Malaria transmission assisted by interaction between<i>Plasmodium α</i>-tubulin-1 and<i>Anopheles</i>FREP1 protein

Zhang, Genwei; Niu, Guodong; Perez, Laura; Wang, Xiaohong; Li, Jun

doi:10.1101/2019.12.16.878082

2019

DOI: 10.1101/2019.12.16.878082

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Malaria transmission assisted by interaction betweenPlasmodium α-tubulin-1 andAnophelesFREP1 protein

Genwei Zhang

Guodong Niu

Laura Perez

et al.

Abstract: Passage of Plasmodium through a mosquito midgut is essential for malaria transmission. FREP1, a peritrophic matrix protein in a mosquito midgut, binds to the parasite and mediates Plasmodium infection in Anopheles. The FREP1-mediated Plasmodium invasion pathway is highly conserved across multiple species of Plasmodium and Anopheles. Through pulldown, nine P. berghei proteins were co-precipitated with FREP1-conjugated beads. After cloning these nine genes from P. berghei and expressing them in insect cells, six… Show more

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Cited by 2 publications

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References 19 publications

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“…Development of the vaccines that interrupt malaria transmission (VIMTs) was emphasized by the vaccine consultative group for countries that have passed the pre-elimination step and have proceeded to the global goal [10]. VIMTs are divided into various types; one type is the classical transmissionblocking vaccine that blocks the sexual parasite development by targeting the required effector molecules in the vector, including mosquito-based transmission-blocking vaccines with targets such as Anopheles gambiae aminopeptidase N-1 (AgAPN-1) [11], CPBAg1 (Carboxy Peptidase B1) [12,13], Trypsin [14], saglin [15], FREP 1 [16,17], and SGS1 [18]. APN-1 is a candidate molecule for which the blocking efficacy against Plasmodium falciparum in An.…”

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confidence: 99%

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Identification, molecular characterization and expression of aminopeptidase N-1 (APN-1) from Anopheles stephensi in SF9 cell line as a candidate molecule for developing a vaccine that interrupt malaria transmission

Pakdel

Zakeri

et al. 2020

Malar J

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Background: According to the World Health Organization reports, billions of people around the world are at risk for malaria disease and it is important to consider the preventive strategies for protecting the people that are living in high risk areas. One of the main reasons of disease survival is diversity of vectors and parasites in different malaria regions that have their specific features, behaviour and biology. Therefore, specific regional strategies are necessary for successful control of malaria. One of the tools that needs to be developed for elimination and prevention of reintroduction of malaria is a vaccine that interrupt malaria transmission (VIMTs). VIMT is a broad concept that should be adjusted to the biological characteristics of the disease in each region. One type of VIMT is a vector-based vaccine that affects the sexual stage of Plasmodium life cycle. According to recent studies, the aminopeptidase N-1 of Anopheles gambiae (AgAPN-1) is as a potent vector-based VIMT with considerable inhibition activity against the sexual stage of Plasmodium parasite.Methods: Systems for rapid amplification of cDNA ends (3ʹ-RACE) and genome walking methods were used for sequence determination of apn-1 gene from Anopheles stephensi and distinct bioinformatics software were used for structural analysis. AsAPN-1 was expressed in Spodoptera frugiperda (Sf9) insect cell line using the baculovirus expression system. Recombinant AsAPN-1 was purified under the hybrid condition and its biological activity was assayed.

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confidence: 99%

“…gambiae. Some glycoproteins, such as APN-1, are receptors for the lectin-similar structures of ookinete that trigger the attachment of ookinetes to the internal side of the epithelium and are essential for preceding the sexual development of parasite in the mosquito midgut [13,16,20].…”

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confidence: 99%

Identification, molecular characterization and expression of aminopeptidase N-1 (APN-1) from Anopheles stephensi in SF9 cell line as a candidate molecule for developing a vaccine that interrupt malaria transmission

Pakdel

Zakeri

et al. 2020

Malar J

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Molecular interactions between parasite and mosquito during midgut invasion as targets to block malaria transmission

Keleta

Ramelow

2021

npj Vaccines

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Despite considerable effort, malaria remains a major public health burden. Malaria is caused by five Plasmodium species and is transmitted to humans via the female Anopheles mosquito. The development of malaria vaccines against the liver and blood stages has been challenging. Therefore, malaria elimination strategies advocate integrated measures, including transmission-blocking approaches. Designing an effective transmission-blocking strategy relies on a sophisticated understanding of the molecular mechanisms governing the interactions between the mosquito midgut molecules and the malaria parasite. Here we review recent advances in the biology of malaria transmission, focusing on molecular interactions between Plasmodium and Anopheles mosquito midgut proteins. We provide an overview of parasite and mosquito proteins that are either targets for drugs currently in clinical trials or candidates of promising transmission-blocking vaccines.

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Malaria transmission assisted by interaction betweenPlasmodium α-tubulin-1 andAnophelesFREP1 protein

Cited by 2 publications

References 19 publications

Identification, molecular characterization and expression of aminopeptidase N-1 (APN-1) from Anopheles stephensi in SF9 cell line as a candidate molecule for developing a vaccine that interrupt malaria transmission

Identification, molecular characterization and expression of aminopeptidase N-1 (APN-1) from Anopheles stephensi in SF9 cell line as a candidate molecule for developing a vaccine that interrupt malaria transmission

Molecular interactions between parasite and mosquito during midgut invasion as targets to block malaria transmission

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