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Absence of developmental and reproductive toxicity in rats, rabbits, and zebrafish embryos exposed to antimalarial drug cabamiquine.

Andreas GadoPhilip HewittPeter BallardBelen TornesiTobias Hyun Ho BaeurleClaude OeuvrayThomas SpangenbergClaudia Demarta-Gatsi
Published in: Birth defects research (2024)
The results obtained in a full set of reproductive toxicity studies did not provide evidence of detrimental effects on the conceptuses and progeny at maternally nontoxic doses and exposures, still representing a multiple of the anticipated systemic exposures in women of childbearing potential (WOCBP). Cabamiquine can therefore be considered a suitable therapeutic option for WOCBP and pregnant women living in malaria-endemic regions by significantly reducing maternal and infant malaria death rates.
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