<i>piggyBac</i>transposon mediated transgenesis of the human blood fluke,<i>Schistosoma mansoni</i>

Morales, Maria E.; Mann, Victoria H.; Kines, Kristine J.; Gobert, Geoffrey N.; Fraser, Malcolm J.; Kalinna, Bernd H.; Correnti, Jason; Pearce, Edward J.; Brindley, Paul J.

doi:10.1096/fj.07-8726com

Cited by 85 publications

(100 citation statements)

References 64 publications

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“…Attenuated growth of the C9 MKP-null mutant remained stable over multiple subsequent generations, suggesting that survival was not due to phenotype reversion. This is consistent with general experience using the piggyBac system as it is now extensively used in a number of organisms, and the transposable elements remain integrated in the genome in the absence of transposase (31,(54)(55)(56)(57)(58). However, the extended maintenance of P. falciparum intraerythrocytic cultures required for transfection and the selection process in the experimental studies increases the possibility for secondary mutations to alter the cell cycle or cause growth attenuation.…”

Section: Identification Of An Attenuated Growth Mutant In P Falciparumsupporting

confidence: 84%

Atypical Mitogen-Activated Protein Kinase Phosphatase Implicated in Regulating Transition from Pre-S-Phase Asexual Intraerythrocytic Development of Plasmodium falciparum

et al. 2013

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Intraerythrocytic development of the human malaria parasite Plasmodium falciparum appears as a continuous flow through growth and proliferation. To develop a greater understanding of the critical regulatory events, we utilized piggyBac insertional mutagenesis to randomly disrupt genes. Screening a collection of piggyBac mutants for slow growth, we isolated the attenuated parasite C9, which carried a single insertion disrupting the open reading frame (ORF) of PF3D7_1305500. This gene encodes a protein structurally similar to a mitogen-activated protein kinase (MAPK) phosphatase, except for two notable characteristics that alter the signature motif of the dual-specificity phosphatase domain, suggesting that it may be a low-activity phosphatase or pseudophosphatase. C9 parasites demonstrated a significantly lower growth rate with delayed entry into the S/M phase of the cell cycle, which follows the stage of maximum PF3D7_1305500 expression in intact parasites. Genetic complementation with the full-length PF3D7_1305500 rescued the wild-type phenotype of C9, validating the importance of the putative protein phosphatase PF3D7_1305500 as a regulator of pre-S-phase cell cycle progression in P. falciparum. Malaria caused by Plasmodium falciparum infection is the major type of severe malaria and results in hundreds of thousands of deaths each year and hundreds of millions of clinical illnesses (1, 2). Within the blood of infected individuals, asexual forms of the intraerythrocytic parasite grow rapidly through successive cycles of growth and proliferation. In each asexual generation, active entry into erythrocytes is followed by a growth phase culminating in dynamic release of erythrocyte-invading merozoites. The Plasmodium mitotic cycle is not fully understood and differs from the well-defined models established in yeast and mammalian cells (3). Observing the exact mitotic transitions during the cycle has been difficult due to variations in processes such as chromatid segregation, nuclear division, and spindle formation (4). However, this pattern of development has been observed in other members of the Apicomplexa, such as Toxoplasma gondii and Eimeria tenella, demonstrating the importance and conservation of this process across the phylum (5, 6).In eukaryotic systems, phosphorylation cascades are critical to cellular development and depend on the coordinated activity of kinases, which are in turn modulated by the activity of phosphatases. There is growing evidence that kinases are critical regulators of cell growth and development in Plasmodium species (7-9). Plasmodium kinases, for example, have been found to be involved with the initial invasion of host cells in addition to egress and differentiation (6, 10). Additional studies have identified kinases in phosphorylation cascades of the gametocyte-ookinete-oocyst transition in the mosquito midgut (11)(12)(13)(14)(15)(16)(17). In contrast, few studies have described the phosphatases involved in these processes, which would understandably function with kinases to coregul...

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Section: Identification Of An Attenuated Growth Mutant In P Falciparumsupporting

confidence: 84%

Atypical Mitogen-Activated Protein Kinase Phosphatase Implicated in Regulating Transition from Pre-S-Phase Asexual Intraerythrocytic Development of Plasmodium falciparum

et al. 2013

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“…Similar findings have been described in schistosomes, and stage- and tissue-specific expression of schistosome genes has been investigated using reporter transgenes driven by the promoters of schistosome genes, including cathepsin L (125). Recently, Brindley and coworkers have described somatic transgenesis of S. mansoni facilitated by either the piggyBac transposon (126) or the murine leukemia retrovirus (127), including the first demonstration of integration of reporter genes into the chromosomes of a parasitic worm.…”

Section: Helminth Genomics Postgenomics and Gene Manipulationmentioning

confidence: 62%

Helminth infections: the great neglected tropical diseases

et al. 2008

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Helminths are parasitic worms. They are the most common infectious agents of humans in developing countries and produce a global burden of disease that exceeds better-known conditions, including malaria and tuberculosis. As we discuss here, new insights into fundamental helminth biology are accumulating through newly completed genome projects and the nascent application of transgenesis and RNA interference technologies. At the same time, our understanding of the dynamics of the transmission of helminths and the mechanisms of the Th2-type immune responses that are induced by infection with these parasitic worms has increased markedly. Ultimately, these advances in molecular and medical helminth biology should one day translate into a new and robust pipeline of drugs, diagnostics, and vaccines for targeting parasitic worms that infect humans.

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“…Both vector-based RNAi and expression of foreign transgenes have begun to be deployed in studies with schistosomes, with potential outcomes including validation of putative vaccine candidates and even the overexpression of candidate antigens. Pseudotyped murine leukemia virus and the piggyBac transposon have both been shown to transduce developmental stages of schistosomes, leading to chromosomal integration of retroviral transgenes and transgene reporter activity Morales et al, 2007;Yang et al, 2010). Moreover, a vector-based RNAi approach has been reported in which the MLV transgene encoded a long hairpin RNA specific for a schistosome protease involved in hemoglobinolysis (Tchoubrieva et al 2010).…”

Section: Schistosomesmentioning

confidence: 99%

Vaccinomics for the Major Blood Feeding Helminths of Humans

Loukas

Gaze

Mulvenna

et al. 2011

OMICS: A Journal of Integrative Biology

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Approximately one billion people are infected with hookworms and/or blood flukes (schistosomes) in developing countries. These two parasites are responsible for more disability adjusted life years lost than most other neglected tropical diseases (NTDs), and together, are second only to malaria. Although anthelmintic drugs are effective and widely available, they do not protect against reinfection, resistant parasites are likely to emerge, and mass drug administration programs are unsustainable. Therefore, there is a pressing need for the development of vaccines against these parasites. In recent years, there have been major advances in our understanding of hookworms and schistosomes at the molecular level through the use of ''omics'' technologies. The secretomes of these parasites have been characterized using transcriptomics, genomics, proteomics, and newly developed gene manipulation and silencing techniques, and the proteins of interest are now the target of novel antigen discovery approaches, notably immunomics. This research has resulted in the discovery, development, and early stage clinical trials of subunit vaccines against hookworms and schistosomes.

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piggyBactransposon mediated transgenesis of the human blood fluke,Schistosoma mansoni

Cited by 85 publications

References 64 publications

Atypical Mitogen-Activated Protein Kinase Phosphatase Implicated in Regulating Transition from Pre-S-Phase Asexual Intraerythrocytic Development of Plasmodium falciparum

Atypical Mitogen-Activated Protein Kinase Phosphatase Implicated in Regulating Transition from Pre-S-Phase Asexual Intraerythrocytic Development of Plasmodium falciparum

Helminth infections: the great neglected tropical diseases

Vaccinomics for the Major Blood Feeding Helminths of Humans

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