
pmid: 24583862
The stereoselective transport of methotrexate (L-amethopterin, L-MTX) and its antipode (D-amethopterin, D-MTX) by human reduced folate carrier (hRFC) has been examined in HEK293 cells expressing H27-hRFC and R27-hRFC. The uptake of both L-MTX and D-MTX increased as the extracellular pH increased from 6.0 to 7.4. The initial uptake rate of L-MTX into the H27- and R27-hRFCs of the HEK293 cells followed Michaelis-Menten kinetics with Km values of approximately 0.24 and 0.47 µM, respectively. Dixon plots revealed that the [(3)H]-L-MTX uptake mediated by the H27- and R27-hRFCs was inhibited competitively by unlabeled L-MTX with Ki values of approximately 0.1 and 0.5 µM, respectively. D-MTX also competitively inhibited the H27- and R27-hRFC mediated uptake of [(3)H]-L-MTX with Ki values of approximately 3.4 and 3.2 µM, respectively. The RFC-mediated uptake clearance of L-MTX was approximately 15-fold greater than that of D-MTX in the H27-hRFC-HEK293 cells, and was more than 30-fold greater than that of D-MTX in the R27-hRFC-HEK293 cells. The results of the current study have revealed that the enantiomers of MTX enantiomers can be transported in a stereoselective manner by the H27- and R27-hRFCs because of significant differences in the affinities of the enantiomers to the hRFC.
Adult, Male, stereoselective transport, Biological Transport, Stereoisomerism, Hydrogen-Ion Concentration, Transfection, methotrexate, Kinetics, Reduced Folate Carrier Protein, Young Adult, HEK293 Cells, Methotrexate, single nucleotide polymorphism, Folic Acid Antagonists, Humans, reduced folate carrier, amethopterin
Adult, Male, stereoselective transport, Biological Transport, Stereoisomerism, Hydrogen-Ion Concentration, Transfection, methotrexate, Kinetics, Reduced Folate Carrier Protein, Young Adult, HEK293 Cells, Methotrexate, single nucleotide polymorphism, Folic Acid Antagonists, Humans, reduced folate carrier, amethopterin
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