ABCD1 p.Ser515Tyr

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PMID: 26454440 [PubMed] Chu SS et al: "Eight novel mutations in the ABCD1 gene and clinical characteristics of 25 Chinese patients with X-linked adrenoleukodystrophy."
No. Sentence Comment
86 Eight of the 22 mutations [c.1017G>T (p.W339C), c.892G>C (p.G289R), c.532C>T (p.Q178*), c.1544C>A (p.S515Y), c.1428C>A (p.C476*), c.1182delG (p.A395Lfs*15), c.424delC (p.L142Sfs*56), c.1759_1761dup (p.I588H)] were novel (Fig. 2).
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ABCD1 p.Ser515Tyr 26454440:86:101
status: NEW
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111 However, some X-ALD males remain asymptomatic and one-third of heterozygous women remain free of clinical symptoms during their Patient number Exon Nucleotide change Amino acid change Protein localization References P1 2 c.1017G>T p.Trp339Cys TMD Novel P2 8 c.1850G>A p.Arg617His NBD Fanen et al, 1994[12] P4 1 c.892G>C p.Gly298Arg TMD Novel P5, P6 5 c.1415_16delAG p.Gln472Argfs*83 TMD to NBD Barcelo et al, 1994[13] P7 1 c.532C>T p.Gln178* TMD Novel P8 1 c.473T>C p.Leu158Pro TMD The peroxisomal diseases laboratory (unpublished) P10 6 c.1552C>T p.Arg518Trp NBD Fanen et al, 1994[12] P11 3 c.1202G>A p.Arg401Gln TMD to NBD Fuchs et al, 1994[14] P12 1 c.887A>G p.Tyr296Cys TMD Takano et al, 1999[15] P13 1 c.893G>A p.Gly298Asp TMD Lachtermacher et al, 2000[16] P14 1 c.310C>T p.Arg104Cys TMD Kok et al, 1995[17] P15 IVS 8 c.1866-10G>A p.Pro623fs* NBD Kemp et al, 1995[18] P16 5 c.1428C>A p.Cys476* NBD Novel P17 5 c.1421T>C p.Ile474Thr NBD Shimozawa et al, 2011[19] P18 6 c.1538A>G p.Lys513Arg NBD Piti&#e9;-Salp&#e9;tri&#e8;re Hospital (unpublished) P19 1 c.310C>T p.Arg104Cys TMD Kok et al, 1995[17] P20 6 c.1544C>A p.Ser515Tyr NBD Novel P21 2 c.901-1G>A p.Val301fs* TMD Kemp et al, 2001[20] P22 2 c.974T>C p.Leu325Pro TMD The peroxisomal diseases laboratory (unpublished) P23 3 c.1182delG p.Ala395Leufs*15 TMD to NBD Novel P24 1 c.424delC p.Leu142Serfs*56 TMD Novel P25 7 c.1759_1761dup p.Ile588His NBD Novel Table 2.
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ABCD1 p.Ser515Tyr 26454440:111:1121
status: NEW
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114 Variables P1 P4 P20 cDNA mutations c.1017G>T c.892G>C c.1544C>A Protein level p.Trp339Cys p.Gly298Arg p.Ser515Tyr Conservation Highly conserved Highly conserved Highly conserved Polyphen prediction Probably damaging Probably damaging Probably damaging SIFT prediction Deleterious Deleterious Deleterious Align-GVGD Most likely to interfere with function Most likely to interfere with function Most likely to interfere with function Amino acid location (wild-type residue) A transmembrane domain ABC transmembrane type-1 ABC transporter Amino acid size change (than the wild-type residue) Smaller Bigger Bigger Amino acid physicochemical property change Aromatic amino acids to neutral polar amino acids (hydrophilicity) Non polar aliphatic amino acids to alkaline amino acids Neutral polar amino acids to aromatic amino acids (hydrophilic reduced) Charge characteristic change No Neutral to positive No Form a hydrogen bond with the neighbors No No Yes Influence from the mutant residue Disturb either the contacts with the other transmembrane domains or with the lipid-membrane Change the flexibility of wild-type residue which might abolish protein function The size difference makes that the new residue is not in the correct position and interferes with hydrogen bond Table 3.
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ABCD1 p.Ser515Tyr 26454440:114:104
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118 A: c.1017G>T (p.W339C); B: c.892G>C (p.G289R); C: c.532C>T (p.Q178*); D: c.1544C>A (p.S515Y); E: c.1428C>A (p.C476*); F: c.1182delG (p.A395Lfs*15); G: c.424delC (p.L142Sfs*56); H: c.1759_1761dup (p.I588H).
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ABCD1 p.Ser515Tyr 26454440:118:86
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121 b1;-Helix is presented in green, b2;-strands is displayed in yellow and coil is marked with gray respectively; B: Change of ALDP structure in three patients with novel missense mutations: c.1017G>T (p.Trp339Cys) in P1, c.892G>C (p.Gly298Arg) in P4, and c.1544C>A (p.Ser515Tyr) in P20.
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ABCD1 p.Ser515Tyr 26454440:121:272
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123 A B p.Trp339Cys p.Gly298Arg p.Ser515Tyr entire life.
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ABCD1 p.Ser515Tyr 26454440:123:30
status: NEW
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