Abstract

Classical Phenylketonuria (PKU) is a birth defect caused by an inborn error in amino acid metabolism. The genetic disorder is autosomal recessive and is characterized by deficiency of the hepatic enzyme phenylalanine hydroxylase (PAH) which catalyzes the hydroxylation of phenylalanine to tyrosine. The lack of activity causes elevated phenylalanine level in blood and results in severe mental retardation of the untreated children. The prevalance of PKU among Caucasions is about 1/10,000, and 2% of the population are carriers of PKU. We have previously reported the isolation and characterization of a full-length human PAH cDNA clone which was used to detect restriction fragment- length polymorphisms (RFLP's) at the PAH locus and led to the development of an analytical method for prenatal diagnosis of PKU. This method of analysis however, is applicable only to those families with prior PKU history. RFLP haplotypes for both normal and PKU alleles have been determined for Northern European PKU families. We observed that 90% of mutant alleles are restricted to 4 distinct RFLP haplotypes. Cloning and sequencing analyses of two to these prevalent mutant alleles have revealed point mutations affecting normal mRNA splicing and an amino acid substitution. Oligonucleotides specific for the mutations have been used as hybridization probes to demonstrate that there is a tight association between these mutations and the particular RFLP haplotypes among mutant alleles due to linkage disequilibrium. Additional prevalent PKU genes will be characterized by sequence analysis, and their respective frequencies as well as haplotype associations will be determine. If PKU is indeed caused by a limited number of prevalent mutant alleles, it will be possible to develop a cassett of specific oligonucleotides for carrier detection in the population without prior family history of PKU. Furthermore, mutant alleles in individuals of the less severe hyperphenylalaninemic phenotypes will also be analyzed, which may contain structural mutations that will provide further insight into the structure-function relationship of the enzyme. In addition, the cis-acting elements in the PAH gene responsible for its liver-specific expression and regulation will be characterized and the corresponding trans- acting factors identified. Finally, we will be characterized and the corresponding trans-acting factors identified. Finally, we will attempt to create an animal model of PKU through transgenic mouse technology in order to better understand the pathophysiology of mental retardation in patients.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37HD017711-07
Application #
3485134
Study Section
Mammalian Genetics Study Section (MGN)
Project Start
1983-04-01
Project End
1993-03-31
Budget Start
1989-04-01
Budget End
1990-03-31
Support Year
7
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Baylor College of Medicine
Department
Type
Schools of Medicine
DUNS #
074615394
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Enns, G M; Martinez, D R; Kuzmin, A I et al. (1999) Molecular correlations in phenylketonuria: mutation patterns and corresponding biochemical and clinical phenotypes in a heterogeneous California population. Pediatr Res 46:594-602
Eisensmith, R C; Martinez, D R; Kuzmin, A I et al. (1996) Molecular basis of phenylketonuria and a correlation between genotype and phenotype in a heterogeneous southeastern US population. Pediatrics 97:512-6
Santos, M; Kuzmin, A I; Eisensmith, R C et al. (1996) Phenylketonuria in Costa Rica: preliminary spectrum of PAH mutations and their associations with highly polymorphic haplotypes. Hum Hered 46:128-31
Eisensmith, R C; Woo, S L (1995) Molecular genetics of phenylketonuria: from molecular anthropology to gene therapy. Adv Genet 32:199-271
Eisensmith, R C; Goltsov, A A; Woo, S L (1994) A simple, rapid, and highly informative PCR-based procedure for prenatal diagnosis and carrier screening of phenylketonuria. Prenat Diagn 14:1113-8
Li, J; Eisensmith, R C; Wang, T et al. (1994) Phenylketonuria in China: identification and characterization of three novel nucleotide substitutions in the human phenylalanine hydroxylase gene. Hum Mutat 3:312-4
Wang, Y; Hahn, T M; Tsai, S Y et al. (1994) Functional characterization of a unique liver gene promoter. J Biol Chem 269:9137-46
Svensson, E; von Dobeln, U; Eisensmith, R C et al. (1993) Relation between genotype and phenotype in Swedish phenylketonuria and hyperphenylalaninemia patients. Eur J Pediatr 152:132-9
Goltsov, A A; Eisensmith, R C; Naughton, E R et al. (1993) A single polymorphic STR system in the human phenylalanine hydroxylase gene permits rapid prenatal diagnosis and carrier screening for phenylketonuria. Hum Mol Genet 2:577-81
Svensson, E; Wang, Y; Eisensmith, R C et al. (1993) Three polymorphisms but no disease-causing mutations in the proximal part of the promoter of the phenylalanine hydroxylase gene. Eur J Hum Genet 1:306-13

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