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Saccharomyces cerevisiae Multidrug Resistance Transporter Qdr2 Is Implicated in Potassium Uptake, Providing a Physiological Advantage to Quinidine-Stressed Cells
Author(s) -
Rita C. Vargas,
Raúl García-Salcedo,
Sandra Tenreiro,
Miguel C. Teixeira,
Alexandra R. Fernandes,
José Ramos,
Isabel SáCorreia
Publication year - 2007
Publication title -
eukaryotic cell
Language(s) - English
Resource type - Journals
eISSN - 1535-9778
pISSN - 1535-9786
DOI - 10.1128/ec.00290-06
Subject(s) - quinidine , saccharomyces cerevisiae , antiporter , biology , biochemistry , yeast , intracellular , efflux , amino acid , microbiology and biotechnology , pharmacology , membrane
TheQDR2 gene ofSaccharomyces cerevisiae encodes a putative plasma membrane drug:H+ antiporter that confers resistance against quinidine, barban, bleomycin, and cisplatin. This work provides experimental evidence of defective K+ (Rb+ ) uptake in the absence ofQDR2 . The direct involvement of Qdr2p in K+ uptake is reinforced by the fact that increased K+ (Rb+ ) uptake due toQDR2 expression is independent of the Trk1p/Trk2p system.QDR2 expression confers a physiological advantage for the yeast cell during the onset of K+ limited growth, due either to a limiting level of K+ in the growth medium or to the presence of quinidine. This drug decreases the K+ uptake rate and K+ accumulation in the yeast cell, especially in the Δqdr2 mutant. Qdr2p also helps to sustain the decrease of intracellular pH in quinidine-stressed cells in growth medium at pH 5.5 by indirectly promoting H+ extrusion affected by the drug. The results are consistent with the hypothesis that Qdr2p may also couple K+ movement with substrate export, presumably with quinidine. Other clues to the biological role ofQDR2 in the yeast cell come from two additional lines of experimental evidence. First,QDR2 transcription is activated under nitrogen (NH4 + ) limitation or when the auxotrophic strain examined enters stationary phase due to leucine limitation, this regulation being dependent on general amino acid control by Gcn4p. Second, the amino acid pool is higher in Δqdr2 cells than in wild-type cells, indicating thatQDR2 expression is, directly or indirectly, involved in amino acid homeostasis.

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