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Propylene Glycol is a synthetic organic compound used as a solvent, humectant, and drug vehicle. Classified as a non-standardized chemical allergen, it plays a critical role in drug delivery and metabolic processes.

Because Propylene Glycol is primarily used as a vehicle or as part of a compound, there is no single 'standard dose' for all patients. Instead, dosage is determined by the specific application:

• For Topical Use (Dermatitis/Dry Skin): Apply a thin layer of the Propylene Glycol-containing cream or lotion to the affected area 2 to 4 times daily, or as directed by your dermatologist.
• For Intravenous Medications: The amount of Propylene Glycol administered is dependent on the dose of the primary drug (e.g., Lorazepam). Healthcare providers monitor the 'Propylene Glycol load,' especially when doses exceed 0.1 mg/kg/hour of the primary medication for prolonged periods.
• For Calculi Dissolution: Specific urological protocols involve irrigation of the bladder or renal pelvis with solutions containing Propylene Glycol, often administered over several days under strict medical supervision.

Extreme caution is required in pediatric dosing. The FDA and the World Health Organization (WHO) have established an Acceptable Daily Intake (ADI) of 25 mg per kilogram of body weight.

• Neonates (Preterm and Term): Propylene Glycol is NOT recommended for use in neonates if an alternative is available. Neonates have an immature alcohol dehydrogenase enzyme system, leading to a half-life that can extend to nearly 17 hours, significantly increasing the risk of 'Gasping Syndrome' and metabolic acidosis.
• Children (1 year and older): Dosing is usually based on the requirements of the primary medication. Pediatricians will calculate the total glycol load to ensure it remains within safe limits.

Renal Impairment

Patients with kidney disease (reduced GFR) require significant monitoring. Since 25% of Propylene Glycol is cleared unchanged by the kidneys, those with renal failure can accumulate the substance rapidly. If the serum creatinine is elevated, healthcare providers may switch to PG-free formulations of IV drugs to prevent lactic acidosis.

Hepatic Impairment

Because the liver metabolizes Propylene Glycol via alcohol dehydrogenase, patients with cirrhosis or liver failure may experience slower clearance. While specific dose-reduction tables do not exist for the excipient itself, clinicians should be aware of the increased risk of CNS depression in these patients.

Elderly Patients

Older adults often have a natural decline in renal function. Dose adjustments for medications containing Propylene Glycol should be conservative, starting at the lower end of the dosing range to avoid accumulation and associated confusion or metabolic imbalances.

• Topical Application: Ensure the skin is clean and dry. Avoid applying to open wounds or severely broken skin unless specifically instructed by a doctor, as this increases systemic absorption.
• Oral Use: If taking an oral liquid containing Propylene Glycol, use a calibrated measuring device (oral syringe or dose cup). Do not use household spoons, which are inaccurate.
• Intravenous Use: This is always performed by a healthcare professional in a clinical setting.
• Storage: Store products containing Propylene Glycol at room temperature (68°F to 77°F). Keep containers tightly closed to prevent evaporation or contamination.

If you are using a topical product and miss a dose, apply it as soon as you remember. If it is almost time for your next application, skip the missed dose. For IV medications administered in a hospital, the clinical staff will manage the schedule. Do not 'double up' on doses to make up for a missed one.

Propylene Glycol overdose is a medical emergency, typically seen in the context of high-dose IV therapy (e.g., long-term sedation in an ICU).

Signs of Overdose include:

• Unexplained metabolic acidosis (high acid levels in the blood)
• Increased serum osmolality (concentrated blood)
• Acute kidney injury (sudden decrease in urine output)
• Severe CNS depression or stupor
• Seizures

In the event of a suspected overdose, the medication must be discontinued immediately. Hemodialysis is highly effective at removing Propylene Glycol from the bloodstream and may be required in severe cases.

> Important: Follow your healthcare provider's dosing instructions. Do not adjust your dose or stop a prescribed medication containing Propylene Glycol without medical guidance.

Most patients tolerate Propylene Glycol well when used in standard amounts. However, the following common side effects may occur, particularly with topical or oral use:

• Skin Irritation: A mild stinging, burning, or redness at the site of application. This usually resolves within minutes as the product dries.
• Dryness: Ironically, in some individuals, excessive use of glycol-based products can lead to a paradoxical drying effect on the skin.
• Mild Nausea: When found in oral syrups, some patients may experience slight stomach upset or a metallic taste in the mouth.

Propylene Glycol is ubiquitous in modern medicine, but it is not without risk. Patients must be aware that while it is 'safe' for the general population, individual tolerance varies significantly. If you have a known allergy to other glycols or alcohols, you must inform your doctor. Furthermore, Propylene Glycol toxicity is a 'hidden' danger in hospital settings because its symptoms often mimic the underlying critical illness (e.g., sepsis or multi-organ failure).

No FDA black box warnings for Propylene Glycol. However, clinicians must strictly adhere to the black box warnings of the primary drugs (like Phenytoin) that utilize Propylene Glycol as a solvent, particularly regarding infusion rates and cardiovascular risks.

• Allergic Reactions / Anaphylaxis Risk: While rare, systemic allergic reactions can occur. Patients with a history of 'idiopathic' (unknown cause) hives or rashes should be screened for Propylene Glycol sensitivity via patch testing.

• Disulfiram (Antabuse): Disulfiram inhibits the enzyme aldehyde dehydrogenase. Since Propylene Glycol is metabolized through this pathway, taking the two together can lead to a 'disulfiram-like reaction.' Symptoms include severe flushing, pounding headache, nausea, vomiting, and chest pain. This combination must be strictly avoided.
• Metronidazole (Flagyl): Similar to disulfiram, metronidazole can interfere with the metabolism of glycols, potentially leading to a toxic accumulation and severe gastrointestinal distress.

• Ethanol (Alcohol): As mentioned, both substances compete for the alcohol dehydrogenase enzyme. This can lead to prolonged half-lives for both alcohol and Propylene Glycol, increasing the risk of CNS depression and lactic acidosis.

Propylene Glycol must NEVER be used in the following circumstances:

1. 1Known Hypersensitivity: Patients with a documented severe allergy (anaphylaxis or severe contact dermatitis) to Propylene Glycol or other glycols (like polyethylene glycol) must avoid all products containing this substance.
2. 2Disulfiram Therapy: Due to the risk of a severe disulfiram-like reaction, Propylene Glycol-containing oral or IV medications are absolutely contraindicated in patients currently taking Antabuse.
3. 3Premature Neonates: The use of Propylene Glycol-containing injections in premature infants is contraindicated due to the high risk of 'Gasping Syndrome' and fatal metabolic complications caused by their immature liver function.

Propylene Glycol is generally classified as FDA Pregnancy Category C. This means that animal reproduction studies have shown an adverse effect on the fetus, or there are no adequate and well-controlled studies in humans. However, the risk is usually associated with very high doses that cause maternal toxicity. In standard pharmaceutical amounts (as an excipient), it is generally considered low-risk. Nevertheless, during the first trimester, it is prudent to minimize exposure to high-dose IV formulations containing this vehicle unless the medical benefit to the mother outweighs the potential risk to the fetus.

Propylene Glycol is known to pass into breast milk, although the amounts absorbed by the nursing infant from maternal use of topical or oral products are likely negligible. The WHO considers it compatible with breastfeeding in standard doses. However, nursing mothers should avoid applying Propylene Glycol-containing creams directly to the nipple area to prevent direct ingestion by the infant, which could cause irritation or sensitization.

As previously noted, Propylene Glycol is of significant concern in the pediatric population. The 'Gasping Syndrome' is a well-documented toxic reaction in neonates, characterized by metabolic acidosis, respiratory distress, and CNS collapse. This occurs because the neonatal liver lacks the mature enzymes required to break down glycols. For children over the age of one, Propylene Glycol is generally safe, but cumulative doses from multiple medications (e.g., a child receiving an IV sedative, an oral antibiotic syrup, and a topical steroid) must be monitored by a pediatric pharmacist.

Propylene Glycol acts as a multi-functional agent. In its role as a Non-Standardized Chemical Allergen, it interacts with skin proteins to form a hapten-protein complex, which is then recognized by Langerhans cells, triggering a T-cell mediated immune response in sensitized individuals.

In its role as a Nitrogen Binding Agent and Acidifying Activity agent, its metabolism is key. The conversion of Propylene Glycol to L-lactic acid increases the hydrogen ion concentration in the extracellular fluid. This acidification can be utilized therapeutically in specific contexts but is more often a side effect of high-dose administration. The Ammonium Ion Binding Activity is a secondary effect of its influence on the renal tubular environment and its role in specific metabolic pathways where it can influence nitrogenous waste excretion.

The pharmacodynamic effects of Propylene Glycol are dose-dependent. At low concentrations, it is inert. At higher concentrations (serum levels > 18-25 mg/dL), it begins to exert osmotic pressure on cells and CNS depressive effects. The duration of effect is closely tied to its metabolic rate; once the alcohol dehydrogenase enzymes are saturated, the duration of action increases exponentially.