ABCB11 p.Asn591Ser
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PMID: 15077010
[PubMed]
Pauli-Magnus C et al: "Sequence analysis of bile salt export pump (ABCB11) and multidrug resistance p-glycoprotein 3 (ABCB4, MDR3) in patients with intrahepatic cholestasis of pregnancy."
No.
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Comment
8
Three nonsynonymous sites in codons for evolutionarily conserved amino acids were specific for the ICP collective (BSEP, N591S; MDR3, S320F and G762E).
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ABCB11 p.Asn591Ser 15077010:8:121
status: NEW95 Non-synonymous changes observed as singletons or doubletons in our sample set coded for the amino acid changes R415Q and N591S.
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ABCB11 p.Asn591Ser 15077010:95:121
status: NEW96 Alignment of all mammalian BSEP sequences indicated that three of the four non-synonymous coding variants were in codons for evolutionarily conserved amino acids (R415Q, V444A and N591S) (Table 1).
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ABCB11 p.Asn591Ser 15077010:96:180
status: NEW136 1 , 1 Splicing 2 , 1 N591S 3 NA 4 3.7 Splicing 5 NA 6 9.0 7 , 1 8 , 1 9 , 1 10 1.7 G762E 11 , 1 12 2.6 13 2.8 14 4.5 15 2.9 Splicing 16 , 1 17 4.2 18 2.5 Splicing 19 2.3 20 1.4 S320F 21 , 1 ICP-specific variants are indicated with their respective variant number (Tables 1 and 2).
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ABCB11 p.Asn591Ser 15077010:136:21
status: NEW
PMID: 17181454
[PubMed]
Sakurai A et al: "Prediction of drug-induced intrahepatic cholestasis: in vitro screening and QSAR analysis of drugs inhibiting the human bile salt export pump."
No.
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Comment
120
H2N COOH S56L G238V G260D C336S L339V V444A K461E D482G T923P K930X G982R R1090X R1153C Outside Inside R1268Q A1228VE1186K R1128H R1057X R1050C A926P A865V R698H E636G M677V S593R E592Q N591S R575XA570T Q558H I498T R432T R415Q R299K E297G V284A I206V S194P E186G cholestasis Expert Opin. Drug Saf. (2007) 6(1) Table 1.
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ABCB11 p.Asn591Ser 17181454:120:186
status: NEW123 [40] rs1156869 14 1674 G→C Gln558His - [102] - 14 1708 G→A Ala570Thr BRIC2 [45] - 14 1723 C→T Arg575X PFIC2 [35,46,47] rs11568367 15 1772 A→G Asn591Ser ICP [39,102] rs11568370 15 1774 G→C Glu592Gln - [102] - 15 1779 T→A/G Ser593Arg PFIC2?
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ABCB11 p.Asn591Ser 17181454:123:170
status: NEW
PMID: 17855769
[PubMed]
Lam P et al: "Levels of plasma membrane expression in progressive and benign mutations of the bile salt export pump (Bsep/Abcb11) correlate with severity of cholestatic diseases."
No.
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Comment
9
Therefore we compared the effect of two PFIC2 mutations (D482G, E297G) with two BRIC2 mutations (A570T and R1050C) and one ICP mutation (N591S) with regard to the subcellular localization, maturation, and function of the rat Bsep protein.
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ABCB11 p.Asn591Ser 17855769:9:137
status: NEW11 Mutant proteins were expressed at reduced levels on the plasma membrane of transfected HEK293 cells compared with wild-type (WT) Bsep in the following order: WT Ͼ N591S Ͼ R1050C ϳ A570T ϳ E297G ϾϾ D482G.
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ABCB11 p.Asn591Ser 17855769:11:169
status: NEW45 All point mutations (D482G, E297G, A570T, R1050C, N591S) were introduced with the QuickChange Site-Directed Mutagenesis Kit (Stratagene, La Jolla, CA).
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ABCB11 p.Asn591Ser 17855769:45:50
status: NEW64 PFIC2 (D482G, E297G), BRIC2 (A570T, R1050C), and ICP (N591S) mutations that are investigated in this study are indicated in italics.
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ABCB11 p.Asn591Ser 17855769:64:54
status: NEW94 Sf9 cells infected with recombinant virus (mock, WT, D482G, E297G, A570T, R1050C, and N591S) were harvested, and cell membranes were prepared as described previously (23).
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ABCB11 p.Asn591Ser 17855769:94:86
status: NEW107 The subcellular distributions of D482G, E297G, A570T, R1050C, and N591S were examined first because intracellular accumulation of misfolded proteins has been shown for many diseases.
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ABCB11 p.Asn591Ser 17855769:107:66
status: NEW118 The level of cell surface expression of Bsep protein was quantitated by densitometry and determined to be in the following order: WT (100%) Ͼ N591S (75.6 Ϯ 15.6%) Ͼ E297G (38.5 Ϯ 12.6%) ϳ R1050C (35.6 Ϯ 14.5%) ϳ A570T (29.5 Ϯ 8.8%) ϾϾ D482G (5.7 Ϯ 2.3%).
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ABCB11 p.Asn591Ser 17855769:118:148
status: NEW120 The total expression (cell surface and intracellular proteins) also showed changes similar to those in cell surface expression: WT (100%) Ͼ N591S (73.5 Ϯ 4.3%) Ͼ E297G (33.7 Ϯ 20.4%) ϳ R1050C (26.7 Ϯ 16.0%) ϳ A570T (11.9 Ϯ 5.2%) ϾϾ D482G (2.5 Ϯ 2.0%) (Fig. 4B).
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ABCB11 p.Asn591Ser 17855769:120:146
status: NEW146 Membrane vesicles containing WT Bsep (17.1 Ϯ 2.5 nmol Pi ⅐min-1 ⅐mg protein-1 ) and mutant N591S Bsep (18.4 Ϯ 1.53 nmol Pi ⅐min-1 ⅐mg protein-1 ) showed slightly higher basal ATPase activity than membrane vesicles containing the mock-transfected control (12.3 Ϯ 0.67 nmol Pi ⅐min-1 ⅐mg protein-1 ) (Fig. 7B).
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ABCB11 p.Asn591Ser 17855769:146:111
status: NEW150 The membrane vesicles expressing D482G, A570T, R1050C, or N591S showed similar levels of taurocholate uptake compared with WT Bsep.
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ABCB11 p.Asn591Ser 17855769:150:58
status: NEW155 Cells were transiently transfected with pEGFPN1 (control), rat Bsep-GFP [wild type (WT)], D482G-GFP, E297G-GFP, A570T-GFP, R1050C-GFP, and N591S-GFP constructs.
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ABCB11 p.Asn591Ser 17855769:155:139
status: NEW157 In contrast, 4 of the mutant GFP-tagged Bsep proteins are variably localized to both intracellular and apical membranes, whereas localization of N591S-GFP is similar to WT.
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ABCB11 p.Asn591Ser 17855769:157:145
status: NEW165 In contrast, the surface expression of the ICP variant N591S is close to the level of the WT protein (ϳ70%).
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ABCB11 p.Asn591Ser 17855769:165:55
status: NEW169 Cells were transfected with rat Bsep-GFP (WT), D482G-GFP, E297G-GFP, A570T-GFP, R1050C-GFP, and N591S-GFP constructs and were examined for GFP by confocal laser microscopy.
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ABCB11 p.Asn591Ser 17855769:169:96
status: NEW172 N591S was mainly expressed on the membrane surface, a pattern similar to the WT protein.
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ABCB11 p.Asn591Ser 17855769:172:0
status: NEW176 D4, D482G; E2, E297G; A5, A570T; R10, R1050C; N5, N591S.
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ABCB11 p.Asn591Ser 17855769:176:50
status: NEW183 P Ͻ 0.05, D482G, E297G, A570T, R1050C, and N591S compared with WT control.
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ABCB11 p.Asn591Ser 17855769:183:49
status: NEW229 A: immunoblot of the isolated Sf9 cell membrane proteins with anti-Bsep polyclonal antibody: GFP control expressed in HEK293 cells, WT expressed in HEK293 cells, rat liver homogenate (L), pFastBac1-Gus control (C), wild type (WT), D482G (D4), E297G (E2), A570T (A5), R1050C (R10), N591S (N5).
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ABCB11 p.Asn591Ser 17855769:229:281
status: NEW231 B: TCA (200 M) stimulates and orthovanadate inhibits ATPase activity in membrane vesicles containing comparable levels of WT or D482G, E297G, A570T, R1050C, and N591S mutant Bsep.
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ABCB11 p.Asn591Ser 17855769:231:169
status: NEW
PMID: 18987030
[PubMed]
Dixon PH et al: "Contribution of variant alleles of ABCB11 to susceptibility to intrahepatic cholestasis of pregnancy."
No.
Sentence
Comment
2
Methods: ABCB11 variation in ICP was investigated by screening for five mutant alleles (E297G, D482G, N591S, D676Y and G855R) and the V444A polymorphism (c.1331T.C, rs2287622) in two ICP cohorts (n = 333 UK, n = 158 continental Europe), and controls (n = 261) for V444A.
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ABCB11 p.Asn591Ser 18987030:2:102
status: NEW6 N591S was present in two patients; D676Y and G855R were not observed.
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ABCB11 p.Asn591Ser 18987030:6:0
status: NEW10 The molecular basis of V444A and N591S was not apparent from the Sav1866 structure.
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ABCB11 p.Asn591Ser 18987030:10:33
status: NEW12 N591S is a recurrent mutation; however, the mechanism may be independent of protein stability or function.
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ABCB11 p.Asn591Ser 18987030:12:0
status: NEW19 This was initially proposed in the Finnish population following analysis of a two SNP (single nucleotide polymorphism) haplotype in 57 cases.30 However, a subsequent study in a larger cohort of 142 ICP cases failed to replicate the initial findings, leaving the role of BSEP open to question.31 A recent study of the entire coding region of the BSEP gene identified a single potential mutation (N591S) in a cohort of 21 women with ICP.32 In addition, a polymorphism (c.1331C.T, V444A, rs2287622) possibly affecting BSEP expression has been suggested to play a role in ICP32 33 and has recently been reported to be associated with drug-induced cholestasis (DIC).34 This association has been replicated recently in a slightly larger cohort.24 We sought to clarify the role of ABCB11 mutations in predisposition to ICP by screening a large cohort of patients for the two common mutant alleles, together with the N591S mutation found previously in a case of ICP32 and the two recently described mutations (D676Y and G855R) associated with DIC.34 We also genotyped the V444A polymorphism in the largest case/control study to date in ICP.
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ABCB11 p.Asn591Ser 18987030:19:395
status: NEWX
ABCB11 p.Asn591Ser 18987030:19:910
status: NEW21 BSEP is homologous with the bacterial multidrug resistance protein (Sav1866) for which two structures have recently been determined at high resolution by x ray crystallography.35 36 We therefore used this structure to consider the possible effects of E297G, D482G, N591S and V444A on BSEP, all of which were identified in patients with ICP, to provide insights into potential mutational mechanisms.
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ABCB11 p.Asn591Ser 18987030:21:265
status: NEW48 RESULTS Sequencing DNA sequence was generated for the UK ICP cohort (333 patients) for exons 9 and 14 which contain the common European mutations E297G and D482G, together with exons 15, 17 and 21 containing the previously described ICP-linked mutation (N591S) and the two DIC-linked mutations (D676Y and G855R), respectively.
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ABCB11 p.Asn591Ser 18987030:48:254
status: NEW54 In this cohort, a single occurrence each of E297G and D482G was identified together with two occurrences of N591S.
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ABCB11 p.Asn591Ser 18987030:54:108
status: NEW77 S363 occupies the position of V444 in Sav1866. S363 hydrogen-bonds with D341 in an adjacent antiparallel b-strand within the Sav1866 NBD (fig 2C), but as it is only one of many bonds between the Table 1 Clinical features of ICP patients with heterozygous ABCB11 mutations Patient No Cohort Biochemistry (highest level measured) Other maternal clinical findings Fetal and labour complications Family history of ICPBile acids* ALT* GGT* E297G 1 UK 32 133 27 - - Yes 2{ UK 41 166 16 - M, H No 3{ UK 118 229 NP G, C Pr No 4 CE 41 82 NP - - No D482G 5 CE 74 98 15 J, P, BR - No N591S 6 CE 270 195 29 - - - 7 CE 32 60 11 - - - *Normal ranges: bile acids, ,14 mmol/l; alanine aminotransferase (ALT), (31 IU/l; c-glutamyl transferase (GGT), ,30 IU/l; bilirubin (BR), ,17 mmol/l.
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ABCB11 p.Asn591Ser 18987030:77:573
status: NEW84 Likewise, the functional or structural significance of the N591S variant of BSEP is not apparent from the crystal structure of Sav1866 (fig 2D).
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ABCB11 p.Asn591Ser 18987030:84:59
status: NEW88 Indeed, in the sequence of MJ0796 from Methanococcus jannaschii this position is occupied by a serine, suggesting that the serine side chain is likely to be tolerated as a replacement for N591 in BSEP.38 DISCUSSION We report here the identification of seven heterozygous carriers of BSEP (ABCB11) mutations (four E297G, one D482G and two N591S) in a large cohort of patients with ICP.
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ABCB11 p.Asn591Ser 18987030:88:338
status: NEW118 The N591S mutation has been previously described in a case of ICP in a screen of 21 cases.32 This residue is not highly conserved across ABC transporter NBDs, suggesting that folding and/or function may not be affected by this change.
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ABCB11 p.Asn591Ser 18987030:118:4
status: NEW123 Examination of clinical information for the E297G and N591S carriers failed to identify any factor to distinguish them from the general ICP population.
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ABCB11 p.Asn591Ser 18987030:123:54
status: NEW
PMID: 19101985
[PubMed]
Byrne JA et al: "Missense mutations and single nucleotide polymorphisms in ABCB11 impair bile salt export pump processing and function or disrupt pre-messenger RNA splicing."
No.
Sentence
Comment
68
Continued Exon Nucleotide Change Predicted Protein Effect Location in Protein Associated Phenotype Prevalence or frequency* Any Defect(s) Identified Reference BRIC, 1 family (both hom) 15 c.1757CϾT T586I Adj WB BRIC 1 family (het) No splicing † 15 c.1763CϾT A588V Adj WB PFIC 2 families (both het) No protein 31, 32 15 c.1772AϾG N591S Adj WB SNP-ICP 2.6% 42 15 c.1779TϾA S593R NBF1 PFIC 1 family (het) 29 15 c.1791GϾT V597V NBF1 SNP 2.6% 42 16 c.1880TϾC I627T IC3 PFIC 1 family (het) ‡ 16 c.1964CϾT T655I IC3 BRIC / ICP / DC 1 family (het) Reduced levels of mature protein ‡ 17 c.2029AϾG M677V IC3 SNP 1.6-5.6% 39, 42-45 18 c.2093GϾA R698H IC3 SNP 0.3 - 0.8% 43, 45 18 c.2125GϾA E709K IC3 SNP-PFIC 1 family (het) ‡ 18 c.2130TϾC P710P IC3 SNP-PBC 0.5 - 3.1% 43 20-21 c.2412AϾC A804A TM8 SNP 1.1% 45 20-21 c.2453AϾT Y818F IC4 SNP-PFIC 2 families (hom) Reduced levels of mature protein ‡ 20-21 c.2494CϾT R832C IC4 PFIC 2 families (1 het, 1 consanguineous) Moderate differential splicing 31, 32 20-21 c.2576CϾG T859R IC4 PFIC 1 family (het) 31 22 c.2767AϾC T923P IC5 BRIC 1 family (het) 8 22 c.2776GϾC A926P IC5 BRIC 1 family (het) Mild exon skipping 8 23 c.2842CϾT R948C IC5 PFIC 2 families (both het) Immature protein 31 23 c.2935AϾG N979D TM11 PFIC 1 family (consanguineous) 31 23 c.2944GϾA G982R TM11 PFIC 4 families (1 hom, 1 consanguineous, 2 het) Immature protein 7, 29, 31 23 c.3011GϾA G1004D EC6 PFIC 1 family (hom) 28 24 c.3084AϾG A1028A TM12 SNP-PBC 39.86 - 56.3% Severe exon skipping 8, 43, 45 24 c.3148CϾT R1050C C term BRIC 2 familes (1 hom, 1 het) Immature protein 8 25 c.3329CϾA A1110E Adj WA PFIC 2 familes (both het) Mild exon skipping; immature protein 31 25 c.3346GϾC G1116R WA PFIC / BRIC 1 family (consanguineous) Mild exon skipping ‡ 25 c.3382CϾT R1128C NBF2 PFIC 1 family (consanguineous) Mild exon skipping; immature protein 31 25 c.3383GϾA R1128H NBF2 BRIC 1 family (hom) Mild exon skipping; greatly reduced levels of mature protein 8 26 c.3432CϾA S1144R NBF2 PFIC 1 family (het) Severe differential splicing 29 26 c.3457CϾT R1153C NBF2 PFIC 4 families (2 consanguineous, 2 het) Immature protein 7, 31, 36 26 c.3458GϾA R1153H NBF2 PFIC 4 families (2 consanguineous, 2 het) Severe differential splicing; immature protein 31 26 c.3460TϾC S1154P NBF2 PFIC 1 family (het) Severe differential splicing 31 26 c.3556GϾA E1186K NBF2 SNP 1%-10% Mild exon skipping ‡ 26 c.3589_3590 delCTinsGG L1197G NBF2 BRIC 1 family (het) † 27 c.3628AϾC T1210P Adj ABCm PFIC 1 family (hom) Immature protein 31 27 c.3631AϾG N1211D Adj ABCm SNP-PFIC 1 family (het) ‡ 27 c.3669GϾC E1223D ABCm Prolonged NNH 1 family (het) ‡ 27 c.3683CϾT A1228V Adj ABCm/WB SNP-PBC 0.8% 43 27 c.3691CϾT R1231W Adj ABCm/WB PFIC 1 family (het) Severe exon skipping; immature protein 30, 31 27 c.3692GϾA R1231Q Adj ABCm/WB PFIC 2 families (1 consanguineous, 1 het) No splicing; immature protein 31, 34 27 c.3724CϾA L1242I WB PFIC 1 family (het) 31 28 c.3892GϾA R1268Q¶ NBF2 PFIC 1 family (hom) Immature protein 7 *Prevalence or frequency is quoted depending on how data were presented in the original publication(s).
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ABCB11 p.Asn591Ser 19101985:68:354
status: NEW140 Variant BSEP forms found in this study to have the same molecular weight and about the same abundance as the wild-type protein are I498T (c.1493TϾC; Fig. 5A), N1211D (c.3631AϾG), L1242I (c.3724CϾA), E709K (c.2125GϾA; Fig. 5C), , T586I (c.1757CϾT; Fig. 5E), as well as the SNP N591S (c.1772AϾG; Fig. 5F).
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ABCB11 p.Asn591Ser 19101985:140:306
status: NEW
PMID: 20010382
[PubMed]
Ho RH et al: "Polymorphic variants in the human bile salt export pump (BSEP; ABCB11): functional characterization and interindividual variability."
No.
Sentence
Comment
144
In addition, several rare BSEP polymorphisms, including 616A > G (Ile206Val), 1674G > C (Gln558His), 1772A > G (Asn591Ser), and 3556G > A (Glu1186Lys) were also associated with significantly impaired taurocholate transport compared with wild-type BSEP, exhibited by retained increased intracellular taurocholate accumulation (P < 0.05).
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ABCB11 p.Asn591Ser 20010382:144:112
status: NEW156 Calnexin, an intracellular resident Table 1 Single-nucleotide polymorphisms in ABCB11 Allele frequencies (%) SNP rs number Amino acid change African-American European-American Asian-American Mexican-American Pacific Islanders 108T > C rs3815675 Synonymous 1.5 1.5 25 5.0 21.4 167C > T rs11568361 Ser56Leu 0.5 0 0 0 0 174C > T rs11568362 Synonymous 0.5 0 0 0 0 270T > C rs414877 Synonymous 3.0 3.5 5.0 0 7.1 402C > T rs11568377 Synonymous 3.5 0 0 0 0 585G > C rs11568365 Synonymous 0.5 0 0 0 0 616A > G rs11568357 Ile206Val 2.5 0 0 0 0 696G > T rs11568358 Synonymous 0 0.5 0 0 0 807T > C rs2287616 Synonymous 2.0 0.5 23.3 5.0 21.4 890A > G rs11568372 Glu297Gly 0 0.5 0 0 0 957A > G rs7563233 Synonymous 31.5 0.5 0 15.0 0 1281C > T rs11568360 Synonymous 0.5 0 0 0 0 1331T > C rs2287622 Val444Ala 53.0 57.1 66.7 50.0 92.9 1671C > T rs11568368 Synonymous 0 0.5 0 0 0 1674G > C rs11568369 Gln558His 0 0.5 0 0 0 1772A > G rs11568367 Asn591Ser 0 0.5 0 0 0 1774G > C rs11568370 Glu592Gln 0 0.5 0 0 0 1791G > T rs11568371 Synonymous 0 0.5 0 0 0 2029A > G rs11568364 Met677Val 15.0 5.5 1.7 5.0 0 2412A > G rs11568373 Synonymous 8.0 0 0 5.0 0 3084A > G rs97692 Synonymous 28.6 54.6 63.3 37.5 21.4 3258A > G rs11568359 Synonymous 7.0 0 0 0 0 3435A > G rs11568366 Synonymous 1.0 0 0 0 0 3556G > A rs1521808 Glu1186Lys 2.5 0 0 0 0 Allele frequencies for single-nucleotide polymorphisms (SNPs) in ABCB11 were determined from a DNA panel of ethnically defined healthy individuals - African-Americans (n = 100), European-Americans (n = 100), Asian-Americans (n = 30), Mexican-Americans (n = 10) and Pacific Islanders (n = 7).
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ABCB11 p.Asn591Ser 20010382:156:927
status: NEW
PMID: 20232290
[PubMed]
Davit-Spraul A et al: "ATP8B1 and ABCB11 analysis in 62 children with normal gamma-glutamyl transferase progressive familial intrahepatic cholestasis (PFIC): phenotypic differences between PFIC1 and PFIC2 and natural history."
No.
Sentence
Comment
104
14b† p.I420T p.I1061VfsX34 na na PFIC2 no. 15*,‡ p.A167T p.G1058HfsX38 0.5 BSEP À PFIC2 no. 16* p.R1231W p.I528X na na PFIC2 no. 17 p.M62K p.I112T þ p.R698H 0.10 BSEP À PFIC2 no. 18* p.E297G p.H484RfsX5 0.16 BSEP À PFIC2 no. 19* p.E297G p.I610GfsX45 0.23 BSEP À PFIC2 no.
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ABCB11 p.Asn591Ser 20232290:104:118
status: NEW107 24† p.R1153C c.3213 14 A>G 0.13 BSEP À PFIC2 no. 25* p.G982R p.Q101DfsX8 0.10 BSEP À PFIC2 no. 26* p.N591S þ p.V597V nf 0.39 BSEP À PFIC2 no. 27* p.G982R p.R1001R na BSEP À PFIC2 no. 28 p.L232CfsX9 nf na BSEP À PFIC2 no. 29 p.W114R nf 0.50 BSEP À PFIC2 no.
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ABCB11 p.Asn591Ser 20232290:107:118
status: NEW
PMID: 20422495
[PubMed]
Lam P et al: "The bile salt export pump: clinical and experimental aspects of genetic and acquired cholestatic liver disease."
No.
Sentence
Comment
49
Similar to the results of immunofluorescence studies in liver tissue from PFIC2 patients,47 when PFIC2 human mutations were expressed in model mammalian cell lines (MDCK, HEK293, HepG2), the proteins failed to reach or be maintained at the cell surface.54-57 When BSEP mutations that cause PFIC2 (D482G, E297G), BRIC2 (A590T, R1050C), and ICP (N591S) were compared, the clinical severity of these mutations tended to correlate inversely with the amount of protein expressed on the cell surface.
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ABCB11 p.Asn591Ser 20422495:49:344
status: NEW
PMID: 20422497
[PubMed]
Pauli-Magnus C et al: "Genetic determinants of drug-induced cholestasis and intrahepatic cholestasis of pregnancy."
No.
Sentence
Comment
79
In the same study, heterozygosity for the BSEP mutations p.E297G, p.D482G, and p.N591S formerly associated with benign and progressive forms of familial intrahepatic cholestasis type 2 were found in four, one, and two ICP patients, respectively, allowing the extrapolation that 1% of European ICP cases are caused by these mutations.105 Although the molecular and mechanistic basis for p.V444A and p.N591S were not apparent, in silico structural and functional analysis suggests that p.E297G and p.D482G destabilizes the protein fold of BSEP, leading to decreased taurocholate transport in case of p.E297G.105,106 In addition, decreased hepatic BSEP expression,107,108 and very recently, significantly reduced hepatic mRNA levels109 was reported in healthy human liver tissue carrying the alanine allele in position 444 of BSEP, which could predispose to the development of ICP by way of decreased canalicular availability of BSEP.
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ABCB11 p.Asn591Ser 20422497:79:81
status: NEWX
ABCB11 p.Asn591Ser 20422497:79:400
status: NEW
PMID: 21103971
[PubMed]
Stieger B et al: "The role of the sodium-taurocholate cotransporting polypeptide (NTCP) and of the bile salt export pump (BSEP) in physiology and pathophysiology of bile formation."
No.
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Comment
432
Some patients with cholestasis of pregnancy were found to have a novel mutation in the BSEP gene, leading to a p.N591S variant (Dixon et al. 2009; Pauli-Magnus et al. 2004b).
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ABCB11 p.Asn591Ser 21103971:432:113
status: NEW
PMID: 16890614
[PubMed]
Keitel V et al: "Combined mutations of canalicular transporter proteins cause severe intrahepatic cholestasis of pregnancy."
No.
Sentence
Comment
58
Two ICP-specific nonsynonymous SNPs were detected in the MDR3 gene (S320F and G762E).6 In the BSEP gene, one ICP-specific SNP was found (N591S).6 Another nucleotide exchange from T to C at position Figure 2.
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ABCB11 p.Asn591Ser 16890614:58:137
status: NEW
PMID: 20799350
[PubMed]
Kelly L et al: "Functional hot spots in human ATP-binding cassette transporter nucleotide binding domains."
No.
Sentence
Comment
72
Predictions of the Functional Effects of 40 nsSNPs in ABC Transporters Comon name HUGO name Mutation NBD Prediction BSEP ABCB11 E592Q NBD1 Neutral BSEP ABCB11 N591S NBD1 Neutral BSEP ABCB11 Q558H NBD1 Neutral BSEP ABCB11 V444A NBD1 Neutral BSEP ABCB11 E1186K NBD2 Disease MDR1 ABCB1 P1051A NBD2 Neutral MDR1 ABCB1 S1141T NBD2 Neutral MDR1 ABCB1 T1256K NBD2 Disease MDR1 ABCB1 V1251I NBD2 Neutral MDR1 ABCB1 W1108R NBD2 Disease MRP2 ABCC2 I670T NBD1 Disease MRP2 ABCC2 L849R NBD1 Disease MRP2 ABCC2 C1515Y NBD2 Disease MRP3 ABCC3 D770N NBD1 Neutral MRP3 ABCC3 K718M NBD1 Neutral MRP3 ABCC3 T809M NBD1 Disease MRP3 ABCC3 V765L NBD1 Disease MRP3 ABCC3 Q1365R NBD2 Disease MRP3 ABCC3 R1297H NBD2 Disease MRP3 ABCC3 R1348C NBD2 Disease MRP3 ABCC3 R1381S NBD2 Disease MRP4 ABCC4 G487E NBD1 Disease MRP4 ABCC4 K498E NBD1 Neutral MRP4 ABCC4 R1220Q NBD2 Neutral MRP4 ABCC4 T1142M NBD2 Neutral MRP4 ABCC4 V1071I NBD2 Neutral MRP6 ABCC6 I1330L NBD1 Neutral MRP6 ABCC6 I742V NBD1 Neutral MRP6 ABCC6 P664S NBD1 Neutral MRP6 ABCC6 R724K NBD1 Neutral MRP6 ABCC6 R769K NBD1 Neutral MRP6 ABCC6 A1291T NBD2 Neutral MRP6 ABCC6 E1369K NBD2 Neutral MRP6 ABCC6 G1327E NBD2 Disease MRP6 ABCC6 L1416R NBD2 Disease MRP6 ABCC6 R1268Q NBD2 Disease MRP6 ABCC6 R1461H NBD2 Disease MXR ABCG2 I206L NBD1 Neutral MXR ABCG2 P269S NBD1 Disease MXR ABCG2 Q141K NBD1 Neutral nsSNPs.
X
ABCB11 p.Asn591Ser 20799350:72:159
status: NEW
PMID: 22089923
[PubMed]
Chong CP et al: "Bile acid-CoA ligase deficiency--a new inborn error of bile acid metabolism."
No.
Sentence
Comment
8
She also was homozygous for the missense mutation c.1772A>G in ABCB11, predicted to alter a highly conserved amino-acid residue (p.N591S) in bile salt export pump (BSEP).
X
ABCB11 p.Asn591Ser 22089923:8:131
status: NEW103 She was, however, homozygous for the sequence change c.1772A>G (p.N591S) in ABCB11. This has been described in the heterozygous state in one patient with intrahepatic cholestasis of pregnancy and is assessed as probably pathogenic (Pauli-Magnus et al. 2004).
X
ABCB11 p.Asn591Ser 22089923:103:66
status: NEW107 The sister proved homozygous for the c.1012>T (p.H338Y) mutation in SLC27A5 and heterozygous for the c.1772A>G (p.N591S) sequence change in ABCB11.
X
ABCB11 p.Asn591Ser 22089923:107:114
status: NEW
No.
Sentence
Comment
185
PFIC BRIC/NFC ICP Other liver diseases Genetic variants without disease association Missense mutations M1V C336S D549V L1055P E135K E137K T87R V43I S701P G19R W342G G556R C1083Y E137K L198P M123T S56L L712L L50S A382G G562D A1110E E186G E297G S194P Q121K A865D M62K R387H A570T S1114R L198P R415Q L198P R128H A865G C68Y A390P L581F G1116E E297G V444A G260D I206V S874P C107R G410D A588V G1116F G374S D482G E297K V284A I939M I112T L413W S593R G1116R A390P N591S V444A G295C R958Q W114R I420T I627T S1120N R432T T655I T510T G295R F959C Y157C D440E E636G R1128C V444A T655I G295S F959V A167T G455E R698C S1144R I498T D676Y R299K T965S A167V K461E S699P R1153C A570T P710P R303K F971L I182K T463I E709K R1153H T586I L827I L339V F971Y M183T Q466K G758R S1154P G648V G855R H423R L1006F M183V R470Q G766R N1173D T655I E1186K V444A N1009H G188W Y472C Y818F T1210P T923P V444D K1145N M217R V481E R832C N1211D A926P V444G I1183T R223C D482G R832H V1212F R948C A459V S226L R487H T859R R1231Q G1004D I468I G238V R487P A865V R1231W R1050C R487L T242I N490D Q869P L1242I G1116R Q546K A257G I498T G877R D1243G R1128H Q558H V284L G499E S901R R1268Q L1197G E592Q E297G I512T R948C A1283V R1231Q V597M R303G N515T N979D G1292V R616G R303K R517H G982R G1298R T619A Q312H F540L G1004D M677L R313S I541L T1029K M677V G327E I541T G1032R R696Q W330R F548Y A1044P R698H Nonsense mutations (premature stop-codons) S25X Y472X Y772X R1090X E96X W493X Q791X V1147X W330X R520X R928X Q1215X Y354X I528X Y1041X R1235X R415X R575X R1057X E1302X R470X Q702X Q1058X Table 1 (Continued) PFIC BRIC/NFC ICP Other liver diseases Genetic variants without disease association Splice site mutations 76 + 3G > T 908 + 1delG 2178 + 1G > T 3057-2A > G Q159Q 77-1G > C 908 + 1G > T 2179-2A > G 3213 + 1delG Q361Q 99-1G > T 908 + 1G > A 2343 + 1G > T 3213 + 4A > G 150 + 3A > C 1435-13 -8del 2343 + 2T > C 3213 + 5G > A 390-1G > A 2012-8T > G 2611-2A > T 611 + 1G > A 2178 + 1G > A R1001R Deletions/insertions/frame shifts Q101Dfs8X L380Wfs18X G648Vfs5X Q1058Hfs38X F959Hfs1X T127Hfs6X A382 A388del K700Sfs12X I1061Vfs34X F959Gfs48X N199Ifs14X P456Pfs24X T919del L1165del L232Cfs9X H484Rfs5X K930Efs92X A1192Efs50X R303Sfs17X I528Sfs21X K930Efs79X T1256Tfs40X V368Rfs27X I610Qfs45X K969 K972del Synonymous variants without disease association R33R F90F L232L I416I G557G I876I A1028A K1145K D36D I134I Y269Y G418G V597V G937G K1070K R52R S136S Q312Q F427F A804A Y981Y T1086T D58D V195V G319G E395E A535A G817G G1004G A1110A The overview shows ࣈ 290 known variants of BSEP on the protein level, except splice site mutations, which are shown on cDNA level.
X
ABCB11 p.Asn591Ser 22795478:185:455
status: NEW208 A few ''common`` BSEP mutations (including p.E297G, p.D482G and p.N591S) have been detected in ICP-patients in heterozygous form and account for about 1.4% (7/491) of ICP-patients [150].
X
ABCB11 p.Asn591Ser 22795478:208:66
status: NEW209 Canalicular expression of BSEP with the ''typical`` ICP mutation p.N591S was higher than that of the BRIC-2 (p.A570 T, p.R1050 C) or PFIC-2 mutations (p.D482G, p.E297G) [144].
X
ABCB11 p.Asn591Ser 22795478:209:67
status: NEW210 Recently, a neonate has been described with homozygousity for p.N591S and, in addition, a homozygous mutation (p.H338Y) in the SLC27A5 gene.
X
ABCB11 p.Asn591Ser 22795478:210:64
status: NEW212 This child presented with liver fibrosis within the first year of life, while a sibling was free of symptoms although it had the same homozygous SLC27A5 mutation, while it was heterozygous for p.N591S [151], demonstrating a ''dose effect`` of N591S.
X
ABCB11 p.Asn591Ser 22795478:212:195
status: NEWX
ABCB11 p.Asn591Ser 22795478:212:243
status: NEW
No.
Sentence
Comment
89
Among these p.E297G, p.D482G and p.N591S belong to the more frequent mutations.
X
ABCB11 p.Asn591Ser 25027376:89:35
status: NEW100 For example, the two 'BRIC-2 mutations` p.A570T and p.R1050C had lower expression levels than the 'ICP mutation` p.N591S, but higher expression levels as compared to the PFIC-2 mutations p.D482G and p.E297G [59].
X
ABCB11 p.Asn591Ser 25027376:100:115
status: NEW138 b Some variants (such as E297G or N591S of BSEP) may affect transport handling on different levels.
X
ABCB11 p.Asn591Ser 25027376:138:34
status: NEW
PMID: 26019043
[PubMed]
Czubkowski P et al: "Successful pregnancy after ileal exclusion in progressive familial intrahepatic cholestasis type 2."
No.
Sentence
Comment
59
Several estrogens and progesterone metabolites are able to induce trans-inhibition of BSEP and the subsequent toxicity induced by the accumulation of bile acids, which may also play a role in the etiopathogenesis of intrahepatic cholestasis of pregnancy (ICP).10,11 Mutations in MDR3 (ABCB4) gene coding transporter for phospholipids across the canalicular membrane may account for 15% of cases of ICP.12 Interestingly, a Czubkowski P, et al. , 2015; 14 (4): 550-552 few "common" BSEP mutations (including p.E297G, p.D482G, and p.N591S) have been detected in ICP-patients in heterozygous form, and common BSEP polymorphism (p.V444A) has been linked to ICP as well.13 The reoccurrence of BSEP cholestasis and development of ICP may be clinically indistinguishable, since both usually present with pruritus, elevated bile acids and aminotransferases, and normal hepatic imaging.11,12 Moreover, in ICP, mutations or polymorphisms of some hepatobiliary transport proteins may contribute to disease pathogenesis or severity, but on the other hand consideration must be given to the possibility of other rare underlying hepatic disorders that may be unmasked during pregnancy with cholestasis as its first manifestation.14 Thus, the diagnosis of ICP should be given after exclusion of preexisting liver disease.15 Pruritus remains the most important clinical symptom of PFIC-2.
X
ABCB11 p.Asn591Ser 26019043:59:532
status: NEW