Phenylketonuria
Phenylketonuria
Phenylketonuria
Definition:
The signs and symptoms of PKU vary from mild to severe. The most severe form
of this disorder is known as classic PKU. Infants with classic PKU appear normal
until they are a few months old. Without treatment, these children develop
permanent intellectual disability. Seizures, delayed development, behavioral
problems, and psychiatric disorders are also common. Untreated individuals may
have a musty or mouse-like odor as a side effect of excess phenylalanine in the
body. Children with classic PKU tend to have lighter skin and hair than
unaffected family members and are also likely to have skin disorders such as
eczema.
Less severe forms of this condition, sometimes called variant PKU and non-PKU
hyperphenylalaninemia, have a smaller risk of brain damage. People with very
mild cases may not require treatment with a low-phenylalanine diet.
Babies born to mothers with PKU and uncontrolled phenylalanine levels (women
who no longer follow a low-phenylalanine diet) have a significant risk of
intellectual disability because they are exposed to very high levels of
phenylalanine before birth. These infants may also have a low birth weight and
grow more slowly than other children. Other characteristic medical problems
include heart defects or other heart problems, an abnormally small head size
(microcephaly), and behavioral problems. Women with PKU and uncontrolled
phenylalanine levels also have an increased risk of pregnancy loss.
Metabolic pathway:
PAH is an integral enzyme used to convert the amino acid Phenylalanine to the
amino acid Tyrosine. Tyrosine is then subsequently catalyzed using another
enzyme, Tyrosine hydroxylase (TH). TH functions in conjunction with
tetrahydrobiopterin (BH4), the same cofactor used with PAH, to produce L-3,4-
dihydroxyphenylalanine, more commonly referred to as L-DOPA.
Pathophysiology:
Genetics:
Manifestations:
Older individuals who cease dietary treatment in childhood may have evidence of
demyelination on MRI. Occasionally, deterioration of cognitive performance or
motor skills also may be present. Intelligence quotients (IQs) may drop by 10
points or more if the diet is stopped in midchildhood.
Diagnostic Procedures:
If a child is not screened during the routine newborn screening test (typically
performed 2 – 7 days after birth, using samples drawn by neonatal heel prick),
the disease may present clinically with seizures, albinism (excessively fair hair
and skin), and a "musty odor" to the baby's sweat and urine (due to
phenylacetate, one of the ketones produced). In most cases, a repeat test should
be done at approximately two weeks of age to verify the initial test and uncover
any phenylketonuria that was initially missed.
Untreated children are normal at birth, but fail to attain early developmental
milestones, develop microcephaly, and demonstrate progressive impairment of
cerebral function. Hyperactivity, EEG abnormalities, and seizures, and severe
learning disabilities are major clinical problems later in life. A "musty or mousy"
odor of skin, hair, sweat and urine (due to phenylacetate accumulation), as well
as a tendency towards hypopigmentation and eczema, are also observed.
In contrast, affected children who are detected and treated are less likely to
develop neurological problems or have seizures and intellectual disability, though
such clinical disorders are still possible.
Management/ Treatment:
Another therapeutic approach is to orally supply all of the large neutral amino
acids, except phenylalanine, in order to compete with phenylalanine for transport
into the brain, which is mediated by the neutral amino acid carrier at the blood-
brain barrier. This therapy lowers brain phenylalanine concentrations and leads
to improvements in EEG patterns of adults with hyperphenylalaninemia (Pietz et
al 1999). With the addition of arginine and lysine to the neutral amino acid mix,
some competition with phenylalanine uptake in the intestinal lumen may also be
achieved resulting in decreased plasma phenylalanine concentrations (Matalon
et al 2006). This therapy is not sufficiently robust to be routinely used in young
children or women during pregnancy, but can be successfully employed to block
the central nervous system effects of hyperphenylalaninemia in adolescents and
adults who are unable to adhere to the protein-restricted diet.
There is some discussion about which individuals will tolerate relaxation of the
diet as adults. Possible predictors include brain phenylalanine concentrations or
genotype predictors of residual enzyme activity (Greeves et al 2000). Current
recommendations are that therapy should be for life to prevent declining
intellectual performance. However, unlike individuals with other inborn errors of
protein metabolism, patients with phenylketonuria do not feel ill when they ingest
excessive protein. The effects are subtle, but certainly can affect quality of life
just as severely as in other inborn errors of protein metabolism. These issues
must be addressed during adolescence, yet the typical adolescent must be
allowed some personal control over the treatment of their disease. It can be a
delicate balance.