarial drugs such as azithromycin inhibit basic processes in the apicoplast and result in the disruption of the organelle. Surprisingly, addition of a single metabolite, isopentenyl pyrophosphate (IPP), allows the parasites to survive in culture after disruption of the apicoplast. Unfortunately, using IPP to study this phenomenon has several limitations: IPP is prohibitively expensive, has to be used at high concentrations, and has a half-life less than 5 hours. To address these problems, we engineered parasites to express four enzymes from an alternative pathway capable of producing IPP in the parasites. We validated this new system and used it to metabolically label essential metabolites, to delete an essential apicoplast protein, and to characterize the state of apicoplast-disrupted parasites. A key finding from these studies comes from transcriptomic and metabolomic analysis of parasites treated with the drug azithromycin. We found that apicoplast disruption results in few changes in parasite metabolism. In particular, the expression of hundreds of nuclear-encoded apicoplast proteins are not affected by disruption of the apicoplast organelle, making it likely that apicoplast metabolic pathways and processes are still functional in apicoplast-disrupted parasites.

Published

2020

7. Keratin 6 regulates collective keratinocyte migration by altering cell-cell and cell-matrix adhesion

Author

Carole A. Parent, Pierre A. Coulombe, Hans B. Liu, Fengrong Wang, and Song Chen

Subjects

0301 basic medicine, Keratinocytes, Cell, Biology, Article, Focal adhesion, 03 medical and health sciences, Mice, Cell-matrix adhesion, Cell Movement, Keratin, medicine, Cell Adhesion, Animals, Keratinocyte migration, Intermediate filament, Research Articles, chemistry.chemical_classification, integumentary system, Desmoplakin, Keratin-6, Cell Biology, Adhesion, Mice, Mutant Strains, Cell biology, Extracellular Matrix, 030104 developmental biology, medicine.anatomical_structure, chemistry, Desmoplakins, biology.protein

Abstract

Keratin 6 (K6) isoforms are induced in wound-proximal keratinocytes after injury to skin. Paradoxically, absence of K6 isoforms leads to faster directional cell migration. Wang et al. report that K6 promotes collective keratinocyte migration by interacting with desmoplakin and myosin IIA and stabilizing cell adhesion., The a and b isoforms of keratin 6 (K6), a type II intermediate filament (IF) protein, are robustly induced upon injury to interfollicular epidermis. We previously showed that complete loss of K6a/K6b stimulates keratinocyte migration, correlating with enhanced Src activity. In this study, we demonstrate that this property is cell autonomous, depends on the ECM, and results from elevated speed, enhanced directionality, and an increased rate of focal adhesion disassembly. We show that myosin IIA interacts with K6a/K6b, that its levels are markedly reduced in Krt6a/Krt6b-null keratinocytes, and that inhibiting myosin ATPase activity normalizes the enhanced migration potential of Krt6a/Krt6b-null cells. Desmoplakin, which mediates attachment of IFs to desmosomes, is also expressed at reduced levels and is mislocalized to the nucleus in Krt6a/Krt6b-null cells, correlating with defects in cell adhesion. These findings reveal that K6a/K6b modulate keratinocyte migration by regulating cell–matrix and cell–cell adhesion and highlight a role for keratins in collective cell migration.

Published

2017

8. Telomere Shortening, Inflammatory Cytokines, and Anti-Cytomegalovirus Antibody Follow Distinct Age-Associated Trajectories in Humans

Author

Palchamy Elango, Hans B. Liu, Luigi Ferrucci, Ana Lustig, Melissa A. Swaby, Richard J. Hodes, E. Jeffrey Metter, Nan-ping Weng, and Yang An

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, Immunology, Biology, Proinflammatory cytokine, 03 medical and health sciences, Immune system, medicine, Immunology and Allergy, Interferon gamma, Interleukin 6, Original Research, IL-6, aging, Antibody titer, telomeres, Telomere, Interleukin 10, Titer, 030104 developmental biology, interferon gamma, anti-CMV IgG, IL-10, biology.protein, lcsh:RC581-607, medicine.drug

Abstract

A number of biological parameters have been cited as hallmarks of immune aging. However, it is not clear whether these multiple biological changes are the result of common underlying aging processes and follow correlated trajectories, or whether the patterns of change for multiple parameters vary across individuals and reflect heterogeneity in the aging process. Here, we have studied parameters of immune system aging through longitudinal analysis of telomere length, inflammatory cytokines, and antibody titer to cytomegalovirus (CMV) in 465 subjects ranging in age from 21 to 88 years at the first visit, with an average of 13 years (7–19 years) follow-up. We observed a highly variable rate of change in telomere length of PBMCs with a relatively slow average rate of telomere shortening (−16 bp/year). Similarly, there were significant increases with age in vivo in three inflammation-related cytokines (interferon gamma, IL-6, and IL-10) and in anti-CMV IgG titer, which varied widely across individuals as well. We further observed positive correlative changes among different inflammatory cytokines. However, we did not find significant correlations among the rate of changes in telomere length, inflammatory cytokines, and anti-CMV IgG titers. Our findings thus reveal that age-related trajectories of telomere attrition, elevated circulating inflammatory cytokines, and anti-CMV IgG are independent and that aging individuals do not show a uniform pattern of change in these variables. Immune aging processes are complex and vary across individuals, and the use of multiple biomarkers is essential to evaluation of biological aging of the immune system.

Published

2017