Published 8 November 2004. doi:10.1083/jcb.200406068
The Rockefeller University Press, 0021-9525 $8.00
JCB, Volume 167, Number 3, 425-432
A malaria membrane skeletal protein is essential for normal morphogenesis, motility, and infectivity of sporozoites
Emad I. Khater,
Robert E. Sinden, and
Johannes T. Dessens
Department of Biological Sciences, Imperial College London, London SW7 2AZ, England, UK
Correspondence to J.T. Dessens: j.dessens{at}imperial.ac.uk
Abstract
Membrane skeletons are structural elements that provide mechanical support to the plasma membrane and define cell shape. Here, we identify and characterize a putative protein component of the membrane skeleton of the malaria parasite. The protein, named PbIMC1a, is the structural orthologue of the Toxoplasma gondii inner membrane complex protein 1 (TgIMC1), a component of the membrane skeleton in tachyzoites. Using targeted gene disruption in the rodent malaria species Plasmodium berghei, we show that PbIMC1a is involved in sporozoite development, is necessary for providing normal sporozoite cell shape and mechanical stability, and is essential for sporozoite infectivity in insect and vertebrate hosts. Knockout of PbIMC1a protein expression reduces, but does not abolish, sporozoite gliding locomotion. We identify a family of proteins related to PbIMC1a in Plasmodium and other apicomplexan parasites. These results provide new functional insight in the role of membrane skeletons in apicomplexan parasite biology.
Abbreviations used in this paper: IFA, immunofluorescent antibody; IMC, inner membrane complex; SMT, subpellicular microtubules; SPN, subpellicular network; WT, wild-type.

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