The cell biology of malaria infection of mosquito: advances and opportunities

Sinden, Robert E.

doi:10.1111/cmi.12413

Cited by 61 publications

(62 citation statements)

References 192 publications

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“…In the mosquito midgut, the gametes mate to form a zygote that develops further into the motile ookinete. After crossing the midgut epithelium and establishing a sessile oocyst, the ookinete gives rise to thousands of sporozoites capable of infecting a subsequent mammalian host (1).…”

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confidence: 99%

Maternally supplied S-acyl-transferase is required for crystalloid organelle formation and transmission of the malaria parasite

Santos

Duarte

Kehrer

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Transmission of the malaria parasite from the mammalian host to the mosquito vector requires the formation of adequately adapted parasite forms and stage-specific organelles. Here we show that formation of the crystalloid-a unique and short-lived organelle of the Plasmodium ookinete and oocyst stage required for sporogonyis dependent on the precisely timed expression of the S-acyltransferase DHHC10. DHHC10, translationally repressed in female Plasmodium berghei gametocytes, is activated translationally during ookinete formation, where the protein is essential for the formation of the crystalloid, the correct targeting of crystalloid-resident protein LAP2, and malaria parasite transmission.T he malaria parasite is capable of infecting both the vertebrate host and mosquito vector. After a mosquito blood meal, sexual precursor cells rapidly differentiate into mature gametes. In the mosquito midgut, the gametes mate to form a zygote that develops further into the motile ookinete. After crossing the midgut epithelium and establishing a sessile oocyst, the ookinete gives rise to thousands of sporozoites capable of infecting a subsequent mammalian host (1).Sharing key organelles like the nucleus, endoplasmic reticulum, Golgi, and mitochondria with other eukaryotes, this parasite has evolved specialized, stage-specific structures that are necessary for developmental progression during parasite transmission. These include, for example, osmiophilic bodies (secretory vesicles) that release protein factors capable of lysing the parasitophorous vacuole and erythrocyte membranes, thus producing free gametes (2) and a gliding motility motor anchored to the inner membrane complex (IMC), allowing the ookinete to migrate across the mosquito midgut epithelium and establish an oocyst (3). Sporozoite formation in the oocyst finally requires the presence of a stage-specific organelle, the crystalloid, a multivesicular structure assembled in the ookinete and putative reservoir of proteins and lipids used during sporogony. Although this enigmatic organelle was discovered more than 40 y ago, its formation and function remain largely unknown (4-9). Six LCCL proteins have been shown to reside within (9) and maintain the stability (8, 9) of these organelles essential for sporogony (10).The morphological changes taking place during zygote-toookinete development and the generation of thousands of sporozoites inside a single oocyst require extensive protein translation and membrane biogenesis to support the formation of organelles and plasma membrane (PM) surrounding each new parasite. Onethird of the proteins identified in the oocyst and oocyst-derived (midgut) sporozoites of the human parasite Plasmodium falciparum are putatively membrane-bound (11). The targeting of such proteins to organelles, and perhaps formation of certain organelles per se, requires appropriate sorting signals, along with transmembrane (TM) domains to keep these factors in place. Posttranslational modifications, such as lipidation, can increase the affinity of a modif...

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confidence: 99%

Maternally supplied S-acyl-transferase is required for crystalloid organelle formation and transmission of the malaria parasite

Santos

Duarte

Kehrer

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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“…16 The bacterial population increases hundreds of times and may stimulate the mosquito's immune response, which includes the production of AMP, ROS and nitric oxide (NO). 16 Plasmodium gametocytes transform to gametes and fertilization produces mobile ookinetes that interact with the insect midgut molecules, invade, and establish the infection on the midgut outer surface 17 ( figure 1). The interacting parasite and midgut molecules are the basis for transmission blocking vaccines (TBV), which aim at inducing host antibodies against molecules critical for parasite development and vector-parasite interactions.…”

Section: Discussionmentioning

confidence: 99%

Pathogen-insect interaction candidate molecules for transmission-blocking control strategies of vector borne diseases

Zumaya-Estrada¹,

Rodríguez²,

Rodrı́guez³

2017

Salud Publica Mex

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Zumaya ResumenObjetivo. Analizar el conocimiento actual de las interacciones patógeno-insecto susceptibles a incluirse en el diseño de estrategias moleculares para el control de enfermedades transmitidas por vectores. Material y métodos. Se examinaron los agentes causales de la malaria, el dengue y la enfermedad de Chagas, y las moléculas de insectos que participan en interacciones durante la infección de sus vectores. Resultados. Se presentan moléculas de patógenos que participan en la invasión del intestino del insecto y moléculas inmunes inducidas en los vectores. Se discute su inclusión en vacunas bloqueadoras de transmisión (VBT) y en la modificación genética de vectores (MGI) o de sus bacterias simbióticas. Conclusión. La interrupción de procesos mediante el bloqueo de las interacciones patógeno-vector proporciona varios candidatos para las estrategias de control molecular, pero la eficacia de VBT y MGI es aún limitada y los efectos secundarios de MGI (aumento de la transmisión de otros patógenos y afectación de otros organismos) deben descartase.

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“…Gametocytes are highly specialized cells, very different to the asexual pathogenic stages [6]. In P. vivax, gametocytes require only a slightly longer time to develop than that required for asexual stages to complete their multiplication cycle.…”

Section: Malaria: From Control To Eliminationmentioning

confidence: 99%

“…bone marrow) during development and only mature stage V gametocytes circulating in the blood stream where they can be transmitted to mosquitoes [8]. After the stochastic, epigenetically driven [9][10][11][12] gametocyte conversion rate of ~1% of the asexual population [6], the immature stage I-III gametocytes are to some extent biochemically more aligned to asexual parasites than their stage V partners [8] whose metabolism effectively decreases to only retain household activities such as ATP production and redox maintenance [13]. This raises unique issues in the identification of drugs active on P. falciparum gametocytes, and specifically on the mature stage V forms, compared for instance to those of P.…”

Section: Malaria: From Control To Eliminationmentioning

confidence: 99%

Discovering New Transmission-Blocking Antimalarial Compounds: Challenges and Opportunities

Birkholtz

Coetzer

Mancama

et al. 2016

Trends in Parasitology

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The ability to target human-mosquito parasite transmission challenges global malaria elimination. However, it is not obvious what a transmission-blocking drug will look like; should it 1) target only parasite transmission stages; 2) be combined with a partner drug killing the pathogenic asexual stages or 3) kill both the sexual and asexual blood stages, preferably displaying polypharmacology. The development of transmission-blocking anti-malarials requires objective analyses of the current strategies. Here, pertinent issues and unanswered questions regarding the target candidate profile of a

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The cell biology of malaria infection of mosquito: advances and opportunities

Cited by 61 publications

References 192 publications

Maternally supplied S-acyl-transferase is required for crystalloid organelle formation and transmission of the malaria parasite

Maternally supplied S-acyl-transferase is required for crystalloid organelle formation and transmission of the malaria parasite

Pathogen-insect interaction candidate molecules for transmission-blocking control strategies of vector borne diseases

Discovering New Transmission-Blocking Antimalarial Compounds: Challenges and Opportunities

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