Kinesin-8B controls basal body function and flagellum formation and is key to malaria transmission.

Mohammad Zeeshan ORCID logo; David Jp Ferguson ORCID logo; Steven Abel; Alana Burrrell ORCID logo; Edward Rea ORCID logo; Declan Brady; Emilie Daniel; Michael Delves ORCID logo; Sue Vaughan ORCID logo; Anthony A Holder ORCID logo; +3 more... Karine G Le Roch; Carolyn A Moores; Rita Tewari ORCID logo; (2019) Kinesin-8B controls basal body function and flagellum formation and is key to malaria transmission. Life science alliance, 2 (4). e201900488-e201900488. ISSN 2575-1077 DOI: 10.26508/lsa.201900488
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Eukaryotic flagella are conserved microtubule-based organelles that drive cell motility. Plasmodium, the causative agent of malaria, has a single flagellate stage: the male gamete in the mosquito. Three rounds of endomitotic division in male gametocyte together with an unusual mode of flagellum assembly rapidly produce eight motile gametes. These processes are tightly coordinated, but their regulation is poorly understood. To understand this important developmental stage, we studied the function and location of the microtubule-based motor kinesin-8B, using gene-targeting, electron microscopy, and live cell imaging. Deletion of the kinesin-8B gene showed no effect on mitosis but disrupted 9+2 axoneme assembly and flagellum formation during male gamete development and also completely ablated parasite transmission. Live cell imaging showed that kinesin-8B-GFP did not co-localise with kinetochores in the nucleus but instead revealed a dynamic, cytoplasmic localisation with the basal bodies and the assembling axoneme during flagellum formation. We, thus, uncovered an unexpected role for kinesin-8B in parasite flagellum formation that is vital for the parasite life cycle.


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