ered. administer sodium polystyrene sulfonate at least 3 hours before or 3 hours after other oral medications. patients with gastroparesis may require a 6 hour separation. monitor for clinical response and/or blood levels where possible. 7.2 cation-donating antacids the simultaneous oral administration of sodium polystyrene sulfonate with nonabsorbable cation-donating antacids and laxatives may reduce the resin's potassium exchange capability and increase the risk of systemic alkalosis. 7.3 sorbitol sorbitol may contribute to the risk of intestinal necrosis [see warnings and precautions (5.1)] and concomitant use is not recommended.

lure. concomitant administration of sorbitol is not recommended. • use only in patients who have normal bowel function. avoid use in patients who have not had a bowel movement post-surgery. • avoid use in patients who are at risk for developing constipation or impaction (including those with history of impaction, chronic constipation, inflammatory bowel disease, ischemic colitis, vascular intestinal atherosclerosis, previous bowel resection, or bowel obstruction). discontinue use in patients who develop constipation. 5.2 electrolyte disturbances monitor serum potassium during therapy because severe hypokalemia may occur. sodium polystyrene sulfonate is not totally selective for potassium, and small amounts of other cations such as magnesium and calcium can also be lost during treatment. monitor calcium and magnesium in patients receiving sodium polystyrene sulfonate. 5.3 fluid overload in patients sensitive to high sodium intake each 15 g dose of sodium polystyrene sulfonate contains 1500 mg (60 meq) of sodium. monitor patients who are sensitive to sodium intake (heart failure, hypertension, edema) for signs of fluid overload. adjustment of other sources of sodium may be required. 5.4 risk of aspiration cases of acute bronchitis or bronchopneumonia caused by inhalation of sodium polystyrene sulfonate particles have been reported. patients with impaired gag reflex, altered level of consciousness, or patients prone to regurgitation may be at increased risk. administer sodium polystyrene sulfonate with the patient in an upright position. 5.5 binding to other orally administered medications sodium polystyrene sulfonate may bind orally administered medications, which could decrease their gastrointestinal absorption and lead to reduced efficacy. administer other oral medications at least 3 hours before or 3 hours after sodium polystyrene sulfonate. patients with gastroparesis may require a 6 hour separation [see dosage and administration (2.1) and drug interactions (7)] .

lter the exchange properties of the resin. one level teaspoon contains approximately 3.5 g of sodium polystyrene sulfonate and 15 meq of sodium. oral suspension suspend each dose in a small quantity of water or syrup, approximately 3 to 4 ml of liquid per gram of resin. administer with patient in an upright position [see warnings and precautions (5.4)] . enema after an initial cleansing enema, insert a soft, large size (french 28) rubber tube into the rectum for a distance of about 20 cm, with the tip well into the sigmoid colon, and tape in place. administer as a warm (body temperature) emulsion in 100 ml of aqueous vehicle and flush with 50 to 100 ml of fluid. a somewhat thicker suspension may be used, but do not form a paste. agitate the emulsion gently during administration. the resin should be retained for as long as possible and follow by a cleansing enema with a nonsodium containing solution. ensure an adequate volume of cleansing solution (up to 2 liters) is utilized.

), ischemic colitis, nausea, vomiting. to report suspected adverse reactions, contact kvk-tech, inc. at 1-215-579-1842 or fda at 1-800-fda-1088 or www.fda.gov/medwatch .

ered. administer sodium polystyrene sulfonate at least 3 hours before or 3 hours after other oral medications. patients with gastroparesis may require a 6 hour separation. monitor for clinical response and/or blood levels where possible. 7.2 cation-donating antacids the simultaneous oral administration of sodium polystyrene sulfonate with nonabsorbable cation-donating antacids and laxatives may reduce the resin's potassium exchange capability and increase the risk of systemic alkalosis. 7.3 sorbitol sorbitol may contribute to the risk of intestinal necrosis [see warnings and precautions (5.1)] and concomitant use is not recommended.

precautions (5.4)] .

ys. 12.3 pharmacokinetics the in vivo efficiency of sodium-potassium exchange resins is approximately 33 percent; hence, about one third of the resin's actual sodium content is delivered to the body. sodium polystyrene sulfonate is not absorbed systemically. drug interactions in vitro binding studies showed that sodium polystyrene sulfonate bound significantly to the following tested drugs – warfarin, metoprolol, phenytoin, furosemide, amlodipine and amoxicillin.