Insertion of an extra codon for threonine is a cause of dihydropteridine reductase deficiency
The mutation in a patient with dihydropteridine reductase deficiency has been located and characterized. Polymerase chain reaction (PCR) was used to amplify the coding sequence of human dihydropteridine reductase from the messenger RNA of skin fibroblasts. Chemical cleavage of mismatches indicated a...
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| Published in | American journal of human genetics Vol. 47; no. 2; pp. 279 - 285 |
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| Main Authors | , , , |
| Format | Journal Article |
| Language | English |
| Published |
Chicago, IL
University of Chicago Press
01.08.1990
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| Subjects | |
| Online Access | Get full text |
| ISSN | 0002-9297 1537-6605 |
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| Abstract | The mutation in a patient with dihydropteridine reductase deficiency has been located and characterized. Polymerase chain reaction (PCR) was used to amplify the coding sequence of human dihydropteridine reductase from the messenger RNA of skin fibroblasts. Chemical cleavage of mismatches indicated a mismatched thymine and cytosine at approximately 117 and 147 bases, respectively, from the end of the probe. Cloning and sequencing of the mutant PCR products revealed the insertion of the triplet ACT (threonine), after alanine 122 (base 390). Amplification of a small region around this mutation by using genomic DNA as the PCR target indicates that the mutation is completely within an exon. Unequal crossing-over at the second base in the preceding alanine codon and duplication of the bases CTA may be the mechanism of mutagenesis. The cleavage site 147 bases from the end of the probe corresponded to the conversion of guanine to adenine at base 420 (CTG to CTA) and does not alter the code for leucine. This change, which was also seen in another dihydropteridine reductase-deficient child and in a control subject probably represents a common neutral polymorphism. |
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| AbstractList | The mutation in a patient with dihydropteridine reductase deficiency has been located and characterized. Polymerase chain reaction (PCR) was used to amplify the coding sequence of human dihydropteridine reductase from the messenger RNA of skin fibroblasts. Chemical cleavage of mismatches indicated a mismatched thymine and cytosine at approximately 117 and 147 bases, respectively, from the end of the probe. Cloning and sequencing of the mutant PCR products revealed the insertion of the triplet ACT (threonine), after alanine 122 (base 390). Amplification of a small region around this mutation by using genomic DNA as the PCR target indicates that the mutation is completely within an exon. The mutation in a patient with dihydropteridine reductase deficiency has been located and characterized. Polymerase chain reaction (PCR) was used to amplify the coding sequence of human dihydropteridine reductase from the messenger RNA of skin fibroblasts. Chemical cleavage of mismatches indicated a mismatched thymine and cytosine at approximately 117 and 147 bases, respectively, from the end of the probe. Cloning and sequencing of the mutant PCR products revealed the insertion of the triplet ACT (threonine), after alanine 122 (base 390). Amplification of a small region around this mutation by using genomic DNA as the PCR target indicates that the mutation is completely within an exon. Unequal crossing-over at the second base in the preceding alanine codon and duplication of the bases CTA may be the mechanism of mutagenesis. The cleavage site 147 bases from the end of the probe corresponded to the conversion of guanine to adenine at base 420 (CTG to CTA) and does not alter the code for leucine. This change, which was also seen in another dihydropteridine reductase-deficient child and in a control subject probably represents a common neutral polymorphism.The mutation in a patient with dihydropteridine reductase deficiency has been located and characterized. Polymerase chain reaction (PCR) was used to amplify the coding sequence of human dihydropteridine reductase from the messenger RNA of skin fibroblasts. Chemical cleavage of mismatches indicated a mismatched thymine and cytosine at approximately 117 and 147 bases, respectively, from the end of the probe. Cloning and sequencing of the mutant PCR products revealed the insertion of the triplet ACT (threonine), after alanine 122 (base 390). Amplification of a small region around this mutation by using genomic DNA as the PCR target indicates that the mutation is completely within an exon. Unequal crossing-over at the second base in the preceding alanine codon and duplication of the bases CTA may be the mechanism of mutagenesis. The cleavage site 147 bases from the end of the probe corresponded to the conversion of guanine to adenine at base 420 (CTG to CTA) and does not alter the code for leucine. This change, which was also seen in another dihydropteridine reductase-deficient child and in a control subject probably represents a common neutral polymorphism. The mutation in a patient with dihydropteridine reductase deficiency has been located and characterized. Polymerase chain reaction (PCR) was used to amplify the coding sequence of human dihydropteridine reductase from the messenger RNA of skin fibroblasts. Chemical cleavage of mismatches indicated a mismatched thymine and cytosine at approximately 117 and 147 bases, respectively, from the end of the probe. Cloning and sequencing of the mutant PCR products revealed the insertion of the triplet ACT (threonine), after alanine 122 (base 390). Amplification of a small region around this mutation by using genomic DNA as the PCR target indicates that the mutation is completely within an exon. Unequal crossing-over at the second base in the preceding alanine codon and duplication of the bases CTA may be the mechanism of mutagenesis. The cleavage site 147 bases from the end of the probe corresponded to the conversion of guanine to adenine at base 420 (CTG to CTA) and does not alter the code for leucine. This change, which was also seen in another dihydropteridine reductase-deficient child and in a control subject probably represents a common neutral polymorphism. |
| Author | COTTON, R. G. H DAHL, H.-H. M FORREST, S. M HOWELLS, D. W |
| AuthorAffiliation | Olive Miller Laboratory, Murdoch Institute, Royal Children's Hospital, Parkville, Victoria, Australia |
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| Keywords | Human Phenylketonuria Enzyme Deficiency Dihydropteridine reductase Mutation Genetic disease |
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| References_xml | – reference: 3540926 - Postgrad Med J. 1986 Feb;62(724):113-23 – reference: 14279179 - J Pharmacol Exp Ther. 1965 Apr;148:1-8 – reference: 6379341 - Med Res Rev. 1984 Jul-Sep;4(3):267-321 – reference: 2483035 - Anal Biochem. 1989 Dec;183(2):263-8 – reference: 4405600 - J Biol Chem. 1972 Oct 10;247(19):6082-91 – reference: 6844267 - Prenat Diagn. 1983 Jan;3(1):7-11 – reference: 7326033 - Biochem J. 1981 Sep 15;198(3):677-82 – reference: 2895188 - J Med Genet. 1988 Jan;25(1):25-8 – reference: 2787020 - Nucleic Acids Res. 1989 Jun 12;17(11):4223-33 – reference: 13525410 - J Biol Chem. 1958 Feb;230(2):931-9 – reference: 3031582 - Nucleic Acids Res. 1987 Mar 11;15(5):1921-32 – reference: 3680258 - J Biol Chem. 1987 Dec 5;262(34):16412-6 – reference: 3033643 - Proc Natl Acad Sci U S A. 1987 May;84(10):3329-33 – reference: 6101503 - Lancet. 1980 Jan 19;1(8160):160 – reference: 3260032 - Proc Natl Acad Sci U S A. 1988 Jun;85(12):4397-401 – reference: 5294952 - J Biol Chem. 1966 Jan 10;241(1):192-6 – reference: 7115669 - Biochemistry. 1982 Jul 6;21(14):3284-94 |
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| SubjectTerms | Amino Acid Sequence Aminoacid disorders Base Sequence Biological and medical sciences Codon Dihydropteridine Reductase - genetics DNA - genetics DNA Probes Errors of metabolism Humans insertion Medical sciences Metabolic diseases Molecular Sequence Data NADH, NADPH Oxidoreductases - deficiency Nucleic Acid Heteroduplexes - genetics Phenylketonurias Polymerase Chain Reaction RNA, Messenger Threonine - genetics |
| Title | Insertion of an extra codon for threonine is a cause of dihydropteridine reductase deficiency |
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