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(Received for publication, October 16, 1995; and in revised form, December 11, 1995)
The multidrug resistance-associated protein (MRP) is a member of
the ATP binding cassette superfamily of transporters which includes the
mammalian P-glycoproteins (P-gp) family. In order to facilitate the
biochemical and genetic analyses of MRP, we have expressed human MRP in
the yeast Saccharomyces cerevisiae and have compared its
functional properties to those of the mouse Mdr3 P-gp isoform.
Expression of both MRP and Mdr3 in the anthracycline hypersensitive
mutant VASY2563 restored cellular resistance to Adriamycin in this
mutant. MRP and Mdr3 expression produced pleiotropic effects on drug
resistance in this mutant, as corresponding VASY2563 transformants also
acquired resistance to the anti-fungal agent FK506 and to the
K/H
ionophore valinomycin. The
appearance of increased cellular resistance to the toxic effect of
Adriamycin (ADM) in MRP and Mdr3 transformants was concomitant with a
reduced intracellular accumulation of [
C]ADM in
spheroplasts prepared from these cells. Moreover, MRP and Mdr3, but not
control spheroplasts, could mediate a time-dependent reduction in the
overall cell-associated [
C]ADM from preloaded
cells, suggesting the presence of an active ADM transport mechanism in
MRP and Mdr3 transformants. Finally, human MRP was found to complement
the biological activity of the yeast peptide pheromone transporter Ste6 and partially restored mating in a sterile ste6 null mutant. These findings suggest that despite their relatively
low level of structural homology, MRP and P-gp share similar functional
aspects, since both proteins can mediate transport of chemotherapeutic
drugs and the a mating peptide pheromone in yeast.
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