Functional dissection of the apicomplexan glideosome molecular architecture.

Abstract : The glideosome of apicomplexan parasites is an actin- and myosin-based machine located at the pellicle, between the plasma membrane (PM) and inner membrane complex (IMC), that powers parasite motility, migration, and host cell invasion and egress. It is composed of myosin A, its light chain MLC1, and two gliding-associated proteins, GAP50 and GAP45. We identify GAP40, a polytopic protein of the IMC, as an additional glideosome component and show that GAP45 is anchored to the PM and IMC via its N- and C-terminal extremities, respectively. While the C-terminal region of GAP45 recruits MLC1-MyoA to the IMC, the N-terminal acylation and coiled-coil domain preserve pellicle integrity during invasion. GAP45 is essential for gliding, invasion, and egress. The orthologous Plasmodium falciparum GAP45 can fulfill this dual function, as shown by transgenera complementation, whereas the coccidian GAP45 homolog (designated here as) GAP70 specifically recruits the glideosome to the apical cap of the parasite.
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Cell Host and Microbe, Elsevier, 2010, 8 (4), pp.343-57. 〈10.1016/j.chom.2010.09.002〉
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Contributeur : Valérie Polonais <>
Soumis le : lundi 6 mai 2013 - 11:56:24
Dernière modification le : jeudi 11 janvier 2018 - 06:23:13

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Karine Frénal, Valérie Polonais, Jean-Baptiste Marq, Rolf Stratmann, Julien Limenitakis, et al.. Functional dissection of the apicomplexan glideosome molecular architecture.. Cell Host and Microbe, Elsevier, 2010, 8 (4), pp.343-57. 〈10.1016/j.chom.2010.09.002〉. 〈hal-00820623〉

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