Disruption of plasmepsin-4 and merozoites surface protein-7 genes in Plasmodium berghei induces combined virulence-attenuated phenotype

Roberta Spaccapelo; Elena Aime; Sara Caterbi; Paola Arcidiacono; Barbara Capuccini; Manlio Di Cristina; Tania Dottorini; Mario Rende; Francesco Bistoni; Andrea Crisanti

doi:10.1038/srep00039

Disruption of plasmepsin-4 and merozoites surface protein-7 genes in Plasmodium berghei induces combined virulence-attenuated phenotype

Roberta Spaccapelo, Elena Aime, Sara Caterbi, Paola Arcidiacono, Barbara Capuccini, Manlio Di Cristina, Tania Dottorini, Mario Rende, Francesco Bistoni, Andrea Crisanti

Research output: Journal Publication › Article › peer-review

22 Citations (Scopus)

Abstract

Blood stage malaria parasites causing a mild and self limited infection in mice have been obtained with either radiation or chemical mutagenesis showing the possibility of developing an attenuated malaria vaccine. Targeted disruption of plasmepsin-4 (pm4) or the merozoite surface protein-7 (msp7) genes also induces a virulence-attenuated phenotype in terms of absence of experimental cerebral malaria (ECM), delayed increase of parasitemia and reduced mortality rate. The decrease in virulence in parasites lacking either pm4 or msp7 is however incomplete and dependent on the parasite and mouse strain combination. The sequential disruption of both genes induced remarkable virulence-attenuated blood-stage parasites characterized by a self-resolving infection with low levels of parasitemia and no ECM. Furthermore, convalescent mice were protected against the challenge with P. berghei or P. yoelii parasites for several months. These observations provide a proof-of-concept step for the development of human malaria vaccines based on genetically attenuated blood-stage parasites.

Original language	English
Article number	39
Journal	Scientific Reports
Volume	1
DOIs	https://doi.org/10.1038/srep00039
Publication status	Published - 2011
Externally published	Yes

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@article{8e4f748962d943dd90e8596b82d8822b,

title = "Disruption of plasmepsin-4 and merozoites surface protein-7 genes in Plasmodium berghei induces combined virulence-attenuated phenotype",

abstract = "Blood stage malaria parasites causing a mild and self limited infection in mice have been obtained with either radiation or chemical mutagenesis showing the possibility of developing an attenuated malaria vaccine. Targeted disruption of plasmepsin-4 (pm4) or the merozoite surface protein-7 (msp7) genes also induces a virulence-attenuated phenotype in terms of absence of experimental cerebral malaria (ECM), delayed increase of parasitemia and reduced mortality rate. The decrease in virulence in parasites lacking either pm4 or msp7 is however incomplete and dependent on the parasite and mouse strain combination. The sequential disruption of both genes induced remarkable virulence-attenuated blood-stage parasites characterized by a self-resolving infection with low levels of parasitemia and no ECM. Furthermore, convalescent mice were protected against the challenge with P. berghei or P. yoelii parasites for several months. These observations provide a proof-of-concept step for the development of human malaria vaccines based on genetically attenuated blood-stage parasites.",

author = "Roberta Spaccapelo and Elena Aime and Sara Caterbi and Paola Arcidiacono and Barbara Capuccini and {Di Cristina}, Manlio and Tania Dottorini and Mario Rende and Francesco Bistoni and Andrea Crisanti",

note = "Funding Information: We thank MR4 for providing us with plasmid pL0008 (MRA-797) and P. yoelii 17X (MRA-426). We also thank Chris Janse for providing 1037cl1 parasite line. This work was supported by grants of the Italian Ministry of Research FIRB (Basic Research Investments Programme). The funders had no role in study design, data collection and analysis, decision to publish, or preparation on the manuscript.",

year = "2011",

doi = "10.1038/srep00039",

language = "English",

volume = "1",

journal = "Scientific Reports",

issn = "2045-2322",

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AU - Spaccapelo, Roberta

AU - Aime, Elena

AU - Caterbi, Sara

AU - Arcidiacono, Paola

AU - Capuccini, Barbara

AU - Di Cristina, Manlio

AU - Dottorini, Tania

AU - Rende, Mario

AU - Bistoni, Francesco

AU - Crisanti, Andrea

N1 - Funding Information: We thank MR4 for providing us with plasmid pL0008 (MRA-797) and P. yoelii 17X (MRA-426). We also thank Chris Janse for providing 1037cl1 parasite line. This work was supported by grants of the Italian Ministry of Research FIRB (Basic Research Investments Programme). The funders had no role in study design, data collection and analysis, decision to publish, or preparation on the manuscript.

PY - 2011

Y1 - 2011

N2 - Blood stage malaria parasites causing a mild and self limited infection in mice have been obtained with either radiation or chemical mutagenesis showing the possibility of developing an attenuated malaria vaccine. Targeted disruption of plasmepsin-4 (pm4) or the merozoite surface protein-7 (msp7) genes also induces a virulence-attenuated phenotype in terms of absence of experimental cerebral malaria (ECM), delayed increase of parasitemia and reduced mortality rate. The decrease in virulence in parasites lacking either pm4 or msp7 is however incomplete and dependent on the parasite and mouse strain combination. The sequential disruption of both genes induced remarkable virulence-attenuated blood-stage parasites characterized by a self-resolving infection with low levels of parasitemia and no ECM. Furthermore, convalescent mice were protected against the challenge with P. berghei or P. yoelii parasites for several months. These observations provide a proof-of-concept step for the development of human malaria vaccines based on genetically attenuated blood-stage parasites.

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Disruption of plasmepsin-4 and merozoites surface protein-7 genes in Plasmodium berghei induces combined virulence-attenuated phenotype

Abstract

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UN SDGs

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