ABCC7 p.Gly970Asp

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PMID: 10453741 [PubMed] Wagner JA et al: "Two novel mutations in a cystic fibrosis patient of Chinese origin."
No. Sentence Comment
5 In exon 16, mutation 3041G→A causes the missense change G970D.
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ABCC7 p.Gly970Asp 10453741:5:63
status: NEW
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6 Functional analysis using an isotopic flux assay indicated that the G970D mutation retains partial function; western blotting indicated that the protein is glycosylated.
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ABCC7 p.Gly970Asp 10453741:6:68
status: NEW
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32 Functional analysis G970D was evaluated by introducing the change into human CFTR cDNA using the Stratagene (La Jolla, Calif.)
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ABCC7 p.Gly970Asp 10453741:32:20
status: NEW
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62 Exon 16 was heterozygous for 3041G→A, which converts the codon GGT to GAT and causes the missense 512 Table 1 Primer sequences used to amplify specific CFTR exons Exon Name Base Sequence (5'-3') pair 1 SO-006 204 TTGAGCGGCAGGCACCCAG SO-007 ACACGCCCTAATCTTTCGTG 2 SO-093 178 AGTGAATATCTCTTCCTCCTC SO-094 TTTCTCTTCAACTAAACAATGT 4 SO-016 369 TGTGTTGAAATTCTCAGGGT SO-017 CAGAATATATGTGCCATGGG 5 SO-087 185 ATTATCTAACTTTCCATTTTT SO-88 ACTCCGCCTTTCTTCCAGTTGTA 14a SO-101 200 ATTCTTTTATTCAGGAGTGC SO-102 CCAAACTATCTTAATTTAACTTTA 14b SO-099 203 GGAGGAATAGGTGAAGATGT SO-100 TGGGAGAAATGAAACAAAGT 15 SO-023 485 GTGCATGCTCTTCTAATGCA SO-024 AAGGCACATGCCTCTGTGCA 16 SO-89 191 TGTGATCCAAACTTAGTATTG SO-90 CTTAACGGTACTTATTTTTACA 17a SO-091 199 CATGTTTTCTTTGATCTTACAG SO-092 TGAGTATCGCACATTCACTG 18 SO-097 188 AGGTTCATTTACGTCTTTTG SO-098 ACTTTGTTACTTGTCTGAATTT 23 SO-108 190 ATTACAAGGGCAATGAGATC SO-087 ATTATCTAACTTTCCATTTTT change G970D (Fig.2).
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ABCC7 p.Gly970Asp 10453741:62:922
status: NEW
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63 G970D is a novel mutation, but G970R was reported previously in a single Belgian patient (Cuppens et al. 1993).
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ABCC7 p.Gly970Asp 10453741:63:0
status: NEW
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65 Physiological analysis of G970D To determine whether partial function of G970D might explain this subject`s spared pancreatic function, we made a G970D construct using site-directed mutagenesis, expressed it in HEK cells and assayed for CFTR function using an iodide efflux assay.
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ABCC7 p.Gly970Asp 10453741:65:26
status: NEW
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ABCC7 p.Gly970Asp 10453741:65:73
status: NEW
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ABCC7 p.Gly970Asp 10453741:65:146
status: NEW
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67 As shown in Fig.3, efflux from cells transfected with the G970D construct was significantly reduced relative to that seen in cells transfected with WT CFTR, but was significantly elevated in comparison with control cells transfected with vector alone.
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ABCC7 p.Gly970Asp 10453741:67:58
status: NEW
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71 We used a western assay to compare G970D with WT CFTR, the M470V polymorphism, and ∆F508.
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ABCC7 p.Gly970Asp 10453741:71:35
status: NEW
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75 B Chromatogram to illustrate heterozygosity for G/A at position 3041(N) in exon 16, giving rise to G970D.
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ABCC7 p.Gly970Asp 10453741:75:99
status: NEW
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79 Asterisks above the points for G970D indicate a significant difference from WT; asterisks below the points indicate a significant difference from vector (P < 0.05); bars are SEM Fig.4 Western blot analysis of G970D CFTR protein.
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ABCC7 p.Gly970Asp 10453741:79:31
status: NEW
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ABCC7 p.Gly970Asp 10453741:79:209
status: NEW
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81 The four lanes represent wild type CFTR and the M470V polymorphism (positive controls), ∆F508 (a negative control showing no processing to fully glycosylated CFTR), and G970D Based on this assay, processing of G970D was affected somewhat relative to WT (Fig.), but not more than the common polymorphism M470V.
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ABCC7 p.Gly970Asp 10453741:81:176
status: NEW
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ABCC7 p.Gly970Asp 10453741:81:218
status: NEW
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95 The 8-bp deletion is expected to eliminate all functional CFTR expressed from that chromosome, whereas G970D retains partial function.
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ABCC7 p.Gly970Asp 10453741:95:103
status: NEW
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96 Mutation G970D affects the same codon as the previously reported G970R (Cuppens et al. 1993).
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ABCC7 p.Gly970Asp 10453741:96:9
status: NEW
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102 Of interest, they found that the peak efflux for the construct G970E was about half that of WT, which is very similar to our result for the natural mutation G970D.
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ABCC7 p.Gly970Asp 10453741:102:157
status: NEW
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105 Pancreatic sufficiency could presumably arise from the residual Cl-channel function of G970D CFTR, or from a residual ability to regulate chloride/bicarbonate transport (Lee et al. 1999).
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ABCC7 p.Gly970Asp 10453741:105:87
status: NEW
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106 The relatively large efflux observed for G970D (approximately 50% of WT) is probably an overestimate of function.
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ABCC7 p.Gly970Asp 10453741:106:41
status: NEW
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PMID: 11158459 [PubMed] Wine JJ et al: "Comprehensive mutation screening in a cystic fibrosis center."
No. Sentence Comment
16 Mutations detected in both groups included 7 missense mutations (S13F, P67L, G98R, S492F, G970D, L1093P, N1303K) and 9 deletion, frameshift, nonsense or splicing mutations (R75X, G542X, ⌬F508, 451-458⌬8 bp, 5T, 663⌬T, exon 13 frameshift, 1261؉1G3A and 3272-26A3G).
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ABCC7 p.Gly970Asp 11158459:16:90
status: NEW
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17 Three of these mutations were novel (G970D, L1093P, and 451-458⌬8 bp1).
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ABCC7 p.Gly970Asp 11158459:17:37
status: NEW
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115 Mutation Detection in 10 Participants With Positive Sweat Chloride Values I.D. Pancreatic Function Mutation Status Discovered Mutations (Novel) Polymorphisms SP1 PI N1303K/unk* L1093P (17b), M470V (10)* SP2 PI unk*/unk* S13F (exon1) 2184 ins A (exon 13) GATT7/7, 2694 T/G SP3 PS unk*/unk* ⌬451-458 (4); G970D (16) GATT7/6, 2694 T/G SP4 PS unk*/unk* R75X (3), G98R (4) GATT7/7, 492 G/A SP5 PS unk*/unk 3272-26A/G (17b) M470V/M470V (10) SP6 PI/PS (mild) ⌬F508/unk None found - SP7 PI ⌬F508/unk None found GATT6/7,1001ϩ11C/T (6b), M470V (10) SP8 PI unk*/unk S492F (10) GATT7/7 GT11/11 M470V/M470V SP9 PI ⌬F508/unk None found - SP10 PI unk*/unk* 663 ⌬T/663 ⌬T GATT6/6, 2694T3G Column labeled Pancreatic Function indicates the need for dietary supplementation with pancreatic enzymes.
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ABCC7 p.Gly970Asp 11158459:115:310
status: NEW
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135 Novel mutations ⌬451-458 and G970D were reported separately1; novel mutation L1093P has been submitted for publication.
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ABCC7 p.Gly970Asp 11158459:135:36
status: NEW
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PMID: 15357566 [PubMed] Ngukam A et al: "A novel missense mutation A1081P in the cystic fibrosis transmembrane conductance regulator (CFTR) gene identified in a Laotian patient with congenital bilateral absence of the vas deferens."
No. Sentence Comment
4 Only a few CFTR mutations have been identified in that population (L88X, M152R, K166E, F508del, 1742delAC, 1525-18G>A, 1540del10, L568X, 1898ϩ1G>T, 1898ϩ5G>T, G970D, 451-458del8, 3121-2A>G, H1085R).1-6 We report here a novel missense mutation in a Laotian patient with congenital bilateral absence of the vas deferens (CBAVD).
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ABCC7 p.Gly970Asp 15357566:4:171
status: NEW
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PMID: 19318346 [PubMed] Goubau C et al: "Phenotypic characterisation of patients with intermediate sweat chloride values: towards validation of the European diagnostic algorithm for cystic fibrosis."
No. Sentence Comment
60 Table 2 CFTR mutations in the patient subgroups CF-PS CFTR dysfunction CF unlikely Genotype Subjects (n) Genotype Subjects (n) Genotype Subjects (n) F508del*/Not found 12 F508del*/3849+10 kb(C.T){ 11 Not found/Not found 39 Not found/Not found 10 F508del*/R117H{ 7 F508del*/Not found 4 F508del*/3849+10 kb(C.T){ 7 F508del*/Not found 7 IVS8-5T{/Not found 1 F508del*/R347P{ 5 Not found/Not found 5 S1235E/E528E 1 F508del*/R117H{ 4 F508del*/D1152H{ 4 No mutation analysis 1 F508del*/2789+5G.A{ 4 F508del*/IVS8-5T{ 4 Total 46 F508del*/S945L* 3 F508del*/S945L* 2 2789+5G.A{/Not found 3 W1282X*/IVS8-5T{ 2 F508del*/3272-26 A.G{ 2 F508del*/R1070W{ 1 F508del*/A455E{ 2 F508del*/L159S 1 F508del*/711+5G.A 2 F508del*/T1246I 1 F508del*/2789+5G.A 2 F508del*/L165S 1 G542X*/R334W{ 2 W1282X*/D1152H{ 1 F508del*/R334W{ 2 R1162X*/D1152H{ 1 R347P{/Not found 2 R347Hu/D1152H{ 1 F508del*/2116delCTAA 1 R553X*/R117H{ 1 F508del*/IVS8-5T{ 1 3659delC*/R117H{ 1 F508del*/D1152H{ 1 3849+10kb(C.T){/G551R 1 F508del*/711+3A.G 1 R1162X*/3849+10 kb(C.T){ 1 F508del*/L206W{ 1 2789+5G.A{/Not found 1 F508del*/I336K{ 1 G542X*/T854A 1 F508del*/G970D 1 R553X*/Q1463H 1 F508del*/L159S 1 S1235R/R668C 1 F508del*/R751L 1 2789+5G.A{/S977F 1 F508del*/E656X 1 No mutation analysis 1 F508del*/4015delA 1 Total 59 F508del*/Y913S 1 F508del*/L165S 1 F508del*/2143delT 1 G551D*/I336K{ 1 G551D*/3272-26A.G{ 1 G551D*/711+3A.G 1 R553X*/4005+2T.C 1 R553X*/E92K{ 1 G542X*/L206W{ 1 W1282X*/I336K 1 R1162X*/3849+10 kb(C.T){ 1 R1162X*/2789+5G.A{ 1 574delA*/3141del9 1 9890X/I105N 1 R334W{/R1070Q{ 1 3272-26A.G{/4218insT 1 3272-26A.G{/L165S 1 711+3A.G/G1244E 1 R352Q/1812-1G.A 1 F1052V/IVS8-5T{ 1 R74W/D1270N 1 1898-3G.A/1898-3G.A 1 1717-1G.A*/R334W{ 1 3659delC*/Not found 1 394delTT/Not found 1 R1162X*/Not found 1 R553X*/Not found 1 R117H{/Not found 1 G85E*/Not found 1 3849+10k(C.T){/Not found 1 Total 103 *Mutation class I, II or III.
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ABCC7 p.Gly970Asp 19318346:60:1110
status: NEW
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PMID: 22483971 [PubMed] Li H et al: "Mutations in the cystic fibrosis transmembrane conductance regulator (CFTR) in Chinese patients with congenital bilateral absence of vas deferens."
No. Sentence Comment
77 Lastly, we have observed previously reported mutations and polymorphisms (p.E217G, p.R347H, p.V470M, p.R553X, p.I556V, p.T854T, p.G970D, p.P1290P, p.Q1352H, p.Q1643Q, 744-5delGATT, IVS8-T5) (Supplementary Table 1).
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ABCC7 p.Gly970Asp 22483971:77:130
status: NEW
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119 △F508 R117H Mutation genotypes IVS8-Tn n (%) Two mutations detected Neg Neg I556V/I556V 7T/7T 1(1.3) Neg Neg I556V/1209+2 G-C 5T/7T 1(1.3) Neg Neg I556V/726delATT 5T/5T 1(1.3) Neg Neg I556V/- 5T/5T 1(1.3) Neg Neg I556V/- 5T/7T 1(1.3) Neg Neg G970D/- 5T/7T 1(1.3) Neg Neg C592F/- 5T/5T 1(1.3) Neg Neg 1209+1 G-C/- 5T/7T 1(1.3) Neg Neg R553X/- 5T/7T 1(1.3) Neg Neg Q1352H/- 5T/7T 1(1.3) Neg Neg S485C/- 5T/7T 1(1.3) Neg Neg A357T/- 5T/7T 1(1.3) Neg Neg E217G/- 5T/7T 1(1.3) Neg Neg R347H/- 5T/7T 1(1.3) Neg Neg G451K/- 5T/7T 1(1.3) Neg Neg L558S/- 5T/7T 1(1.3) Neg Neg 3635delT/Q1352H 7T/7T 1(1.3) Neg Neg A1136T/G970D 7T/7T 1(1.3) Neg Neg 870-1 G-C/- 5T/7T 1(1.3) Neg Neg 520-2 A-G/- 5T/7T 1(1.3) Neg Neg R419I/- 5T/7T 1(1.3) Neg Neg C491F/Q1643Q 7T/7T 1(1.3) Neg Neg Q1352H/- 5T/7T 1(1.3) Neg Neg R851X/- 5T/7T 1(1.3) Neg Neg P750L/G970D 7T/7T 1(1.3) One mutation detected Neg Neg -/- 5T/7T 2(2.7) Neg Neg -/- 5T/7T 3(4.1) Neg Neg -/- 5T/7T 5(6.8) Neg Neg -/- 5T/5T 2(2.7) Neg Neg -/- 5T/5T 1(1.3) Neg Neg G970D/- 7T/7T 2(2.7) Neg Neg D993Y/- 7T/7T 1(1.3) Neg Neg I556V/- 7T/7T 1(1.3) Neg Neg T388R/- 7T/7T 1(1.3) No mutation detected Neg Neg -/- 7T/7T 8(10.9) Neg Neg -/- 7T/7T 15(20.5) Neg Neg -/- 7T/9T 2(2.7) Neg Neg -/- 7T/7T 4(5.5) Neg: Negative.
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ABCC7 p.Gly970Asp 22483971:119:249
status: NEW
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ABCC7 p.Gly970Asp 22483971:119:618
status: NEW
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ABCC7 p.Gly970Asp 22483971:119:839
status: NEW
X
ABCC7 p.Gly970Asp 22483971:119:1013
status: NEW
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76 Lastly, we have observed previously reported mutations and polymorphisms (p.E217G, p.R347H, p.V470M, p.R553X, p.I556V, p.T854T, p.G970D, p.P1290P, p.Q1352H, p.Q1643Q, 744-5delGATT, IVS8-T5) (Supplementary Table 1).
X
ABCC7 p.Gly970Asp 22483971:76:130
status: NEW
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118 b3;F508 R117H Mutation genotypes IVS8-Tn n (%) Two mutations detected Neg Neg I556V/I556V 7T/7T 1(1.3) Neg Neg I556V/1209+2 G-C 5T/7T 1(1.3) Neg Neg I556V/726delATT 5T/5T 1(1.3) Neg Neg I556V/- 5T/5T 1(1.3) Neg Neg I556V/- 5T/7T 1(1.3) Neg Neg G970D/- 5T/7T 1(1.3) Neg Neg C592F/- 5T/5T 1(1.3) Neg Neg 1209+1 G-C/- 5T/7T 1(1.3) Neg Neg R553X/- 5T/7T 1(1.3) Neg Neg Q1352H/- 5T/7T 1(1.3) Neg Neg S485C/- 5T/7T 1(1.3) Neg Neg A357T/- 5T/7T 1(1.3) Neg Neg E217G/- 5T/7T 1(1.3) Neg Neg R347H/- 5T/7T 1(1.3) Neg Neg G451K/- 5T/7T 1(1.3) Neg Neg L558S/- 5T/7T 1(1.3) Neg Neg 3635delT/Q1352H 7T/7T 1(1.3) Neg Neg A1136T/G970D 7T/7T 1(1.3) Neg Neg 870-1 G-C/- 5T/7T 1(1.3) Neg Neg 520-2 A-G/- 5T/7T 1(1.3) Neg Neg R419I/- 5T/7T 1(1.3) Neg Neg C491F/Q1643Q 7T/7T 1(1.3) Neg Neg Q1352H/- 5T/7T 1(1.3) Neg Neg R851X/- 5T/7T 1(1.3) Neg Neg P750L/G970D 7T/7T 1(1.3) One mutation detected Neg Neg -/- 5T/7T 2(2.7) Neg Neg -/- 5T/7T 3(4.1) Neg Neg -/- 5T/7T 5(6.8) Neg Neg -/- 5T/5T 2(2.7) Neg Neg -/- 5T/5T 1(1.3) Neg Neg G970D/- 7T/7T 2(2.7) Neg Neg D993Y/- 7T/7T 1(1.3) Neg Neg I556V/- 7T/7T 1(1.3) Neg Neg T388R/- 7T/7T 1(1.3) No mutation detected Neg Neg -/- 7T/7T 8(10.9) Neg Neg -/- 7T/7T 15(20.5) Neg Neg -/- 7T/9T 2(2.7) Neg Neg -/- 7T/7T 4(5.5) Neg: Negative.
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ABCC7 p.Gly970Asp 22483971:118:248
status: NEW
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ABCC7 p.Gly970Asp 22483971:118:617
status: NEW
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ABCC7 p.Gly970Asp 22483971:118:838
status: NEW
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ABCC7 p.Gly970Asp 22483971:118:1012
status: NEW
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