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Journal of Cell Science 114, 3923-3932 (2001)
© 2001 The Company of Biologists Limited


RESEARCH ARTICLE

ABC transporters required for endocytosis and endosomal pH regulation in Dictyostelium

Derrick T. Brazill1,*, Lowell R. Meyer2, R. Diane Hatton1, Debra A. Brock1 and Richard H. Gomer1,2,{ddagger}

1 Howard Hughes Medical Institute
2 Department of Biochemistry and Cell Biology, MS-140, Rice University, 6100 S. Main Street, Houston, TX 77005-1892, USA
* Present address: Department of Biological Sciences Hunter College, Rm 927 North Building, 695 Park Avenue, New York, NY 10021, USA

{ddagger}Author for correspondence (e-mail: richard{at}bioc.rice.edu)

Accepted July 19, 2001

In Dictyostelium, the RtoA protein links both initial cell-type choice and physiological state to cell-cycle phase. rtoA cells (containing a disruption of the rtoA gene) generally do not develop past the mound stage, and have an abnormal ratio of prestalk and prespore cells. RtoA is also involved in fusion of endocytic/exocytic vesicles. Cells lacking RtoA, although having a normal endocytosis rate, have a decreased exocytosis rate and endosomes with abnormally low pHs. RtoA levels vary during the cell cycle, causing a cell-cycle-dependent modulation of parameters such as cytosolic pH (Brazill et al., 2000). To uncover other genes involved in the RtoA-mediated differentiation, we identified genetic suppressors of rtoA. One of these suppressors disrupted two genes, mdrA1 and mdrA2, a tandem duplication encoding two members of the ATP binding cassette (ABC) transporter superfamily. Disruption of mdrA1/mdrA2 results in release from the developmental block and suppression of the defect in initial cell type choice caused by loss of the rtoA gene. However, this is not accomplished by re-establishing the link between cell type choice and cell cycle phase. MdrA1 protein is localized to the endosome. mdrA1/mdrA2 cells (containing a disruption of these genes) have an endocytosis rate roughly 70% that of wild-type or rtoA cells, whereas mdrA1/mdrA2/rtoA cells have an endocytosis rate roughly 20% that of wild-type. The exocytosis rates of mdrA1/mdrA2 and mdrA1/mdrA2/rtoA are roughly that of wild-type. mdrA1/mdrA2 endosomes have an unusually high pH, whereas mdrA1/mdrA2/rtoA endosomes have an almost normal pH. The ability of mdrA1/mdrA2 disruption to rescue the cell-type proportion, developmental defects, and endosomal pH defects caused by rtoA disruption, and the ability of rtoA disruption to exacerbate the endocytosis defects caused by mdrA1/mdrA2 disruption, suggest a genetic interaction between rtoA, mdrA1 and mdrA2.

Key words: ABC, Multidrug, pH, Cell-type choice, Cell fate, Musical chairs




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© The Company of Biologists Ltd 2001