Stage‐specific depletion of myosin A supports an essential role in motility of malarial ookinetes
Summary Functional analysis of Plasmodium genes by classical reverse genetics is currently limited to mutants that are viable during erythrocytic schizogony, the pathogenic phase of the malaria parasite where transfection is performed. Here, we describe a conceptually simple experimental approach to...
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Published in | Cellular microbiology Vol. 13; no. 12; pp. 1996 - 2006 |
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Main Authors | , , , , , , , , |
Format | Journal Article |
Language | English |
Published |
Oxford, UK
Blackwell Publishing Ltd
01.12.2011
Hindawi Limited |
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Abstract | Summary
Functional analysis of Plasmodium genes by classical reverse genetics is currently limited to mutants that are viable during erythrocytic schizogony, the pathogenic phase of the malaria parasite where transfection is performed. Here, we describe a conceptually simple experimental approach to study the function of genes essential to the asexual blood stages in a subsequent life cycle stage by a promoter‐swap approach. As a proof of concept we targeted the unconventional class XIV myosin MyoA, which is known to be required for Toxoplasma gondii tachyzoite locomotion and host cell invasion. By placing the corresponding Plasmodium berghei gene, PbMyoA, under the control of the apical membrane antigen 1 (AMA1) promoter, expression in blood stages is maintained but switched off during transmission to the insect vector, i.e. ookinetes. In those mutant ookinetes gliding motility is entirely abolished resulting in a complete block of life cycle progression in Anopheles mosquitoes. Similar approaches should permit the analysis of gene function in the mosquito forms that are shared with the erythrocytic stages of the malaria parasite. |
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AbstractList | Summary
Functional analysis of Plasmodium genes by classical reverse genetics is currently limited to mutants that are viable during erythrocytic schizogony, the pathogenic phase of the malaria parasite where transfection is performed. Here, we describe a conceptually simple experimental approach to study the function of genes essential to the asexual blood stages in a subsequent life cycle stage by a promoter‐swap approach. As a proof of concept we targeted the unconventional class XIV myosin MyoA, which is known to be required for Toxoplasma gondii tachyzoite locomotion and host cell invasion. By placing the corresponding Plasmodium berghei gene, PbMyoA, under the control of the apical membrane antigen 1 (AMA1) promoter, expression in blood stages is maintained but switched off during transmission to the insect vector, i.e. ookinetes. In those mutant ookinetes gliding motility is entirely abolished resulting in a complete block of life cycle progression in Anopheles mosquitoes. Similar approaches should permit the analysis of gene function in the mosquito forms that are shared with the erythrocytic stages of the malaria parasite. Functional analysis of Plasmodium genes by classical reverse genetics is currently limited to mutants that are viable during erythrocytic schizogony, the pathogenic phase of the malaria parasite where transfection is performed. Here, we describe a conceptually simple experimental approach to study the function of genes essential to the asexual blood stages in a subsequent life cycle stage by a promoter-swap approach. As a proof of concept we targeted the unconventional class XIV myosin MyoA, which is known to be required for Toxoplasma gondii tachyzoite locomotion and host cell invasion. By placing the corresponding Plasmodium berghei gene, PbMyoA, under the control of the apical membrane antigen 1 (AMA1) promoter, expression in blood stages is maintained but switched off during transmission to the insect vector, i.e. ookinetes. In those mutant ookinetes gliding motility is entirely abolished resulting in a complete block of life cycle progression in Anopheles mosquitoes. Similar approaches should permit the analysis of gene function in the mosquito forms that are shared with the erythrocytic stages of the malaria parasite. Summary Functional analysis of Plasmodium genes by classical reverse genetics is currently limited to mutants that are viable during erythrocytic schizogony, the pathogenic phase of the malaria parasite where transfection is performed. Here, we describe a conceptually simple experimental approach to study the function of genes essential to the asexual blood stages in a subsequent life cycle stage by a promoter-swap approach. As a proof of concept we targeted the unconventional class XIV myosin MyoA, which is known to be required for Toxoplasma gondii tachyzoite locomotion and host cell invasion. By placing the corresponding Plasmodium berghei gene, PbMyoA, under the control of the apical membrane antigen 1 (AMA1) promoter, expression in blood stages is maintained but switched off during transmission to the insect vector, i.e. ookinetes. In those mutant ookinetes gliding motility is entirely abolished resulting in a complete block of life cycle progression in Anopheles mosquitoes. Similar approaches should permit the analysis of gene function in the mosquito forms that are shared with the erythrocytic stages of the malaria parasite. |
Author | Mendoza, Jacqueline Siden‐Kiamos, Inga Ganter, Markus Louis, Christos Matuschewski, Kai Sinden, Robert E. Steinbüchel, Marion Kunze, Andreas Hliscs, Marion |
Author_xml | – sequence: 1 givenname: Inga surname: Siden‐Kiamos fullname: Siden‐Kiamos, Inga – sequence: 2 givenname: Markus surname: Ganter fullname: Ganter, Markus – sequence: 3 givenname: Andreas surname: Kunze fullname: Kunze, Andreas – sequence: 4 givenname: Marion surname: Hliscs fullname: Hliscs, Marion – sequence: 5 givenname: Marion surname: Steinbüchel fullname: Steinbüchel, Marion – sequence: 6 givenname: Jacqueline surname: Mendoza fullname: Mendoza, Jacqueline – sequence: 7 givenname: Robert E. surname: Sinden fullname: Sinden, Robert E. – sequence: 8 givenname: Christos surname: Louis fullname: Louis, Christos – sequence: 9 givenname: Kai surname: Matuschewski fullname: Matuschewski, Kai |
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Notes | These authors contributed equally. Present address: Harvard School of Public Health, 665 Huntington Avenue, Boston, MA 02115, USA. Present address: European Molecular Biology Laboratory, 69117 Heidelberg, Germany. ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23 |
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Functional analysis of Plasmodium genes by classical reverse genetics is currently limited to mutants that are viable during erythrocytic schizogony,... Functional analysis of Plasmodium genes by classical reverse genetics is currently limited to mutants that are viable during erythrocytic schizogony, the... Summary Functional analysis of Plasmodium genes by classical reverse genetics is currently limited to mutants that are viable during erythrocytic schizogony,... |
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SubjectTerms | Animals Anopheles Anopheles - parasitology Antigens, Protozoan - genetics Antigens, Protozoan - metabolism Female Gene Deletion Gene Expression Profiling Gene Expression Regulation Genes, Protozoan Genetic Complementation Test Locomotion Membrane Proteins - genetics Membrane Proteins - metabolism Mice Microinjections Myosins - genetics Myosins - metabolism Oocysts - metabolism Plasmodium berghei Plasmodium berghei - genetics Promoter Regions, Genetic Protozoan Proteins - genetics Protozoan Proteins - metabolism Sporozoites - metabolism Toxoplasma - genetics Toxoplasma - metabolism Toxoplasma - pathogenicity Toxoplasma gondii Toxoplasmosis - parasitology Transfection |
Title | Stage‐specific depletion of myosin A supports an essential role in motility of malarial ookinetes |
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