Hyperphenylalaninemia is a medical condition characterized by mildly or strongly elevated concentrations of the amino acidphenylalanine in the blood. Phenylketonuria (PKU) can result in severe hyperphenylalaninemia.[1] Phenylalanine concentrations ([phe]) are routinely screened in newborns by the neonatal heel prick (Guthrie test), which takes a few drops of blood from the heel of the infant. Standard [phe] concentrations in unaffected persons are about 60µM: [phe] concentrations in persons with untreated phenylketonuria may be many times that (600µM to 2400µM), which indicate that the child is at risk for severe intellectual disability. Phenylketonuria is classed as an autosomal recessive condition: in heterozygous form, [phe] shows a moderate elevation, perhaps two-fold over that of unaffected homozygotes, which is classified as hyperphenylalaninemia (hyper- + phenylalanine + -emia = high [phe] in blood).
Hyperphenylalaninemia
Hyperphenylalaninemia can be inherited in an autosomal recessive manner.
The coloration of the skin, hair, and eyes is different in children with PKU. This is caused by low levels of tyrosine, whose metabolic pathway is blocked by deficiency of PAH. Another skin alteration that might occur is the presence of irritation or dermatitis. The child's behaviour may be influenced as well due to augmented levels of phenethylamine which in turn affects levels of other amines in the brain. Psychomotor function may be affected and observed to worsen progressively.[citation needed]
Cause
People with the genotype for PKU are unaffected in utero, because maternal circulation prevents buildup of [phe]. After birth, PKU in newborns is treated by a special diet with highly restricted phenylalanine content. Persons with genetic predisposition to PKU have normal mental development on this diet. Previously, it was thought safe to withdraw from the diet in the late teens or early twenties, after the central nervous system was fully developed; recent studies suggest some degree of relapse, and a continued phenylalanine-restricted diet is now recommended.[2]
PKU or hyperphenylalaninemia may also occur in persons without the PKU genotype. If the mother has the PKU genotype but has been treated so as to be asymptomatic, high levels of [phe] in the maternal blood circulation may affect the non-PKU fetus during gestation. Mothers successfully treated for PKU are advised to return to the [phe]-restricted diet during pregnancy.[citation needed]
A small subset of patients with hyperphenylalaninemia shows an appropriate reduction in plasma phenylalanine levels with dietary restriction of this amino acid; however, these patients still develop progressive neurologic symptoms and seizures and usually die within the first 2 years of life ("malignant" hyperphenylalaninemia). These infants exhibit normal phenylalanine hydroxylase (PAH) enzymatic activity but have a deficiency in dihydropteridine reductase (DHPR), an enzyme required for the regeneration of tetrahydrobiopterin (THB or BH4), a cofactor of PAH.[citation needed]
Less frequently, DHPR activity is normal but a defect in the biosynthesis of THB exists. In either case, dietary therapy corrects the hyperphenylalaninemia. However, THB is also a cofactor for two other hydroxylation reactions required in the syntheses of neurotransmitters in the brain: the hydroxylation of tryptophan to 5-hydroxytryptophan and of tyrosine to L-dopa. It has been suggested that the resulting deficit in the CNS neurotransmitter activity is, at least in part, responsible for the neurologic manifestations and eventual death of these patients.[3] Hyperphenylalaninemia most is commonly diagnosed by newborn screening and must be distinguished from classic PKU by confirmatory testing at an experienced center. Some cases in adult women have been detected using maternal screening programs or following birth of children with birth defects. Elevated phenylalanine levels are associated with neuropsychological effects.[citation needed]
Diagnosis
This section is empty. You can help by adding to it. (October 2021)
Treatment
Maintain plasma phenylalanine values in therapeutic range of 120 to 360 mM using a diet that restricts phenylalanine but otherwise nutritionally complete. Treatment for life is recommended to reduce the risk of long term neuropsychiatric problems and reduce the risk of maternal PKU syndrome.[citation needed]
Outcome
With treatment the outcome is excellent. Most infants with classic PKU who are treated within the first 10 days of life achieve normal intelligence. However learning problems are more frequent than in unaffected peers.[citation needed]
References
^. omim.org. Archived from the original on 2014-05-29. Retrieved 2016-06-03.
^van Wegberg AM, MacDonald A, Ahring K, Bélanger-Quintana A, Blau N, Bosch AM, et al. (October 2017). "The complete European guidelines on phenylketonuria: diagnosis and treatment". Orphanet Journal of Rare Diseases. 12 (1): 162. doi:10.1186/s13023-017-0685-2. PMC5639803. PMID 29025426.
^Lieberman M, Marks AD (2013). Marks' Basic Medical Biochemistry (fourth ed.). ISBN978-1-60831-572-7.
External links
January 11, 2023
hyperphenylalaninemia, medical, condition, characterized, mildly, strongly, elevated, concentrations, amino, acid, phenylalanine, blood, phenylketonuria, result, severe, hyperphenylalaninemia, phenylalanine, concentrations, routinely, screened, newborns, neona. Hyperphenylalaninemia is a medical condition characterized by mildly or strongly elevated concentrations of the amino acid phenylalanine in the blood Phenylketonuria PKU can result in severe hyperphenylalaninemia 1 Phenylalanine concentrations phe are routinely screened in newborns by the neonatal heel prick Guthrie test which takes a few drops of blood from the heel of the infant Standard phe concentrations in unaffected persons are about 60µM phe concentrations in persons with untreated phenylketonuria may be many times that 600µM to 2400µM which indicate that the child is at risk for severe intellectual disability Phenylketonuria is classed as an autosomal recessive condition in heterozygous form phe shows a moderate elevation perhaps two fold over that of unaffected homozygotes which is classified as hyperphenylalaninemia hyper phenylalanine emia high phe in blood HyperphenylalaninemiaHyperphenylalaninemia can be inherited in an autosomal recessive manner SpecialtyEndocrinology Contents 1 Symptoms and signs 2 Cause 3 Diagnosis 4 Treatment 5 Outcome 6 References 7 External linksSymptoms and signs EditThe coloration of the skin hair and eyes is different in children with PKU This is caused by low levels of tyrosine whose metabolic pathway is blocked by deficiency of PAH Another skin alteration that might occur is the presence of irritation or dermatitis The child s behaviour may be influenced as well due to augmented levels of phenethylamine which in turn affects levels of other amines in the brain Psychomotor function may be affected and observed to worsen progressively citation needed Cause EditPeople with the genotype for PKU are unaffected in utero because maternal circulation prevents buildup of phe After birth PKU in newborns is treated by a special diet with highly restricted phenylalanine content Persons with genetic predisposition to PKU have normal mental development on this diet Previously it was thought safe to withdraw from the diet in the late teens or early twenties after the central nervous system was fully developed recent studies suggest some degree of relapse and a continued phenylalanine restricted diet is now recommended 2 PKU or hyperphenylalaninemia may also occur in persons without the PKU genotype If the mother has the PKU genotype but has been treated so as to be asymptomatic high levels of phe in the maternal blood circulation may affect the non PKU fetus during gestation Mothers successfully treated for PKU are advised to return to the phe restricted diet during pregnancy citation needed A small subset of patients with hyperphenylalaninemia shows an appropriate reduction in plasma phenylalanine levels with dietary restriction of this amino acid however these patients still develop progressive neurologic symptoms and seizures and usually die within the first 2 years of life malignant hyperphenylalaninemia These infants exhibit normal phenylalanine hydroxylase PAH enzymatic activity but have a deficiency in dihydropteridine reductase DHPR an enzyme required for the regeneration of tetrahydrobiopterin THB or BH4 a cofactor of PAH citation needed Less frequently DHPR activity is normal but a defect in the biosynthesis of THB exists In either case dietary therapy corrects the hyperphenylalaninemia However THB is also a cofactor for two other hydroxylation reactions required in the syntheses of neurotransmitters in the brain the hydroxylation of tryptophan to 5 hydroxytryptophan and of tyrosine to L dopa It has been suggested that the resulting deficit in the CNS neurotransmitter activity is at least in part responsible for the neurologic manifestations and eventual death of these patients 3 Hyperphenylalaninemia most is commonly diagnosed by newborn screening and must be distinguished from classic PKU by confirmatory testing at an experienced center Some cases in adult women have been detected using maternal screening programs or following birth of children with birth defects Elevated phenylalanine levels are associated with neuropsychological effects citation needed Diagnosis EditThis section is empty You can help by adding to it October 2021 Treatment EditMaintain plasma phenylalanine values in therapeutic range of 120 to 360 mM using a diet that restricts phenylalanine but otherwise nutritionally complete Treatment for life is recommended to reduce the risk of long term neuropsychiatric problems and reduce the risk of maternal PKU syndrome citation needed Outcome EditWith treatment the outcome is excellent Most infants with classic PKU who are treated within the first 10 days of life achieve normal intelligence However learning problems are more frequent than in unaffected peers citation needed References Edit OMIM Entry 261600 Phenylketonuria PKU omim org Archived from the original on 2014 05 29 Retrieved 2016 06 03 van Wegberg AM MacDonald A Ahring K Belanger Quintana A Blau N Bosch AM et al October 2017 The complete European guidelines on phenylketonuria diagnosis and treatment Orphanet Journal of Rare Diseases 12 1 162 doi 10 1186 s13023 017 0685 2 PMC 5639803 PMID 29025426 Lieberman M Marks AD 2013 Marks Basic Medical Biochemistry fourth ed ISBN 978 1 60831 572 7 External links Edit Retrieved from https en wikipedia org w index php title Hyperphenylalaninemia amp oldid 1049627729, wikipedia, wiki, book, books, library,
