Additional Dietary Large Neutral Amino Acids (LNAA) for Improved Symptoms in Adult Classical Phenylktonuria (PKU)

University of Southern California

Status

Active, not recruiting

Conditions

Phenylketonurias

Treatments

Other: PreKUnil® LNAA Medical Food for PKU

Study type

Interventional

Funder types

Other

Identifiers

NCT05174559

LNAA for PKU

Details and patient eligibility

About

This research investigates the effects of combining a phenylalanine restricted diet (usual care) with LNAA supplementation (adjuvant LNAA) in well-controlled adults with classical PKU. The hypothesis is that symptoms are improved in well-controlled patients who receive adjuvant LNAA therapy compared with diet monotherapy. Six symptomatic classical PKU adults will be enrolled to test the hypothesis in a small series of N-of-1 randomized controlled trials over 18-weeks. All assessments will be collected in patient's homes. A 3-month follow-up period will assess the longer-term effects of adjuvant LNAA in patients who show clinical benefit at the end of the intervention period.

Full description

Clinical care of PKU confronts an increasing proportion of early-treated well-controlled adults, with a treatment goal that quality of life be as normal as possible. Even adults who have successfully managed their blood phenylalanine levels from birth can have symptoms which impact daily function. New therapies that target symptoms are needed, especially for symptomatic well-controlled classical adults with few treatment options. In Denmark and the LAC+USC U.S. clinic, adults are offered large neutral amino acid (LNAA) supplements when diet monotherapy becomes less effective for symptom management, or the patient wants a less restrictive diet. Many patients report improved symptoms. LNAA supplementation doesn't significantly reduce blood phenylalanine, suggesting a different mechanism for patient perceived benefits. Both LNAA supplementation and a phenylalanine restricted diet aim to improve brain neurotransmitter biochemistry to optimize outcomes through dietary intervention. The overall objective of this research is to evaluate additional dietary LNAAs on symptom management in adults with classical PKU at an individual level. N-of-1 randomized controlled trials will provide the highest level of evidence. The scientific premise is that manipulation of dietary LNAAs affects blood LNAA concentrations. LNAAs compete with phenylalanine for a shared transporter from blood to brain, dependent on blood concentrations and transporter affinities. Higher blood phenylalanine levels in adult PKU, with high transport affinity, produces excessive phenylalanine brain entry at the expense of other LNAAs. Insufficient LNAAs impairs synthesis of chemicals in the brain (neurotransmitters), a suggested mechanism of action for adult PKU symptoms. Additional dietary LNAAs may help to overcome this limitation of adult usual care. The study uses established PKU treatment products (medical foods) and biomarkers, (1) to determine effect of the adjuvant LNAA diet in symptom management; and (2) to evaluate correlations between changes in biomarkers and changes in symptoms during the intervention. Should findings show additive clinical value of LNAAs to the PKU diet, the strategy may become a useful adjunct. For participants, results will bring them closer to evidence-based individualized care. This work could advance the field closer toward personalized management.

Enrollment

10 estimated patients

Sex

All

Ages

18+ years old

Volunteers

No Healthy Volunteers

Inclusion criteria

age ≥ 18 years
diagnosis of classical PKU (blood phenylalanine ≥1200 µmol pre-treatment or off-treatment
≥ 2 PKU-related symptoms with clinically meaningful negative impact on daily life
is in regular clinical monitoring and is treated with a PKU diet with a natural protein restriction and medical foods
average blood phenylalanine levels between 360 and 900 µmol in past one year
able and willing to provide consent
demonstrates capacity to complete all requirements of the protocol
if on medications approved by the Principal Investigator agrees not to alter dose for duration of study
has stable daily access to phone, internet, and physical address

Exclusion criteria

women who are breastfeeding, pregnant or planning to become pregnant in the next year
use of adjuvant PKU treatments (LNAAs, Kuvan®, Palinziq®) within past 3 months
use of psychotropic medications, melatonin, or any serotonin-reuptake inhibitors within past 3 months
demonstrates insufficient motivation or time required to complete full trial

Trial design

Primary purpose

Treatment

Allocation

Randomized

Interventional model

Crossover Assignment

Masking

Triple Blind

10 participants in 2 patient groups, including a placebo group

Active LNAA

Active Comparator group

Description:

Active LNAA tablets are given to each participant in 3 multiple crossovers for a total exposure to the Active Comparator 3 times. The allocation is randomized within each cycle of two treatments (active/inactive). There are 3 total cycles for each participant. The intervention is PreKUnil® tablets.

Treatment:

Other: PreKUnil® LNAA Medical Food for PKU

Inactive LNAA

Placebo Comparator group

Description:

Inactive LNAA tablets (placebos) are given to each participant in 3 multiple crossovers for a total exposure to the Inactive Comparator 3 times. The allocation is randomized within each cycle of two treatments (inactive/active). There are 3 total cycles for each participant. The placebo intervention is PreKUnil® placebo tablets.

Treatment:

Other: PreKUnil® LNAA Medical Food for PKU

Trial contacts and locations

Central trial contact

Kathryn Moseley, RD, MS; Annie Prince, RD. PhD

Data sourced from clinicaltrials.gov

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