52 Mutagenesis was performed according to the manufacturer`s instructions with the following sense primers (the substituted nucleotides causing the mutation are underlined; silent nucleotide substitutions added to introduce or disrupt a restriction site are in bold; other nucleotide substitutions are in lowercase typeface; and diagnostic restriction enzymes are indicated in parentheses): MRP1-Pro1150Gly (50 -G TCG GTC AGC CGG TCg GGG GTC TAT TCC C-30 ) (BsrFI), MRP1-Pro1150Ile (50 -C AGC CGC TCC ATC GTC TAC TCC CAT TTC AAC-30 ) (AccI), MRP1- Pro1150Leu (50 -CG GTC AGC CGG TCC CTC GTC TAC TCC CAT TTC-30 ) (AccI) and MRP1-Pro1150Val (50 -CG GTC AGC CGG TCC GTG GTC TAT TCC C-30 ) (RsrII).

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ABCC1 p.Pro1150Val 18336795:52:625

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109 Levels of [3 H]LTC4 labeling of the Pro1150Gly, Pro1150Ile, Pro1150Leu and Pro1150Val mutants were also comparable to wild-type MRP1 (Fig. 3A).

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ABCC1 p.Pro1150Val 18336795:109:75

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147 Under these conditions, the Pro1150Gly, Pro1150Ile and Pro1150Leu mutants exhibited similar levels of [a32 P]8N3ADP trapping (50-70% reduction) (Fig. 5B), while trapping by the Pro1150Val mutant was only slightly reduced (20%) relative to wild-type MRP1 (Fig. 5B).

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ABCC1 p.Pro1150Val 18336795:147:177

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221 Although none of the amino acids could replace Pro1150 with respect to the substrate specificity of MRP1, it is interesting that MRP1-Pro1150Val exhibited a substantially smaller decrease in vanadate-induced [a32 P]8N3ADP trapping than the other mutants.

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ABCC1 p.Pro1150Val 18336795:221:134

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758 The Pro1150Gly, Pro1150Ile, Pro1150Leu and Pro1150Val mutants exhibited a phenotype similar to the Pro1150Ala mutant with respect to organic anion transport and [ 32 P]8N3ATP photolabeling [347].

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ABCC1 p.Pro1150Val 21143116:758:43

status: NEW

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