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Eukaryotic Cell, August 2003, p. 769-777, Vol. 2, No. 4
1535-9778/03/$08.00+0 DOI: 10.1128/EC.2.4.769-777.2003
Copyright © 2003, American Society for Microbiology. All Rights Reserved.
Parasitology Section, Bernhard-Nocht-Institute for Tropical Medicine, D-20359 Hamburg,1 Abteilung Membranbiochemie, Max-Planck-Institut für Biologie, D-72076 Tübingen, Germany2
Received 23 May 2003/ Accepted 9 June 2003
During its life cycle, the parasitic protozoon Leishmania mexicana differentiates from a flagellated form, the promastigote, to an amastigote form carrying a rudimentary flagellum. Besides biochemical changes, this process involves a change in overall cell morphology including flagellar shortening. A mitogen-activated protein kinase kinase homologue designated LmxMKK was identified in a homology screening and found to be critically involved in the regulation of flagellar assembly and cell size. LmxMKK is exclusively expressed in the promastigote stage and is likely to be regulated by posttranslational mechanisms such as phosphorylation. A deletion mutant for the single-copy gene revealed motile flagella dramatically reduced in length and lacking the paraflagellar rod, a structure adjacent to the axoneme in kinetoplastid flagella. Moreover, a fraction of the cells showed perturbance of the axonemal structure. Complementation of the deletion mutant with the wild-type gene restored typical promastigote morphology. We propose that LmxMKK influences anterograde intraflagellar transport to maintain flagellar length in Leishmania promastigotes; as such, it is the first protein kinase known to be involved in organellar assembly.
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