ABCC8 p.Thr1531Ala

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PMID: 19475716 [PubMed] Sandal T et al: "The spectrum of ABCC8 mutations in Norwegian patients with congenital hyperinsulinism of infancy."
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11 Altogether, 16 different ABCC8 mutations (including the novel alterations W231R, C267X, IVS6-3C.G, I462V, Q917X and T1531A) were identified.
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ABCC8 p.Thr1531Ala 19475716:11:116
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106 Six of the ABCC8 mutations (W231R, C267X, IVS6-3C.G, I462V, Q917X, and T1531A) were novel, whereas the remaining have been previously reported and in several cases functionally characterized (Table 2).
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ABCC8 p.Thr1531Ala 19475716:106:71
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122 We classified the mutations as either MnMn Hypo-N3 R1493W MMMM Mn Mn Hypo-N6 V21D MM MnMn Hypo-N8 G1400R / R1493W MM nnMn Hypo-N9 IVS10 Mn Hypo-N11 G1478R Mn nnMn Hypo-N16 C267X Mn Mn Hypo-N19 IVS10 / T1531A MM Mn nn Hypo-N29 IVS10 Mn Mn Hypo-N30 W231R / L503P MM MM x Hypo-N23 IVS10 / P1413L MM x Hypo-N14 IVS10 Mn Hypo-N22 IVS6 (I462V) / Q917X MM Hypo-N25 V21D / E490X MM xx Hypo-N26 V187D / R248 X MM x Hypo-N31 R1493W nnMnMnMn nnnnMn MnMn MM MnMn Mn nnnn Fig. 1.
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ABCC8 p.Thr1531Ala 19475716:122:201
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131 In families Hypo-N11 and Hypo-N19, the mutations G1478R and T1531A occurred de novo as they were not seen in blood samples from the parents.
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ABCC8 p.Thr1531Ala 19475716:131:60
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133 ABCC8 mutations found in Norwegian CHI patientsa Nucleotide change Location Amino acid change Mutation type PSIC score PD Number of families Reference c.62 T.A Exon 1 V21D Mis 1.96 PoD 2 (24) c.560 T.A Exon 4 V187D Mis 2.01 PrD 1 (2) c.691 T.C Exon 5 W231R Mis 4.03 PrD 1 NR c.742 C.T Exon 5 R248X Non - - 1 (34, 42) c.801 C.A Exon 5 C267X Non - - 1 NR IVS6-3C.G Intron 6 - AS - - 1 NR c.1384 A.G Exon 9 I462V Mis 0.62 PrB 1 NR c.1468 G.T Exon 10 E490X Non - - 1 (43) c.1508 T.C Exon 10 L503P Mis 2.36 PrD 1 (24) IVS1011G.T Intron 10 - AS - - 5 (44) c.2749 C.T Exon 23 Q917X Non - - 1 NR c.4198 G.A Exon 35 G1400R Mis 2.37 PrD 1 (42) c.4238 C.T Exon 35 P1413L Mis 2.76 PrD 1 (25) c.4432 G.A Exon 37 G1478R Mis 2.37 PrD 1 (14, 31) c.4477 C.T Exon 37 R1493W Mis 2.79 PrD 3 (26) c.4591 A.G Exon 38 T1531A Mis 1.93 PoD 1 NR AS, aberrant splicing; Mis, missense; NR, not previously reported; Non, nonsense; PD, pathogenic description; PoD, possibly damaging; PrB, predicted to be benign; PrD, probably damaging; PSIC, position-specific independent counts.
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ABCC8 p.Thr1531Ala 19475716:133:795
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142 This proband had an IVS1011G.T mutation inherited from the mother and a de novo T1531A mutation likely to have arisen on the paternal allele.
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ABCC8 p.Thr1531Ala 19475716:142:80
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173 Three novel variants (W231R, I462V, and T1531A) are missense mutations.
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ABCC8 p.Thr1531Ala 19475716:173:40
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177 The mutations I462V and T1531A, however, are positioned outside the TMD and NBD of SUR1 and have lower PSIC scores.
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ABCC8 p.Thr1531Ala 19475716:177:24
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181 Concerning T1531A, it must have occurred de novo on the paternal chromosome of the affected child, assuming that the disease in family Hypo-N19 was inherited recessively.
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ABCC8 p.Thr1531Ala 19475716:181:11
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182 This would predict T1531A to be pathogenic.
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ABCC8 p.Thr1531Ala 19475716:182:19
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