Sevelamer Carbonate For Oral Suspension

Sevelamer Carbonate is a non-absorbed phosphate binder used to control serum phosphorus levels in patients with chronic kidney disease (CKD) on dialysis, helping to prevent bone disease and cardiovascular calcification.

The dosage of Sevelamer Carbonate is highly individualized and is based on the patient's current serum phosphorus levels. Healthcare providers typically follow a standardized starting regimen:

• Serum Phosphorus > 5.5 and < 7.5 mg/dL: The recommended starting dose is 800 mg (one tablet or one 0.8 g packet) taken three times daily with meals.
• Serum Phosphorus ≥ 7.5 and < 9.0 mg/dL: The recommended starting dose is 1,600 mg (two 800 mg tablets or two 0.8 g packets) taken three times daily with meals.
• Serum Phosphorus ≥ 9.0 mg/dL: The recommended starting dose is 2,400 mg (three 800 mg tablets or one 2.4 g packet) taken three times daily with meals.

For patients switching from Sevelamer Hydrochloride to Sevelamer Carbonate, the dose is usually transitioned gram-for-gram. For patients switching from calcium-based binders, the dose is titrated based on phosphorus levels.

Sevelamer Carbonate is approved for use in children aged 6 years and older. The dosage is determined by Body Surface Area (BSA):

• BSA ≥ 0.75 to < 1.2 m²: Starting dose is 800 mg three times daily with meals.
• BSA ≥ 1.2 m²: Starting dose is 1,600 mg three times daily with meals.

Titration in children follows the same logic as in adults, with adjustments made every 1-2 weeks until target phosphorus levels are achieved.

Renal Impairment

Since Sevelamer Carbonate is used specifically for patients with severe renal impairment (dialysis), no further dose adjustment is needed based on the degree of kidney failure. However, the dose must be constantly titrated based on the clinical response (serum phosphorus levels).

Hepatic Impairment

Because Sevelamer Carbonate is not absorbed or metabolized by the liver, no dosage adjustments are required for patients with hepatic impairment.

Elderly Patients

Clinical trials did not identify significant differences in safety or efficacy between patients over 65 and younger patients. Dose selection should be cautious, starting at the lower end of the dosing range, reflecting the greater frequency of decreased GI motility in this population.

To achieve maximum efficacy, Sevelamer Carbonate must be taken with meals. It works by binding the phosphorus in the food you are currently eating; taking it on an empty stomach significantly reduces its effectiveness.

• Tablets: Swallow the tablets whole. Do not crush, chew, or break them, as the polymer can expand in the esophagus and cause a choking hazard or irritation.
• Powder: Empty the contents of the packet into a cup and mix with the prescribed amount of water (usually 30 to 60 mL). Stir well and drink immediately. The powder does not dissolve; it forms a suspension. If any residue remains in the glass, add more water, swirl, and drink to ensure the full dose is consumed.
• Storage: Store at room temperature (25°C or 77°F), protected from moisture and heat.

If you miss a dose of Sevelamer Carbonate, skip the missed dose and take your next dose with your next meal. Do not take two doses at once to make up for a missed one. Since the drug only works when food is present in the gut, taking a dose between meals is generally not beneficial.

Because Sevelamer Carbonate is not absorbed, systemic toxicity from an overdose is unlikely. However, taking excessively large amounts may lead to severe constipation or gastrointestinal obstruction. If an overdose is suspected, or if the patient experiences severe abdominal pain or inability to have a bowel movement, contact a poison control center or seek emergency medical attention immediately.

> Important: Follow your healthcare provider's dosing instructions exactly. Do not adjust your dose or stop taking the medication without medical guidance, as this can lead to rapid increases in phosphorus levels.

Because Sevelamer Carbonate acts locally within the digestive tract, the most frequent side effects are gastrointestinal in nature. According to clinical trial data, more than 10% of patients may experience:

• Nausea and Vomiting: This is often most pronounced when starting the medication or during dose increases. Taking the medication exactly as directed with food can help mitigate these symptoms.
• Diarrhea: Some patients report loose stools, which may be related to the way the polymer interacts with the gut flora or bile acids.
• Dyspepsia (Indigestion): A feeling of fullness or burning in the upper abdomen.
• Abdominal Pain: General discomfort or cramping in the stomach area.
• Flatulence (Gas)

Sevelamer Carbonate is a potent medication that requires careful medical supervision. Patients must be aware that this drug is only one part of a comprehensive treatment plan for CKD-MBD, which also includes a low-phosphorus diet and potentially other medications like Vitamin D analogs or calcimimetics.

No FDA black box warnings for Sevelamer Carbonate. However, it is essential to adhere to the safety precautions regarding gastrointestinal health.

• Gastrointestinal Disorders: Sevelamer Carbonate should be used with extreme caution in patients with active gastrointestinal (GI) disease. This includes patients with dysphagia (swallowing disorders), severe GI motility disorders (like severe constipation), or those who have recently had major GI surgery. The polymer can exacerbate these conditions and, in rare cases, lead to bowel perforation.

There are no drugs that are strictly contraindicated for use with Sevelamer Carbonate in the sense of causing a fatal reaction; however, the binding nature of the drug means it can render other life-saving medications completely ineffective if taken at the same time.

• Ciprofloxacin (Cipro): Sevelamer can reduce the bioavailability of ciprofloxacin by approximately 50%. This can lead to treatment failure for serious infections. Ciprofloxacin should be administered at least 2 hours before or 6 hours after Sevelamer.
• Mycophenolate Mofetil (CellCept): In transplant patients, Sevelamer can reduce the absorption of mycophenolate, potentially increasing the risk of organ rejection. These drugs must be separated by at least 2 hours.
• Levothyroxine (Synthroid): Sevelamer can bind to thyroid hormones in the gut, leading to hypothyroidism (underactive thyroid). Thyroid-stimulating hormone (TSH) levels should be monitored closely, and the doses should be separated by several hours.

Sevelamer Carbonate is strictly contraindicated in the following scenarios:

1. 1Bowel Obstruction: Patients with a known or suspected intestinal obstruction must not take Sevelamer Carbonate. Because the medication is a non-digestible polymer that adds bulk to the stool, it can turn a partial obstruction into a complete, life-threatening blockage or cause a bowel rupture.
2. 2Hypersensitivity: Anyone with a documented severe allergic reaction to sevelamer carbonate, sevelamer hydrochloride, or any component of the formulation (such as the film coating or suspension agents) should not use the drug.

Healthcare providers must perform a careful risk-benefit analysis for patients with:

Sevelamer Carbonate is classified as a drug where human data is limited. Because the drug is not absorbed systemically, it is not expected to be directly teratogenic (causing birth defects) to the fetus. However, its secondary effect of binding folic acid and fat-soluble vitamins is a major concern. Folic acid deficiency during pregnancy is a known cause of neural tube defects. If Sevelamer Carbonate is used during pregnancy, aggressive monitoring of vitamin levels and increased supplementation of folic acid are mandatory. The American College of Obstetricians and Gynecologists (ACOG) suggests that maintaining normal phosphorus levels is vital for maternal health, but the risks of nutrient depletion must be balanced.

Sevelamer Carbonate is not absorbed by the mother and therefore cannot be excreted into breast milk. It is generally considered safe for use during breastfeeding. However, the mother should continue to be monitored for vitamin deficiencies to ensure that the nutritional quality of the breast milk remains adequate for the infant.

Sevelamer Carbonate is FDA-approved for children aged 6 years and older. The primary concern in the pediatric population is the impact on growth. Chronic hyperphosphatemia and the resulting bone disease can lead to stunted growth and skeletal deformities. While Sevelamer is effective at lowering phosphorus in children, long-term studies on its impact on bone mineral density in growing children are still ongoing. It is not recommended for children under the age of 6.

Sevelamer Carbonate is a non-absorbed, high-molecular-weight, cross-linked polymer. It contains multiple primary and secondary amines, each separated by one carbon from the polymer backbone. In the physiological environment of the gut, these amines become partially protonated. The resulting positively charged polymer acts as an ion-exchange resin. It binds to the negatively charged phosphate ions (HPO4^2- and H2PO4^-) through a combination of ionic bonding and hydrogen bonding. By binding phosphate in the dietary bolus within the stomach and small intestine, Sevelamer prevents the transport of phosphate across the intestinal epithelium into the blood.

The pharmacodynamic effect of Sevelamer is purely local. The dose-response relationship is well-documented: higher doses of Sevelamer bind more phosphate, up to a saturation point. The onset of effect occurs with the very first meal taken with the medication, although it may take 1-2 weeks of consistent use to see a significant drop in serum phosphorus levels. Sevelamer also exhibits bile-acid sequestering activity, which can lower LDL cholesterol by approximately 15-30%.

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