ABCG2 p.Cys603Ser

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PMID: 16367905 [PubMed] Kage K et al: "Role of Cys-603 in dimer/oligomer formation of the breast cancer resistance protein BCRP/ABCG2."
No. Sentence Comment
5 However, under non-reducing conditions the BCRP-C603S mutant migrated both as a 70-kDa monomer and a 140-kDa dimer, whereas all other mutant BCRP migrated only as dimers.
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ABCG2 p.Cys603Ser 16367905:5:48
status: VERIFIED
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6 PA317 cells transfected with C603S-BCRP (PA/C603S) showed either similar or only marginally lower SN-38 resistance than PA/WT cells, despite the reduced levels of BCRP dimer in these cells.
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ABCG2 p.Cys603Ser 16367905:6:29
status: VERIFIED
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ABCG2 p.Cys603Ser 16367905:6:44
status: VERIFIED
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10 The results were equivalent to those from the PA/C603S cells, with some variations that again corresponded to the monomer levels.
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ABCG2 p.Cys603Ser 16367905:10:49
status: VERIFIED
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57 Under nonreducing conditions, however, the BCRP-C603S mutant was found to migrate as both a 70-kDa monomer and a 140-kDa dimer, whereas the BCRP-WT and each of the other mutant proteins migrated only as 140-kDa dimers (Fig. 2b).
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ABCG2 p.Cys603Ser 16367905:57:48
status: VERIFIED
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58 Also under reducing conditions, the BCRP protein levels in PA/ C43S, PA/C55S, PA/C284S and PA/C603S cells were slightly lower than the levels in the wild-type transfectants.
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ABCG2 p.Cys603Ser 16367905:58:94
status: VERIFIED
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63 Following this increased exposure time, these mutants could also be detected as both a 70-kDa monomer and a 140-kDa dimer, as is the case for BCRP-C603S, although their expression levels were less than 10% of wild-type.
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ABCG2 p.Cys603Ser 16367905:63:147
status: VERIFIED
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64 The ratio of monomer to dimer in these mutants was also far higher than PA/WT, as observed for PA/C603S.
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ABCG2 p.Cys603Ser 16367905:64:98
status: VERIFIED
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67 In contrast, the PA/C43S, PA/C55S, PA/C284S and PA/C603S mutants expressed intermediate amounts of BCRP and, in PA/C438S cells, little surface expression of BCRP was observed.
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ABCG2 p.Cys603Ser 16367905:67:51
status: VERIFIED
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71 Hence, the observed differences in BCRP expression, particularly in the PA/C438S, PA/C592S, PA/C603S and PA/C608S cells, are not attributable to low transcript levels.
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ABCG2 p.Cys603Ser 16367905:71:95
status: VERIFIED
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76 Protein expression and SN-38 sensitivity levels of PA317 cells transfected with mutant BCRP containing Cys-603 substitutions Because the monomeric form of BCRP was detectable in PA/ C603S cells under non-reducing conditions (Fig. 2b), we chose to further analyze this specific cysteine residue by generating additional amino acid substitutions at this position.
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ABCG2 p.Cys603Ser 16367905:76:182
status: VERIFIED
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77 The resulting PA/C603X mutants (X = D, H, R, S, Y, A and W) were also investigated by western blotting under the same conditions used for PA/C603S.
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ABCG2 p.Cys603Ser 16367905:77:141
status: VERIFIED
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89 intensities of the 70-kDa BCRP monomeric mutant bands were similar to wild-type with the exception of PA/C603S and PA/C603Y, which had somewhat lower expression levels (Fig. 6a).
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ABCG2 p.Cys603Ser 16367905:89:105
status: VERIFIED
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108 PA/C43S, PA/C55S, PA/C284S and PA/C603S transfectants acquired similar or somewhat lower degrees of SN-38 resistance than PA/WT cells.
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ABCG2 p.Cys603Ser 16367905:108:34
status: VERIFIED
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120 In contrast, considerable levels of the monomeric form of BCRP were observed for the PA/C603S mutant, which correspondingly showed decreased dimer levels (Fig. 2b).
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ABCG2 p.Cys603Ser 16367905:120:88
status: VERIFIED
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122 Under non-reducing conditions, small quantities of both monomeric and dimeric forms of BCRP could be observed for the PA/C438S, PA/C592S and PA/C608S transfectants as well as in PA/C603S cell extracts following overexposure of the blot (Fig. 2c).
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ABCG2 p.Cys603Ser 16367905:122:181
status: VERIFIED
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125 The intensity of the BCRP-C603S monomer band under non-reducing conditions was far stronger than the other mutants (Fig. 2b).
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ABCG2 p.Cys603Ser 16367905:125:26
status: VERIFIED
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131 The drug resistance levels induced by exogenous PA/ C603S were almost equivalent to PA/WT (Fig. 5b), although the intensity of the 140-kDa BCRP-C603S band under nonreducing conditions was far less than BCRP-WT (Fig. 2b).
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ABCG2 p.Cys603Ser 16367905:131:52
status: VERIFIED
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ABCG2 p.Cys603Ser 16367905:131:144
status: VERIFIED
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143 (c) SN-38 sensitivity of parental PA317, PA/WT, PA/C603D, PA/C603Y, PA/ C603S and PA/C603A.
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ABCG2 p.Cys603Ser 16367905:143:72
status: VERIFIED
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PMID: 18644784 [PubMed] Ozvegy-Laczka C et al: "Interaction with the 5D3 monoclonal antibody is regulated by intramolecular rearrangements but not by covalent dimer formation of the human ABCG2 multidrug transporter."
No. Sentence Comment
28 Interestingly, mutation of Cys-603 to Ala, Gly, or Ser does not remarkably influence the expression and functionality of the transporter (9-11).
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ABCG2 p.Cys603Ser 18644784:28:27
status: VERIFIED
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PMID: 20518788 [PubMed] Shigeta J et al: "BCRP/ABCG2 confers anticancer drug resistance without covalent dimerization."
No. Sentence Comment
1 The BCRP-C603S mutant substituting Ser for Cys-603 in the third extracellular domain formed both a 70-75-kDa monomer and 140-150-kDa dimer, suggesting that Cys-603 is an important residue in the covalent bridge.
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ABCG2 p.Cys603Ser 20518788:1:9
status: VERIFIED
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ABCG2 p.Cys603Ser 20518788:1:35
status: VERIFIED
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8 Among drug-resistant Cys-mutant BCRP transfectants, PA / C603S, PA / C592SÆC608S, and PA / C592SÆC603SÆC608S were found to be more resistant to the reversal effects of fumitremorgin C than PA / WT, suggesting some alteration in the substrate recognition in Cys-mutant BCRPs.
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ABCG2 p.Cys603Ser 20518788:8:57
status: VERIFIED
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21 Among these, BCRP-C603S mutant substituting Ser for Cys-603 was found to migrate both as a 70-75-kDa monomer and as a 140-150-kDa dimer in SDS-PAGE under non-reducing conditions.
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ABCG2 p.Cys603Ser 20518788:21:18
status: VERIFIED
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ABCG2 p.Cys603Ser 20518788:21:44
status: VERIFIED
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22 (16) The PA /C603S transfectant showed the drug resistance phenotype.
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ABCG2 p.Cys603Ser 20518788:22:13
status: VERIFIED
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25 However, the existence of a small amount of 150-kDa dimer in the PA/C603S transfectant suggested the involvement of other Cys residues in this process.
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ABCG2 p.Cys603Ser 20518788:25:68
status: VERIFIED
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29 In the present study, to elucidate the possible involvement of Cys-592 and Cys-608 in BCRP dimerization and protein activity, we established double (C592SÆC603S, C592SÆC608S, and C603SÆC608S) and triple (C592SÆC603SÆC608S) mutant BCRP transfectants, and compared the expression, dimer formation, and function of these BCRP mutants with wild-type and single (C592S, C603S, and C608S) mutant proteins.
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ABCG2 p.Cys603Ser 20518788:29:390
status: VERIFIED
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33 The wild-type and single (C592S, C603S, and C608S) mutant BCRP cDNAs in the same vector were also used as controls.
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ABCG2 p.Cys603Ser 20518788:33:33
status: VERIFIED
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63 PA317 cells were transfected with the wild-type, single (C592S, C603S, and C608S), double (C592SÆC603S, C592SÆC608S, and C603SÆC608S), and triple (C592SÆC603SÆC608S) mutant BCRP cDNAs in pHa-IRES-DHFR bicistronic expression vector as described previously.
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ABCG2 p.Cys603Ser 20518788:63:64
status: VERIFIED
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67 The resulting mixed populations of the drug-selected cells were designated as PA /WT-mix, PA / C592S-mix, PA /C603S-mix, PA /C608S-mix, PA /C592SÆC603S-mix, PA/ C592SÆC608S-mix, PA /C603SÆC608S-mix, and PA /C592SÆC603SÆC608S-mix.
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ABCG2 p.Cys603Ser 20518788:67:110
status: VERIFIED
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71 Wild-type BCRP and BCRP-C603S both migrated as a 75-kDa molecule.
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ABCG2 p.Cys603Ser 20518788:71:24
status: VERIFIED
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74 A high level of BCRP expression was observed in PA /WT-mix, PA /C603S-mix, and PA /C592SÆ C608S-mix cells (Fig. 2a).
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ABCG2 p.Cys603Ser 20518788:74:64
status: VERIFIED
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76 As reported previously, BCRP-C603S migrated as both a 150-kDa dimer and a 70-75-kDa monomer.
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ABCG2 p.Cys603Ser 20518788:76:29
status: VERIFIED
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82 The BCRP expression levels and monomer /dimer formation in PA/ WT and single mutant BCRP transfectants (PA /C592S, PA/C603S, and PA/C608S) were essentially the same as those in our previous report (Fig. 3a-d).
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ABCG2 p.Cys603Ser 20518788:82:118
status: VERIFIED
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94 PA /WT cells expressed 75-kDa BCRP only, and PA /C603S cells mostly expressed the 75-kDa molecule.
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ABCG2 p.Cys603Ser 20518788:94:49
status: VERIFIED
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97 +SH -SH PA/WT-mix PA/C592S-mix PA/C603S-mix PA/C608S-mix PA/C592S·C603S-mix PA/C592S·C608S-mix PA/C603S·C608S-mix PA/C592S·C603S·C608S-mix PA317 PA/WT-mix PA/WT-mix(0.5) PA/C592S-mix PA/C603S-mix PA/C608S-mix PA/C592S·C603S-mix PA/C592S·C608S-mix PA/C603S·C608S-mix PA/C592S·C603S·C608S-mix PA317 150 75 kDa 150 75 kDa GAPDH (b)(a) Fig. 2.
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ABCG2 p.Cys603Ser 20518788:97:34
status: VERIFIED
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ABCG2 p.Cys603Ser 20518788:97:211
status: VERIFIED
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102 -mix -cl.1 -cl.8 PA317 PA/WT PA/C592S PA/C603S PA/WT-mix -mix -cl.3 -cl.7 PA317 PA/WT-mix -mix -cl.5 -cl.7 PA317 PA/C608S PA/WT-mix -mix -cl.6 -cl.7 PA317 BCRP (-SH) 75 150 kDa GAPDH (+SH) BCRP (+SH) PA/WT-mix -mix -cl.1 -cl.4 PA317 PA/WT-mix -mix -cl.6 -cl.7 PA317 PA/WT-mix -mix -cl.6 -cl.7 PA317 PA/C592S ·C603S PA/C592S ·C608S PA/C603S ·C608S PA/C592S ·C603S·C608S PA/WT-mix -mix -cl.2 -cl.7 PA317 BCRP (-SH) 75 150 kDa GAPDH (+SH) BCRP (+SH) (a) (b) (c) (d) (e) (g)(f) (h) Fig. 3.
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ABCG2 p.Cys603Ser 20518788:102:41
status: VERIFIED
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ABCG2 p.Cys603Ser 20518788:102:344
status: VERIFIED
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105 (a) PA / WT cells; (b) PA / C592S cells; (c) PA / C603S cells; (d) PA / C608S cells; (e) PA / C592SÆC603S cells; (f) PA / C592SÆC608S cells; (g) PA / C603SÆC608S cells; (h) PA / C592SÆC603SÆ C608S cells.
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ABCG2 p.Cys603Ser 20518788:105:50
status: VERIFIED
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109 PA /WT, PA/C603S-cl.3, and PA /C603S-cl.7 transfectants showed high levels of resistance to SN-38.
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ABCG2 p.Cys603Ser 20518788:109:11
status: VERIFIED
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ABCG2 p.Cys603Ser 20518788:109:31
status: VERIFIED
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120 Based on the results of drug sensitivity assay, we selected PA /WT-mix, PA/C592S-cl.6, PA /C603S-cl.3, PA /C592SÆC608S-cl.7, and PA/C592SÆC603SÆC608S-cl.7 cells as representative drug-resistant transfectants for further study.
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ABCG2 p.Cys603Ser 20518788:120:91
status: VERIFIED
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122 As shown in Figure 7(a), intracellular mitoxantrone was at low levels in PA /WT-mix and PA /C603S-cl.3 cells and at intermediate levels in PA /C592S-cl.6, PA /C592SÆC608S-cl.7, and PA /C592SÆC603SÆC608S-cl.7 cells.
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ABCG2 p.Cys603Ser 20518788:122:92
status: VERIFIED
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134 Immunofluorescent microscopy analysis using an anti-BCRP antibody BXP-21 was performed to examine whether 250 200 70-kDa BCRP 75-kDa BCRP 100 150 0 50 NormalizedBCRPexpression(%ofPA/WT) PA317 -mix -cl.1 -cl.8 -mix -cl.6 -cl.7 -mix -cl.3 -cl.7 -mix -cl.5 -cl.7 -mix -cl.1 -cl.4 -mix -cl.2 -cl.7 -mix -cl.6 -cl.7 -mix -cl.6 -cl.7 PAC592S ·C603S PA/C592S ·C608S PA/C603S ·C608S PA/C592S ·C603S·C608S PA/WT PA/C592S PA/C603S PA/C608S Fig. 4.
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ABCG2 p.Cys603Ser 20518788:134:372
status: VERIFIED
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ABCG2 p.Cys603Ser 20518788:134:440
status: VERIFIED
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138 SN-38 resistance of mutant BCRP transfectants Cell line IC50 to SN-38† (nM) Degree of resistance‡ (x-fold) Relative expression level Total BCRP§ 75-kDa BCRP- PA317 3.7 ± 0.2 1 - - PA / WT-mix 90 ± 4.4 24 100 100 PA / WT-cl.1 172 ± 6.1 47 207 206 PA / WT-cl.8 77 ± 10.3 21 56 56 PA / C592S-mix 12.4 ± 0.8 3.4 34 24 PA / C592S-cl.6 28.5 ± 1.4 7.7 52 37 PA / C592S-cl.7 13.7 ± 0.5 3.7 16 11 PA / C603S-mix 9.7 ± 0.5 2.6 54 51 PA / C603S-cl.3 409 ± 15.9 110 146 132 PA / C603S-cl.7 158 ± 17.7 43 135 122 PA / C608S-mix 4.8 ± 0.3 1.3 27 3 PA / C608S-cl.5 5.6 ± 0.2 1.5 26 7 PA / C608S-cl.7 6.3 ± 0.6 1.7 43 12 PA / C592SÆC603S-mix 3.6 ± 0.2 1.0 27 10 PA / C592SÆC603S-cl.1 5.1 ± 1.1 1.4 27 10 PA / C592SÆC603S-cl.4 6.2 ± 0.8 1.7 43 26 PA / C592SÆC608S-mix 16.7 ± 1.8 4.6 92 67 PA / C592SÆC608S-cl.2 22.8 ± 2.0 6.2 163 111 PA / C592SÆC608S-cl.7 34.5 ± 4.9 9.4 151 106 PA / C603SÆC608S-mix 2.9 ± 0.2 0.8 21 3 PA / C603SÆC608S-cl.6 4.4 ± 0.4 1.2 57 3 PA / C603SÆC608S-cl.7 3.4 ± 0.1 0.9 51 4 PA / C592SÆC603SÆC608S-mix 4.1 ± 0.2 1.1 13 7 PA / C592SÆC603SÆC608S-cl.6 4.0 ± 0.4 1.1 25 13 PA / C592SÆC603SÆC608S-cl.7 11.1 ± 1.5 3.0 145 102 †The cells were incubated for 4 days at 37°C in the presence or absence of various concentrations of 7-ethyl-10-hydroxycamptothecin (SN-38).
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ABCG2 p.Cys603Ser 20518788:138:447
status: VERIFIED
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ABCG2 p.Cys603Ser 20518788:138:487
status: NEW
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ABCG2 p.Cys603Ser 20518788:138:531
status: NEW
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149 To examine the sensitivity of mutant BCRPs to a BCRP inhibitor, namely FTC, the reversal effect of FTC on the mutant BCRP transfectants was examined. PA /C603S-cl.7 was added to the panel of drug-resistant transfectants in this experiment.
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ABCG2 p.Cys603Ser 20518788:149:154
status: VERIFIED
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151 Fumitremorgin C (FTC) reversed the drug resistance of PA /C603S-cl.3 and PA /C603S-cl.7 cells, although these clones still showed 4-to 15-fold higher levels of resistance to SN-38 and mitoxantrone in the presence of FTC.
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ABCG2 p.Cys603Ser 20518788:151:58
status: VERIFIED
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ABCG2 p.Cys603Ser 20518788:151:77
status: VERIFIED
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162 Consistent with our previous study, PA/C603S cells expressed both monomeric and dimeric BCRP.
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ABCG2 p.Cys603Ser 20518788:162:39
status: VERIFIED
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170 Single mutation on Cys-603 loses this homo-dimerization site, and it can therefore be concluded that BCRP-C603S protein mainly existed as a monomer.
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ABCG2 p.Cys603Ser 20518788:170:106
status: VERIFIED
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171 The intramolecular disulfide bridge between Cys-592 and Cys-608 is partially disrupted for some reason, and small amount of the BCRP dimer could be detected in PA /C603S.
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ABCG2 p.Cys603Ser 20518788:171:164
status: VERIFIED
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172 Introduction of the C592S mutation into BCRP-C603S extinguishes the counter partner against Cys-608 in the intramolecular disulfide bridge.
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ABCG2 p.Cys603Ser 20518788:172:45
status: VERIFIED
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196 PA/C603S-cl.3 5.
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ABCG2 p.Cys603Ser 20518788:196:3
status: VERIFIED
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208 (1) PA317 cells; (2) PA / WT-mix cells; (3) PA / C592S-cl.6 cells; (4) PA / C603S-cl.3 cells; (5) PA / C592SÆC608S-cl.7 cells; (6) PA / C592SÆC603SÆC608S-cl.7 cells.
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ABCG2 p.Cys603Ser 20518788:208:76
status: VERIFIED
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226 PA/WT, PA /C592S, PA/C603S, PA /C592SÆC608S, and PA /C592SÆC603SÆC608S-cl.7 cells exhibited drug resistance and low accumulation of mitoxantrone.
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ABCG2 p.Cys603Ser 20518788:226:21
status: VERIFIED
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227 PA/WT and PA /C603S cells expressed a 75-kDa BCRP product (Fig. 2).
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ABCG2 p.Cys603Ser 20518788:227:14
status: VERIFIED
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234 Effect of FTC on the SN-38 and mitoxantrone resistance of mutant BCRP transfectants Cell line SN-38 Mitoxantrone Relative expression level of total BCRP§ Degree of resistance† RI‡ Degree of resistance† RI‡ )FTC +FTC )FTC + FTC PA317 1.0 ± 0.1 0.9 ± 0.1 - 1.0 ± 0.1 0.9 ± 0.1 - - PA / WT-mix 19.3 ± 1.7 1.4 ± 0.1 13.8 9.0 ± 0.3 1.2 ± 0.1 7.5 100 PA / C592S-cl.6 4.2 ± 0.3 1.2 ± 0.1 3.5 3.7 ± 0.1 1.3 ± 0.1 2.8 52 PA / C603S-cl.3 106 ± 7.3 7.9 ± 0.3 13.4 57 ± 5.9 15 ± 0.7 3.8 146 PA / C603S-cl.7 18 ± 2.0 4.1 ± 0.2 4.4 28 ± 3.9 12 ± 1.0 2.3 135 PA / C592SÆC608S-cl.7 8.4 ± 0.5 4.0 ± 0.2 2.1 3.3 ± 0.2 3.3 ± 0.1 1.0 151 PA / C592SÆC603SÆC608S-cl.7 4.1 ± 0.3 4.6 ± 0.3 0.9 7.5 ± 0.2 6.0 ± 0.8 1.3 145 †The cells were incubated for 4 days at 37°C in the presence or absence of various concentrations of anticancer agents in the presence or absence of 1 lM fumitremorgin C (FTC).
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ABCG2 p.Cys603Ser 20518788:234:510
status: VERIFIED
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ABCG2 p.Cys603Ser 20518788:234:597
status: NEW
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245 Fumitremorgin C (FTC) strongly reversed the resistance of PA /WT and PA /C592S cells to SN-38 and mitoxantrone, and partially reversed the drug resistance of PA /C603S cells.
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ABCG2 p.Cys603Ser 20518788:245:162
status: VERIFIED
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PMID: 20812902 [PubMed] Ni Z et al: "Structure and function of the human breast cancer resistance protein (BCRP/ABCG2)."
No. Sentence Comment
136 Importantly, Shigeta et al. showed that the triple-mutant C592S/C603S/C608S retained substantial resistance to mitoxantrone, topotecan, and SN-38 [86].
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ABCG2 p.Cys603Ser 20812902:136:64
status: VERIFIED
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300 The recent study by Shigeta et al. [86] also demonstrated that the triple-mutant C592S/C603S/C608S in PA317 cells retained substantial activity with some alteration in substrate recognition, although its level of expression was significantly decreased and its subcellular distribution was altered.
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ABCG2 p.Cys603Ser 20812902:300:87
status: VERIFIED
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PMID: 25036722 [PubMed] Szafraniec MJ et al: "Determinants of the activity and substrate recognition of breast cancer resistance protein (ABCG2)."
No. Sentence Comment
209 Position Type of mutation Effect on the transporter References NBD Lys 86 Met (i) No stimulation of the ATPase activity by prazosin; (ii) no influence on the transport of mitoxantrone Henriksen et al. (2005b) Glu 126 stop, Phe 208 Ser, Ser 248 Phe, Glu 334 stop Inability to transport hematoporphyrin Tamura et al. (2006) Glu 211 Gln Complete abolishment of the ATPase activity and methotrexate transport Hou et al. (2009) Pro 392 Ala Significant reduction in the efflux activity of mitoxantrone, BODIPY-prazosin and Hoechst 33342 Ni et al. (2011) TM1 Gly 406 Ala Gly 410 Ala No influence on the activity of the transporter Polgar et al. (2004) Gly 406 Leu Gly 410 Leu (i) Loss of the ability to transport rhodamine123; (ii) impaired transport of mitoxantrone, Pheide and BODIPY-prazosin Polgar et al. (2004) Extracellular loop 1 Phe 431 Leu (i) Loss of the ability to transport methotrexate; (ii) 10% level of hematoporphyrin transport compared to the WT protein Tamura et al. (2006) Ser 441 Asn Inability to transport hematoporphyrin Tamura et al. (2006) Ser 441 Asn Loss of the ability to transport methotrexate Tamura et al. (2006) TM2 Lys 452 Ala His 457 Ala Increase in transport of mitoxantrone, BODIPY-prazosin and Hoechst 33342 Cai et al. (2010) Lys 453 Ala Arg 465 Ala Decrease in transport of mitoxantrone, BODIPY-prazosin, Hoechst 33342, doxorubicin, SN-38 and rhodamine 123 Cai et al. (2010) TM3 Arg 482 Gly Arg 482 Thr (i) No change in the inhibitory activity of lapatinib; (ii) about two times greater inhibition by ritonavir, saquinavir and nalfinavir than in the WT variant; (iii) gaining the ability to transport rhodamine123 and doxorubicin; (iv) no influence on the transport of mitoxantrone; (v) loss of the ability to transport methotrexate Dai et al. (2008), Gupta et al. (2004), Honjo et al. (2001), Mitomo et al. (2003) Arg 482 Thr (i) Lower IC 50 of cyclosporine A for mutant than for WT variant; (ii) lower elacridar inhibition potency Xia et al. (2007) Arg 482 Lys Complete loss of transport activity Ejendal et al. (2006) Phe 489 Leu Impaired transport of porphyrins, no transport of methotrexate Tamura et al. (2006) Extracellular loop 3 Asn 590 Tyr Over twice reduced transport of mitoxantrone, topotecan, daunorubicin and rhodamine 123 Vethanayagam et al. (2005) Cys 592 Ala/Cys 608 Ala (i) Transport of mitoxantrone almost unchanged; (ii) transport of BODIPY-prazosin significantly impaired Henriksen et al. (2005a) Extracellular loop 3 Cys 603 Ser Cys 592 Ser/Cys 608 Ser Cys 592 Ser/Cys 603 Ser/Cys 608 Ser Diminished susceptibility to the inhibitory activity of fumitremorgin C Shigeta et al. (2010) Cys-less Arg 482 Gly-BCRP Complete loss of the ability to efflux mitoxantrone Liu et al. (2008b) The positions of the amino acid residues refer to the topological model of BCRP proposed by Wang et al. (2009).
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ABCG2 p.Cys603Ser 25036722:209:2470
status: NEW
X
ABCG2 p.Cys603Ser 25036722:209:2518
status: NEW
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230 Cys592 Ser/Cys603 Ser-BCRP and Cys592 Ser/Cys608 Ser-BCRP were detected as dimers, while Cys603 Ser/Cys608 Ser-BCRP and Cys592 Ser/Cys603 Ser/Cys608 Ser-BCRP as monomers, suggesting that no other Cys are involved in dimerization.
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ABCG2 p.Cys603Ser 25036722:230:11
status: NEW
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ABCG2 p.Cys603Ser 25036722:230:89
status: NEW
X
ABCG2 p.Cys603Ser 25036722:230:131
status: NEW
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231 At the same time, cells transfected with a triple mutant, Cys592 Ser/Cys603 Ser/Cys608 Ser-BCRP, showed significant drug resistance and a low accumulation of mitoxantrone which indicated that dimer formation might not be required for BCRP functioning as a transporter.
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ABCG2 p.Cys603Ser 25036722:231:69
status: NEW
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