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    A Novel Drug Assay for Assessing the Transmission-Blocking Activity of Compounds on Field-Isolated Plasmodium falciparum Gametocytes.

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    Author
    Ouologuem, Dinkorma T
    Dembele, Laurent
    Dara, Antoine
    Kone, Aminatou K
    Diallo, Nouhoum
    Sangare, Cheick P O
    Ballo, Fatoumata I
    Dao, François
    Goita, Siaka
    Haidara, Aboubecrin S
    Traore, Aliou
    Niangaly, Amadou B
    Dama, Souleymane
    Sissoko, Sekou
    Sogore, Fanta
    Dara, Jacob N
    Barre, Yacouba N
    Daou, Amadou
    Cisse, Fatoumata
    Diakite, Ousmaila
    Doumbia, Diagassan
    Koumare, Sekou
    Fofana, Bakary
    Tandina, Fatalmoudou
    Sylla, Daman
    Sacko, Adama
    Coulibaly, Mamadou
    Tekete, Mamadou M
    Ouattara, Amed
    Djimde, Abdoulaye A
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    Date
    2022-11-02
    Type
    Article
    
    Metadata
    Show full item record
    See at
    https://doi.org/10.1128/aac.01001-22
    Abstract
    The discovery and development of transmission-blocking therapies challenge malaria elimination and necessitate standard and reproducible bioassays to measure the blocking properties of antimalarial drugs and candidate compounds. Most of the current bioassays evaluating the transmission-blocking activity of compounds rely on laboratory-adapted Plasmodium strains. Transmission-blocking data from clinical gametocyte isolates could help select novel transmission-blocking candidates for further development. Using freshly collected Plasmodium falciparum gametocytes from asymptomatic individuals, we first optimized ex vivo culture conditions to improve gametocyte viability and infectiousness by testing several culture parameters. We next pre-exposed ex vivo field-isolated gametocytes to chloroquine, dihydroartemisinin, primaquine, KDU691, GNF179, and oryzalin for 48 h prior to direct membrane feeding. We measured the activity of the drug on the ability of gametocytes to resume the sexual life cycle in Anopheles after drug exposure. Using 57 blood samples collected from Malian volunteers aged 6 to 15 years, we demonstrate that the infectivity of freshly collected field gametocytes can be preserved and improved ex vivo in a culture medium supplemented with 10% horse serum at 4% hematocrit for 48 h. Moreover, our optimized drug assay displays the weak transmission-blocking activity of chloroquine and dihydroartemisinin, while primaquine and oryzalin exhibited a transmission-blocking activity of ~50% at 1 μM. KDU691 and GNF179 both interrupted Plasmodium transmission at 1 μM and 5 nM, respectively. This new approach, if implemented, has the potential to accelerate the screening of compounds with transmission-blocking activity.
    Keyword
    culture
    direct membrane feeding assay
    drug assay
    ex vivo
    field-isolated gametocytes
    transmission-blocking activity
    Identifier to cite or link to this item
    http://hdl.handle.net/10713/20135
    ae974a485f413a2113503eed53cd6c53
    10.1128/aac.01001-22
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