The Complexity of Newborn Screening Follow-Up in Phenylketonuria.

[phenylketonuria]

In the United States , and most developed nations , the newborn screening (NBS ) panel covers many primary disorders of metabolism , including phenylketonuria (PKU ). When an elevated phenylalanine level is identified , the infant is evaluated for PKU and should also be tested for tetrahydrobiopterin (BH 4 ) deficiency . A neonate presented with a phenylalanine level of 254 μmol /L (reference range <138 μmol /L ) on newborn screening . The infant 's confirmatory phenylalanine was 118 μmol /L (reference range <77 μmol /L ). Her urine pterin profile was normal , and initially she had no measurable activity of red blood cell (RBC ) dihydropteridine reductase (DHPR ). Subsequent study revealed normal levels of CSF tetrahydrobiopterin and neurotransmitter metabolites , and by 18 months of age , her RBC DHPR activity was detectable at 0 .5 nmol /min /mgHgb (reference range 0 .8 -3 .9 ). Sequencing of the QDPR gene for DHPR revealed c .1 A >T nucleotide substitution in exon 3 expressed as "p .M ET 1 ?" Phenylalanine hydroxylase (PAH ) gene sequencing revealed compound heterozygosity for L 249 F and A 300 S . Although initial testing suggested the child was affected with DHPR deficiency , further analysis , finding increasing levels of DHPR activity and PAH compound mutant heterozygosity , indicated that the primary disorder is mild hyperphenylalaninemia with carrier status for DHPR deficiency . This is an example of newborn screening results leading to confusing findings requiring extensive biochemical studies and genotyping in order to arrive at the appropriate diagnosis .