ABCD1 p.Arg104His

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PMID: 11336405 [PubMed] Neumann S et al: "Identification of new mutations in Israeli patients with X-linked adrenoleukodystrophy."
No. Sentence Comment
6 Five missense-type mutations were identified: R104H, Y174C, L229P, R401Q, and G512C.
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ABCD1 p.Arg104His 11336405:6:46
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50 Three of the mutations-R104H, R401Q, and R464X-were previouslydescribedin patients with ALD and are substitutions of arginine (Fanen et al., 1994; Fuchs et al., 1994; Braun et al., 1995).
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ABCD1 p.Arg104His 11336405:50:23
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53 MUTATIONS IN THE ALD GENE Family number Exon cDNA alteration Amino acid alteration Missense: 1 1 G697A R104H 2 1 A907G Y174C 3, 4, 5 1 T1072C L229P 6 3 G1588A R401Q 7 6 G1920T G512C Nonsense: 8 4 C1776T R464X Frameshift: 9 1 901insC Y171 frameshift 10 5 1800insC E471 frameshift FIG. 1.
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ABCD1 p.Arg104His 11336405:53:103
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PMID: 11748843 [PubMed] Kemp S et al: "ABCD1 mutations and the X-linked adrenoleukodystrophy mutation database: role in diagnosis and clinical correlations."
No. Sentence Comment
164 X-ALD Mutations Identified in the ABCD1 Gene Allele Exon Mutation Protein Remark fs P42 1 125insC n.d. # fs P84 1 253insC n.d. # E90K 1 268G>A n.d. # S98L 1 293C>T Present S98L 1 293C>T Present R104H 1 311G>A n.d. fs A112 1 337delC Absent # R113C 1 337C>T Present # R113P 1 338G>C n.d. # Q133X 1 397C>T Absent W137X 1 411G>A Absent P143S 1 427C>T n.d. S149N 1 446G>A Present R152S 1 454C>A n.d. R152C 1 454C>T Present R152L 1 455G>T Reduced # S161P 1 481T>C n.d. # R163P 1 488G>C n.d. Y174C 1 521A>G Absent Y174C 1 521A>G n.d. Q177X 1 529C>T Absent Y181C 1 542A>G n.d. fs Y181 1 544ins8bp n.d. # Q195X 1 583C>T n.d. # T198K 1 593C>A n.d. # fs S207 1 621del664bp Absent # SV207-8insAAS 1 622-23ins9bp n.d. # K217E 1 649A>G Present # P218T 1 652C>A n.d. V224E 1 671T>G n.d. # L229P 1 686T>C n.d. L229P 1 686T>C n.d. fs S235 1 706delCGTG n.d. # W242X 1 726G>A Absent G266R 1 796G>A n.d. G266R 1 796G>A n.d. R274W, R280C 1 820C>T, 838C>T n.d. # R285P 1 854G>C n.d. S290X 1 869C>A Absent # E291del 1 871-73delGAG Absent Y296C 1 887A>G n.d. Y296C 1 887A>G n.d. fs E300 IVS1 IVS1+1g>t n.d. # fs E300 IVS1 IVS1-1g>a n.d. # S315X 2 944C>A n.d. # K336M 2 1007A>T n.d. # G343D 2 1028G>A n.d. # R401Q 3 1202G>A Present R401Q 3 1202G>A Present K407X 3 1219A>T n.d. # E427del 4 1279-81delGAA n.d. # Q430X 4 1288C>T n.d. # R464X 4 1390C>T n.d. fs E471 5 1415delAG Absent fs E471 5 1415delAG Absent fs E471 5 1415delAG Absent fs E471 5 1415delAG Absent C511X 6 1533C>A n.d. # R518Q 6 1553G>A Absent fs G528 6 1586-90del Absent # fs Y532 6 1599delG Absent # P543L 6 1628C>T Absent P543L 6 1628C>T Absent fs Q544 6 1628-34duplicated n.d. # fs R545 IVS 6 IVS6+1g>c n.d. # R554H 7 1661G>A Absent fs Q556 7 1670delTG n.d. # (continued) replaced by a pyrimidine (C or T) or vice versa, and transitions, comprising the substitution of one purine by the other, or of one pyrimidine by the other.
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ABCD1 p.Arg104His 11748843:164:194
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PMID: 10190819 [PubMed] Takano H et al: "Mutational analysis and genotype-phenotype correlation of 29 unrelated Japanese patients with X-linked adrenoleukodystrophy."
No. Sentence Comment
87 Review of previous publications indicated that 14 missense mutations are associated exclu- sivelywithAMNorAddisondiseaseonly,includingC696T (R104C),33,34 G697A(R104H),42 C700T(T105I),45 G832A (S149N),35 C918G(Q178E),42 T1045C(L220P),35 C1137T (T254M),37 G1266A(A294T),45 C1551G(R389G),37 G1552A (R389H),33,35 C1638T (R418W),37 C1930T (S515F),38 T2084A(M566K),33 andG2211A(E606K).35,37 Analysisof these mutations may provide important insights into the mechanisms involved in variable phenotypic expressions in ALD.
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ABCD1 p.Arg104His 10190819:87:160
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PMID: 7717396 [PubMed] Braun A et al: "Mutations in the gene for X-linked adrenoleukodystrophy in patients with different clinical phenotypes."
No. Sentence Comment
81 C918G Q178E (missense) 1 Mother, heterozygous for both mutations C1022G Y212STOP (nonsense) ADO-001 .
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ABCD1 p.Arg104His 7717396:81:6
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82 G697A R104H (missenseb) 1 Mother, heterozygous a Nucleotide positions of cDNA as published by Mosser et al.
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ABCD1 p.Arg104His 7717396:82:6
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124 The G-to-A transition at nucleotide position 697 leads to an arginine-to-histidine substitution at position 104.
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ABCD1 p.Arg104His 7717396:124:61
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83 G697A R104H (missenseb) 1 Mother, heterozygous a Nucleotide positions of cDNA as published by Mosser et al.
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ABCD1 p.Arg104His 7717396:83:6
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125 The G-to-A transition at nucleotide position 697 leads to an arginine-to-histidine substitution at position 104.
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ABCD1 p.Arg104His 7717396:125:61
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123 The G-to-A transition at nucleotide position 697 leads to an arginine-to-histidine substitution at position 104.
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ABCD1 p.Arg104His 7717396:123:61
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PMID: 24788897 [PubMed] Durmaz A et al: "Molecular analysis in X-linked adrenoleukodystrophy patients: identification of a novel mutation."
No. Sentence Comment
67 p. R104H and p. R104K mutations occuring at the same amino acid residue had been previously reported (Kemp et al. 2001).
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ABCD1 p.Arg104His 24788897:67:3
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68 An absent enzyme activity was first reported in an Israeli patient having p. R104H mutation (Neumann et al. 2001).
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ABCD1 p.Arg104His 24788897:68:77
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