Sodium Phenylbutyrate

The dosage of Sodium Phenylbutyrate is not "one size fits all." It must be meticulously calculated based on the patient's body surface area (BSA) or body weight and their individual protein tolerance. For adults and children weighing more than 20 kg (approximately 44 lbs), the standard recommended daily dose ranges from 9.9 to 13.0 grams per square meter (g/m²) per day.

This total daily dose is never taken all at once. It is typically divided into equal amounts and administered with each meal (e.g., three to six times per day) to coincide with the intake of dietary protein. The maximum daily dose is generally capped at 20 grams per day to avoid potential neurotoxicity from the phenylacetate metabolite.

In pediatric patients, particularly neonates and infants weighing less than 20 kg, dosing is even more critical. The recommended total daily dose for these small patients is 450 to 600 mg/kg/day.

As with adults, the dose must be divided into equal parts and given with each feeding. Because infants feed frequently, the medication may be administered 4 to 6 times in a 24-hour period. For very young infants, the powder formulation is typically mixed with formula or breast milk. Parents must be careful not to heat the mixture excessively, as this could potentially degrade the medication.

Renal Impairment

Sodium Phenylbutyrate should be used with extreme caution in patients with renal (kidney) impairment. Since the primary route of excretion for the nitrogen-scavenging product (phenylacetylglutamine) is the kidneys, a reduction in renal function can lead to the accumulation of metabolites. Healthcare providers may need to lower the dose or increase the frequency of monitoring for these patients.

Hepatic Impairment

Because the conversion of phenylbutyrate to phenylacetate and the subsequent conjugation with glutamine occur primarily in the liver, patients with hepatic (liver) impairment may have a reduced ability to process the drug. This can lead to increased plasma levels of phenylbutyrate and decreased production of the active scavenger. Close monitoring of ammonia levels is mandatory.

Elderly Patients

Clinical studies of Sodium Phenylbutyrate did not include sufficient numbers of subjects aged 65 and over to determine whether they respond differently than younger subjects. In general, dose selection for an elderly patient should be cautious, usually starting at the low end of the dosing range, reflecting the greater frequency of decreased hepatic, renal, or cardiac function.

Proper administration is vital for the success of UCD management:

1. 1With Food: Sodium Phenylbutyrate should always be taken with meals or feedings. This allows the drug to be present in the system as protein is being broken down into nitrogen.
2. 2Consistency: Take the medication at the same times every day to maintain steady levels in the blood.
3. 3Powder Preparation: If using the powder, mix it with a small amount of soft food (like applesauce) or liquid (water, formula, or fruit juice). The powder has a very salty and bitter taste; mixing it with strongly flavored foods may help.
4. 4Tablet Administration: Tablets should be swallowed whole. Do not crush or chew them unless specifically instructed by your doctor, as they have a very unpleasant taste that can cause gagging.
5. 5Storage: Store at room temperature (20°C to 25°C / 68°F to 77°F) in a tightly closed container, away from moisture and direct heat.

If a dose is missed, it should be taken as soon as the patient remembers, provided it is still close to the time of a meal. If it is almost time for the next scheduled dose, skip the missed dose and resume the regular schedule. Never double the dose to make up for a missed one, as this increases the risk of side effects and sodium overload.

An overdose of Sodium Phenylbutyrate can lead to a condition called metabolic acidosis or neurotoxicity. Symptoms of overdose may include extreme sleepiness, confusion, headache, taste disturbances, and lightheadedness. In the event of a suspected overdose, contact a poison control center or seek emergency medical attention immediately. Treatment is generally supportive and may include intravenous fluids to manage electrolyte imbalances.

> Important: Follow your healthcare provider's dosing instructions exactly. Do not adjust your dose or stop the medication without medical guidance, as this could lead to a rapid and dangerous rise in ammonia levels.

Sodium Phenylbutyrate is associated with several common side effects that, while often manageable, can affect a patient's quality of life. According to clinical data published in the Journal of Pediatrics, the most frequently reported adverse reactions include:

• Menstrual Abnormalities: Amenorrhea (absence of periods) or irregular menstrual cycles occur in up to 23% of post-pubertal female patients. This is thought to be related to the drug's effect on the endocrine system.
• Decreased Appetite (Anorexia): Many patients report a significant loss of appetite, which can be challenging since UCD patients already have restricted diets.
• Body Odor: A very specific "locker room" or "sweaty feet" odor is common. This is caused by the metabolite phenylacetate being excreted through the skin and breath.
• Taste Aversion: The medication is notoriously bitter, and many patients develop a strong dislike for the flavor, which can lead to nausea during administration.

• Gastrointestinal Issues: These include abdominal pain, gastritis (inflammation of the stomach lining), nausea, vomiting, and constipation. These symptoms are often worse if the medication is taken on an empty stomach.
• Dermatological Reactions: Rashes or itchy skin (pruritus) have been reported.
• Electrolyte Imbalances: Because the drug is a sodium salt, it can lead to hypernatremia (high sodium) and hypokalemia (low potassium).

• Hematologic Changes: Rare cases of anemia (low red blood cells), leukopenia (low white blood cells), and thrombocytopenia (low platelets) have been observed. Regular blood counts are usually recommended.
• Metabolic Acidosis: An accumulation of acid in the body, which can cause rapid breathing and confusion.
• Syncope: Fainting or temporary loss of consciousness.

While Sodium Phenylbutyrate is life-saving for UCD patients, it can cause severe reactions that require emergency care.

> Warning: Stop taking Sodium Phenylbutyrate and call your doctor immediately if you experience any of the following:

1. 1Neurotoxicity Symptoms: Phenylacetate (the metabolite) can be toxic to the brain at high levels. Symptoms include extreme lethargy, confusion, hallucinations, or a "foggy" feeling that is different from typical ammonia-related symptoms.
2. 2Severe Allergic Reaction (Anaphylaxis): Signs include hives, swelling of the face, lips, or tongue, difficulty breathing, or a rapid heart rate.
3. 3Signs of High Sodium (Hypernatremia): Extreme thirst, confusion, seizures, or muscle twitching. This is particularly dangerous for patients with heart or kidney disease.
4. 4Hypokalemia: Severe muscle weakness, leg cramps, or irregular heartbeats (arrhythmias).

Long-term use of Sodium Phenylbutyrate requires constant vigilance. Prolonged use can lead to chronic nutritional deficiencies because the drug removes glutamine, an amino acid essential for various bodily functions. If glutamine levels fall too low, it can actually impair the body's ability to manage nitrogen, leading to a paradoxical increase in ammonia. Additionally, the high sodium load over many years can contribute to the development of hypertension (high blood pressure) or kidney strain.

As of 2026, there are no FDA black box warnings specifically for Sodium Phenylbutyrate monotherapy. However, there are significant "Warnings and Precautions" regarding its use in patients with heart failure or renal insufficiency due to the high sodium content.

Report any unusual symptoms or changes in your health to your healthcare provider immediately. Regular laboratory testing is the only way to ensure that the medication is not causing silent side effects like electrolyte imbalances or blood count changes.

Sodium Phenylbutyrate is a potent metabolic modifier. It must be used only under the supervision of a physician experienced in the treatment of inborn errors of metabolism. The most critical safety point is that this drug is not for the treatment of acute hyperammonemic coma. Acute episodes of high ammonia are life-threatening emergencies that require hemodialysis or other rapid-acting interventions. Sodium Phenylbutyrate is for long-term, maintenance therapy only.

No FDA black box warnings for Sodium Phenylbutyrate have been issued. However, the FDA emphasizes that it should be used as part of a comprehensive management plan that includes a low-protein diet and, in some cases, essential amino acid supplementation.

Sodium Loading and Fluid Retention

Each gram of Sodium Phenylbutyrate contains approximately 125 mg (5.4 mEq) of sodium. For a patient taking the maximum dose of 20 grams per day, this equates to 2,500 mg of sodium—more than the total daily recommended intake for a healthy adult. This is a major concern for patients with:

• Congestive Heart Failure (CHF): The sodium load can lead to fluid overload and worsen heart failure symptoms.
• Severe Renal Insufficiency: The kidneys may struggle to excrete the excess sodium.
• Edema (Swelling): Patients prone to fluid retention may see an increase in swelling in the legs or lungs.

Neurotoxicity

High levels of the metabolite phenylacetate have been associated with neurotoxicity in animal studies and some human clinical trials (particularly in cancer research where higher doses were used). Patients who experience unexplained sleepiness or confusion while their ammonia levels are normal should be evaluated for phenylacetate toxicity.

Nutritional Deficiencies

Sodium Phenylbutyrate works by removing glutamine. If glutamine levels are depleted too much, it can lead to a deficiency in essential nitrogen carriers. This is why patients must be monitored by a metabolic nutritionist to ensure they are receiving enough (but not too much) protein and amino acid supplements.

Patients taking Sodium Phenylbutyrate require frequent lab tests to ensure safety and efficacy. According to the American College of Medical Genetics and Genomics (ACMG) guidelines, monitoring should include:

1. 1Plasma Ammonia: To ensure the drug is effectively lowering nitrogen levels.
2. 2Plasma Amino Acids: Specifically glutamine (which should be kept in the normal range) and branched-chain amino acids.
3. 3Electrolytes: Specifically sodium, potassium, and bicarbonate to check for hypernatremia or metabolic acidosis.
4. 4Liver and Kidney Function: Periodic BUN, creatinine, and ALT/AST tests.
5. 5Plasma Protein Levels: Albumin and total protein to monitor nutritional status.

Sodium Phenylbutyrate may cause dizziness, lightheadedness, or confusion in some patients. Patients should not drive or operate heavy machinery until they know how the medication affects them. If neurotoxicity symptoms occur, these activities must be avoided entirely.

Alcohol should be avoided while taking Sodium Phenylbutyrate. Alcohol can irritate the stomach lining, potentially worsening the gastrointestinal side effects of the drug. More importantly, alcohol metabolism can interfere with liver function, which is necessary for the drug to work correctly.

Never stop taking Sodium Phenylbutyrate suddenly. Discontinuing the medication can lead to a rapid and dangerous rise in ammonia levels (hyperammonemia), which can cause brain swelling and coma within hours or days. If the medication must be stopped, it must be done under strict medical supervision, usually in a hospital setting where ammonia levels can be monitored hourly.

> Important: Discuss all your medical conditions, especially heart or kidney problems, with your healthcare provider before starting Sodium Phenylbutyrate.

While there are few absolute contraindications regarding drug-drug interactions, certain combinations are highly dangerous for UCD patients:

• Valproic Acid (Depakene, Depakote): This anti-seizure medication is known to induce hyperammonemia by inhibiting the urea cycle enzymes. Using valproic acid with Sodium Phenylbutyrate can negate the drug's effects and cause a life-threatening spike in ammonia levels.
• Haloperidol: Similar to valproate, this antipsychotic has been reported to cause high ammonia levels in some patients and should be avoided.

• Corticosteroids (e.g., Prednisone, Dexamethasone): Steroids increase the breakdown of body protein (catabolism). This process releases large amounts of nitrogen into the bloodstream, which can overwhelm the scavenging capacity of Sodium Phenylbutyrate. If steroids are necessary, ammonia levels must be monitored daily.
• Probenecid: This medication, often used for gout, can inhibit the renal excretion of the conjugated metabolite phenylacetylglutamine. This leads to the accumulation of phenylacetate in the blood, increasing the risk of neurotoxicity.

• Topiramate (Topamax): This medication can cause metabolic acidosis and hyperammonemia. When used with Sodium Phenylbutyrate, it increases the risk of electrolyte imbalances and treatment failure.
• Salicylates (Aspirin): High doses of aspirin can compete for the same excretory pathways in the kidney, potentially slowing the removal of the drug's metabolites.

• High-Protein Meals: The most significant "interaction" is with dietary protein. Sodium Phenylbutyrate is designed to work with a low-protein diet. Consuming a meal high in protein (e.g., a large steak) can produce more ammonia than the drug can scavenge, leading to a metabolic crisis.
• Sodium Intake: Because the drug itself is very high in sodium, patients should avoid high-sodium foods (processed snacks, canned soups) to prevent hypernatremia and fluid retention.

• Amino Acid Supplements: While many UCD patients take specific amino acid formulas (like BCAA), they should avoid general "protein powders" or "whey supplements" found in health stores, as these contain high levels of nitrogen.
• St. John’s Wort: While no direct interaction is documented, St. John's Wort can induce liver enzymes that might theoretically alter the metabolism of phenylbutyrate to phenylacetate.

Sodium Phenylbutyrate can interfere with certain laboratory tests:

• Urinary Ketones: The metabolites of phenylbutyrate may cause a false-positive result for ketones in some urine dipstick tests.
• Plasma Amino Acid Chromatography: The presence of phenylacetylglutamine can sometimes interfere with the peaks on an amino acid chromatogram, making it difficult for the lab to accurately measure other amino acids.

For each major interaction, the management strategy involves:

1. 1Mechanism: Usually pharmacodynamic (competing effects on ammonia) or pharmacokinetic (renal excretion interference).
2. 2Consequence: Increased risk of hyperammonemia (treatment failure) or increased drug toxicity (neurotoxicity).
3. 3Management: Avoidance of the interacting drug, or if unavoidable, daily monitoring of plasma ammonia and electrolytes.

> Important: Tell your doctor about ALL medications, supplements, and herbal products you are taking. Even over-the-counter cold medicines can sometimes contain ingredients that affect nitrogen metabolism.

Sodium Phenylbutyrate must NEVER be used in the following circumstances:

1. 1Acute Hyperammonemia Emergency: This drug is not a rescue medication. In the event of an acute hyperammonemic crisis (ammonia levels >200-300 µmol/L), the patient requires immediate hospitalization and potentially hemodialysis. Using Sodium Phenylbutyrate in this setting is ineffective and delays life-saving treatment.
2. 2Hypersensitivity: Any patient with a known severe allergy to Sodium Phenylbutyrate or phenylacetate must not use this medication. Anaphylactic reactions, though rare, can be fatal.

These are conditions where the drug should only be used if the benefits clearly outweigh the risks, and under intense supervision:

• Congestive Heart Failure (CHF): Due to the high sodium content (125mg per gram of drug), patients with heart failure are at high risk for fluid overload, which can lead to pulmonary edema (fluid in the lungs).
• Severe Renal Insufficiency: When the kidneys cannot filter waste effectively, the drug's metabolites and the high sodium load can accumulate to toxic levels.
• Severe Hepatic Impairment: Since the liver is the primary site of the drug's activation (conversion to phenylacetate), patients with liver failure may not benefit from the drug and may experience increased side effects from the parent compound.
• Pregnancy: Sodium Phenylbutyrate is generally avoided in pregnancy unless the mother's life is at risk, as the metabolites may be toxic to the developing fetus.

Patients who have had allergic reactions to other phenylalkanoic acids (a chemical class of compounds) should be monitored closely for cross-sensitivity. While not common, the structural similarities between these compounds can occasionally trigger similar immune responses.

> Important: Your healthcare provider will evaluate your complete medical history, including heart and kidney function, before prescribing Sodium Phenylbutyrate. This medication requires a delicate balance between nitrogen scavenging and sodium management.

Sodium Phenylbutyrate is classified as Pregnancy Category C. There are no adequate and well-controlled studies in pregnant women. Animal reproduction studies have shown that phenylacetate (the active metabolite) can be neurotoxic to developing fetuses, potentially causing brain damage or developmental delays.

However, untreated urea cycle disorders in the mother are also extremely dangerous and can lead to fatal hyperammonemia during pregnancy or immediately after delivery (postpartum). Therefore, the use of Sodium Phenylbutyrate during pregnancy is a high-risk decision that must be made by a multidisciplinary team including a geneticist and a high-risk obstetrician. If used, the lowest effective dose should be employed, and ammonia levels must be monitored very frequently.

It is not known whether Sodium Phenylbutyrate or its metabolites are excreted in human milk. Because many drugs are excreted in human milk and because of the potential for serious adverse reactions in nursing infants (including neurotoxicity from phenylacetate), a decision should be made whether to discontinue nursing or to discontinue the drug, taking into account the importance of the drug to the mother. Most experts recommend formula feeding for infants if the mother must remain on Sodium Phenylbutyrate.

Sodium Phenylbutyrate is FDA-approved for use in children of all ages, including neonates, for the management of UCDs. In fact, the pediatric population is the primary user of this medication.

• Neonates: Dosing is based on weight (mg/kg). Neonates are at the highest risk for acute ammonia spikes and require the most intensive monitoring.
• Growth Effects: Long-term use of nitrogen scavengers can sometimes lead to growth retardation if the diet is too protein-restricted or if glutamine levels are chronically low. Pediatricians must track height and weight closely on growth charts.
• Taste and Adherence: This is the biggest challenge in children. Using taste-masked pellets or mixing powder with strong-tasting foods is often necessary to ensure the child actually swallows the medication.

There is very little data on the use of Sodium Phenylbutyrate in patients over 65. Because elderly patients are more likely to have decreased renal function and cardiovascular disease (like hypertension or heart failure), they are at much higher risk for complications from the drug's high sodium content. If used in the elderly, doses should start low and kidney function should be checked frequently.

In patients with renal impairment, the clearance of phenylacetylglutamine (the final waste product) is reduced. This can lead to a "backlog" in the metabolic pathway, causing phenylacetate to build up in the blood. Phenylacetate levels above 3.5 mmol/L are associated with neurotoxicity. Patients with a GFR (Glomerular Filtration Rate) below 30 mL/min require significant dose reductions and potentially alternative therapies.

Patients with liver impairment (e.g., cirrhosis) may have difficulty converting phenylbutyrate to its active form. This reduces the drug's effectiveness as a nitrogen scavenger. In these patients, doctors may prefer using Glycerol Phenylbutyrate (Ravicti), which is processed slightly differently, or may increase the frequency of ammonia monitoring to ensure the drug is still working.

> Important: Special populations require individualized medical assessment and frequent laboratory monitoring to balance the risks of the medication against the risks of the underlying urea cycle disorder.

Sodium Phenylbutyrate is a pro-drug that functions as a nitrogen-scavenging agent. Its molecular mechanism involves the following steps:

1. 1Beta-Oxidation: After ingestion, phenylbutyrate undergoes rapid beta-oxidation in the liver and kidneys to form phenylacetate.
2. 2Conjugation: Phenylacetate then conjugates with the amino acid glutamine. This reaction is mediated by the enzyme phenylacetyl-CoA:L-glutamine N-acetyltransferase.
3. 3Excretion: The resulting molecule, phenylacetylglutamine, is a stable compound that contains two nitrogen atoms. It is excreted by the kidneys via glomerular filtration and tubular secretion.

By removing glutamine, the drug removes the nitrogen that would otherwise be converted into toxic ammonia. This provides an alternative to the urea cycle, which is defective in patients with UCDs.

The pharmacodynamic effect of Sodium Phenylbutyrate is the reduction of plasma ammonia and glutamine levels. The onset of action is relatively fast, with nitrogen excretion increasing within hours of the first dose. However, the full therapeutic effect on steady-state ammonia levels may take several days of consistent dosing to achieve. There is no evidence of tolerance development; the drug remains effective as long as it is taken consistently.

| Parameter | Value |

|---|---|

| Bioavailability | High (>80% in fasting state) |

| Protein Binding | 5% to 80% (variable for metabolites) |

| Half-life | Phenylbutyrate: 0.8 hours; Phenylacetate: 1.2 hours |

| Tmax | 1.0 hour (fasting) |

| Metabolism | Hepatic and Renal Beta-oxidation |

| Excretion | Renal (>80% as phenylacetylglutamine) |

• Molecular Formula: C10H11NaO2
• Molecular Weight: 186.18 g/mol
• Solubility: Highly soluble in water; soluble in organic solvents.
• Structure: It is the sodium salt of 4-phenylbutyric acid. It consists of a phenyl ring attached to a four-carbon carboxylic acid chain.

Sodium Phenylbutyrate is classified as an Ammonia Detoxicant or Nitrogen Scavenger. It is part of a small group of drugs used for inborn errors of metabolism. Related medications include:

• Glycerol Phenylbutyrate (Ravicti): A triglyceride form of phenylbutyrate that is liquid and has no taste.
• Sodium Phenylacetate/Sodium Benzoate (Ammonul): An intravenous formulation used for acute hyperammonemia emergencies.