Sucralfate is an oral gastrointestinal drug. Chemically, it is a sucrose sulfate complex. Sucralfate is indicated for the short term (up to 8 week) treatment of active duodenal ulcers and is also used as maintenance therapy following resolution of a duodenal ulcer. The efficacy of sucralfate in the treatment of gastric ulcers is comparable to cimetidine. It has been used in the relief of GI symptoms occurring with NSAIDs, although in one study, sucralfate was significantly less effective than misoprostol. Other uses for sucralfate include treatment of gastroesophageal reflux disease (GERD) as well as prophylaxis and treatment of stress-induced mucosal damage. Sucralfate was approved by the FDA in 1981.
General Administration Information
For storage information, see the specific product information within the How Supplied section.
Route-Specific Administration
Oral Administration
-Take on an empty stomach at least 1 hour prior to a meal and at bedtime.
-Antacids may be prescribed as needed for relief of pain but should not be taken within one-half hour before or after a sucralfate dose.
Oral Solid Formulations
Tablets
-The sucralfate tablet is scored and may be cut into two pieces for ease of administration.
Oral Liquid Formulations
Sucralfate oral suspension
-for oral administration only. Fatal complications, including pulmonary and cerebral emboli, have occurred with the inadvertent intravenous administration of sucralfate suspension.
-Shake well prior to each administration; measure the dosage with a calibrated oral measuring device.
-For enteral tube administration, flush the tube with 30 mL of water (adults) before and after administering the drug.
Extemporaneous Compounding-Oral
Extemporaneous instructions for a single 1-gram dose of Sucralfate slurry:
NOTE: This preparation is not approved by the FDA, but has been described in the medical literature.
-For patients with difficulty swallowing whole or halved sucralfate tablets, a slurry may be prepared just prior to administration by placing a 1 gram tablet in a 30 mL medicine cup without crushing and adding 15 mL to 30 mL of water, preferably warm water but room temperature is adequate.
-Within 30 seconds the sucralfate will dissolve into a suspension on its own. This will not work with other compounds such as sorbitol, but they may be added to the suspension if desired later.
-Do not prepare the dose ahead of the time it is to be administered; stability information is not available.
Rectal Administration
-Marketed formulations are not available in the U.S. While doses have been characterized in literature reports, extemporaneous formulations for those doses have not been standardized. Water, or 5% or 10% methylcellulose solutions, have been used as diluents for the oral tablets for compounding the dosages reported. Stability data and expiration date recommendations are generally not available for these extemporaneous enemas.
-One article reports a case of rectal administration of the commercially available 10% sucralfate oral suspension to deliver a 2 g/20 mL dosage rectally twice daily; however, the effect of formulation excipients on the rectal mucosal or with regard to safety, efficacy, or tolerability are not known.
-Another article reported an extemporaneous formula for 10% sucralfate rectal enema as follows: Crush one-hundred-twenty (120) sucralfate 1-g tablets to a fine powder using a large mortar and pestle. Add the powder to 300 mL of 10% methylcellulose solution, mixing well. This will form a paste until the rest of the methylcellulose is added and it is important to allow this phase to occur to establish 'high-shear' forces that will allow the powder to be well distributed when the enema suspension is finished. Then, add more methylcellulose to make a final volume of 1200 mL. Package in disposable enema bottles or rectal syringes in 2 g/20 mL packages. Label with 'refrigerate', 'shake well', and 'protect from light'. Because stability data are not available, the author recommended no longer than a 2-week expiration date.
Sucralfate is well tolerated, with few adverse effects reported. Constipation is the most frequent adverse effect, occurring in 2% of patients. Case reports of esophageal or intestinal bezoar formation in critically ill infants, children, and adults receiving sucralfate slurries and suspensions have been published, and have been complicated by risk factors including the presence of dehydration and impaired gastric motility, and multiple medications administered along with enteral feedings via various types of enteral feeding tubes.
Adverse effects reported in fewer than 0.5% of patients taking sucralfate include diarrhea, nausea/vomiting, gastric discomfort, indigestion, flatulence, dry mouth (xerostomia), rash (unspecified), pruritus, headache, dizziness, back pain, drowsiness, and vertigo. These events rarely require discontinuation of sucralfate. In addition, cases of hypersensitivity have been reported with the use of sucralfate suspension, including anaphylactoid reactions, angioedema, dyspnea, lip swelling, edema of the mouth, pharyngeal edema, pruritus, rash, and urticaria.
Small amounts of aluminum can be absorbed following oral administration of sucralfate. This agent should not be given concomitantly with other agents containing aluminum (e.g., aluminum-containing antacids) because the total body burden of aluminum can increase. Patients with renal failure or those receiving dialysis can develop aluminum toxicity with sucralfate therapy, due to impaired aluminum excretion. The systemic burden of aluminum with chronic sucralfate therapy is similar to that present with the use of aluminum-containing antacids. Aluminum intoxication in the form of aluminum osteodystrophy, osteomalacia, or encephalopathy has been described in dialysis patients. There is concern that hypophosphatemia may occur in patients on chronic sucralfate therapy.
Cases of hyperglycemia have been reported in diabetic patients treated with sucralfate suspension. Close monitoring of blood sugar is recommended; antidiabetic therapy may need adjustment during concomitant treatment with sucralfate suspension.
Sucralfate can interfere with the absorption of other medications if administered concomitantly (see Drug Interactions).
Sucralfate should be used with caution in patients with chronic renal failure or on dialysis. When sucralfate is administered orally, small amounts of aluminum are absorbed from the gastrointestinal tract. Concomitant use of sucralfate with other products that contain aluminum, such as aluminum-containing antacids, may increase the total body burden of aluminum. Patients with normal renal function receiving the recommended doses of sucralfate and aluminum- containing products adequately excrete aluminum in the urine. Patients with chronic renal failure or those receiving dialysis have impaired excretion of absorbed aluminum. In addition, aluminum does not cross dialysis membranes because it is bound to albumin and transferrin plasma proteins. Aluminum accumulation and toxicity (aluminum osteodystrophy, osteomalacia, encephalopathy) have been described in patients with renal impairment.
Use sucralfate oral suspension with caution in those with diabetes mellitus as cases of hyperglycemia have been reported during treatment with this product. Close monitoring of blood sugar is recommended; adjust antidiabetic treatment as clinically indicated.
Isolated reports of sucralfate tablet aspiration with accompanying respiratory complications have been received. Use sucralfate tablets with caution in patients with known conditions that may impair swallowing, such as recent or prolonged intubation, tracheostomy, prior history of aspiration, dysphagia, or other conditions that may alter gag and cough reflexes (e.g., conditions causing gag reflex depression) or diminish oropharyngeal coordination or motility.
Teratogenicity studies have been performed in mice, rats, and rabbits at doses up to 50 times the human dose and have revealed no evidence of harm to the fetus due to sucralfate. However, because animal studies are not always indicative of human response, use sucralfate during pregnancy only when clearly needed. Guidelines generally consider sucralfate safe to use during gestation in pregnant patients with normal renal function, due to the local rather than systemic action of the drug and the available clinical data. Epidemiologic evidence, including evidence from a prospective, randomized controlled trial, suggests a lack of association of sucralfate with congenital events.
Only small portions of sucralfate are absorbed systemically, and therefore virtually no excretion is expected into breast milk. According to guidelines, if heartburn/gastroesophageal reflux (GERD) symptoms persist after delivery, antacids and sucralfate are safe to use during lactation and breast-feeding because they are not concentrated in breast milk.
Sucralfate suspension is for oral administration only. Fatal complications, including pulmonary and cerebral emboli, have occurred with the inadvertent intravenous administration of sucralfate suspension. Do not administer sucralfate suspension intravenously.
For the treatment of duodenal ulcer not related to NSAID use:
-for active disease:
Oral dosage:
Adults: 1 g PO four times per day, given 1 hour before meals and at bedtime for 4-8 weeks or less if healing has been effectively demonstrated.
Children: Safety and efficacy have not been established. 40-80 mg/kg/day PO divided every 6 hours has been suggested.
-for maintenance therapy of duodenal ulcer:
Oral dosage (tablets only):
Adults: 1 g PO two times per day on an empty stomach.
Children: Safety and efficacy have not been established.
For the treatment of gastric ulcer* not related to NSAID use or for treatment of esophagitis* associated with gastroesophageal reflux disease (GERD)*:
Oral dosage:
Adults: 1 g PO four times per day given one hour before meals and at bedtime.
Children: Safety and efficacy have not been established. 500 mg PO four times per day given one hour before meals and at bedtime has been suggested.
For NSAID-induced ulcer prophylaxis*:
Oral dosage:
Adults: 1 g PO 4 times daily. Several studies have evaluated sucralfate as an agent to prevent NSAID-induced ulcers. In a small study of healthy males, sucralfate 1 g PO four times per day was superior to placebo in preventing gastric injury due to aspirin. Endoscopy was not used in this study. However, some clinicians feel that sucralfate has no place in the prevention or therapy of NSAID-induced gastric ulcer and does not appear to prevent NSAID-associated duodenal ulcer. In a comparison with misoprostol to prevent the development of NSAID-induced gastric ulcer in patients during 3 months of continuous NSAID administration, the incidence of gastric ulcer was 1.6% in the misoprostol group and 16% in the sucralfate group. The sucralfate dose in this study was 1 g PO four times per day given one hour before meals and at bedtime.
For stress gastritis prophylaxis* in critically ill patients:
Oral dosage:
Adults: 1 g PO 4 times daily.
For the palliative treatment of aphthous ulcer*, or for the palliative treatment of stomatitis* due to chemotherapy or radiation therapy:
Oral rinse dosage (sucralfate suspension):
Adults: 5-10 ml (500 mg to 1 g) PO swished in the mouth for several minutes and spit or swallowed, four times per day. Retain in the mouth for several minutes while swishing to insure contact time with affected oral mucosal surfaces.
Children: Safety and efficacy have not been established.
For the alternative treatment of proctitis* due to ulcerative colitis or radiation injury:
Rectal dosage (rectal suspension retention enema, commercial dosage form not available in U.S):
Adults: Doses range from 2-4 g per 15-20 ml (3 g/15 ml is a common dosage for radiation proctitis) PR once or twice daily or as 20 g/100 ml PR once or twice daily (for ulcerative proctosigmoiditis) in literature reports. Prophylactic use (rectally or orally) to prevent radiation injury does not appear to be effective. Extemporaneous compounds vary and have not been adequately characterized for stability or other attributes (see Administration). One case report described using the commercially available oral suspension to deliver a 2 g/20 ml dosage PR twice daily ; however, the effect of formulation excipients on the rectal mucosal or in regard to safety, efficacy, or tolerability are not known.
Maximum Dosage Limits:
-Adults
4 g/day PO.
-Elderly
4 g/day PO.
-Adolescents
4 g/day PO.
-Children
Maximum dosage not established. 80 mg/kg/day PO or alternatively, up to 2000 mg/day PO has been suggested for most indications.
Patients with Hepatic Impairment Dosing
Specific guidelines for dosage adjustments in hepatic impairment are not available; it appears that no dosage adjustments are needed.
Patients with Renal Impairment Dosing
CrCl > 30 ml/min: Specific guidelines for dosage adjustments in renal impairment are not available; it appears that no dosage adjustments are needed.
CrCl <= 30 ml/min: Sucralfate contains aluminum; systemically absorbed in small amounts. Patients with renal failure can develop aluminum accumulation due to impaired aluminum excretion. Use with caution in patients with renal failure.
Intermittent hemodialysis
Sucralfate contains aluminum, which may be systemically absorbed in small amounts. Aluminum does not cross dialysis membranes because of high plasma protein binding, and may accumulate in patients on dialysis.
*non-FDA-approved indication
Abacavir; Dolutegravir; Lamivudine: (Moderate) Administer dolutegravir 2 hours before or 6 hours after taking sucralfate. The chemical structure of sucralfate contains aluminum, which can bind dolutegravir in the GI tract. Taking these drugs simultaneously may result in reduced bioavailability of dolutegravir.
Alendronate: (Moderate) Concomitant administration of oral alendronate with aluminum-containing medications (e.g., sucralfate) may interfere with the absorption of alendronate. Separation of administration is advised. At least 30 minutes should elapse after an alendronate dose before taking aluminum-containing drugs.
Alendronate; Cholecalciferol: (Moderate) Concomitant administration of oral alendronate with aluminum-containing medications (e.g., sucralfate) may interfere with the absorption of alendronate. Separation of administration is advised. At least 30 minutes should elapse after an alendronate dose before taking aluminum-containing drugs.
Aluminum Hydroxide: (Moderate) Antacids can interfere with the binding capacity of sucralfate to the GI mucosa, decreasing its effectiveness. Antacids should not be administered within 30 minutes of sucralfate. In addition, antacids or other aluminum-containing agents should be used cautiously with sucralfate in patients with chronic renal failure due to the aluminum content of sucralfate and the potential for aluminum toxicity.
Aluminum Hydroxide; Magnesium Carbonate: (Moderate) Antacids can interfere with the binding capacity of sucralfate to the GI mucosa, decreasing its effectiveness. Antacids should not be administered within 30 minutes of sucralfate. In addition, antacids or other aluminum-containing agents should be used cautiously with sucralfate in patients with chronic renal failure due to the aluminum content of sucralfate and the potential for aluminum toxicity.
Aluminum Hydroxide; Magnesium Hydroxide: (Moderate) Antacids can interfere with the binding capacity of sucralfate to the GI mucosa, decreasing its effectiveness. Antacids should not be administered within 30 minutes of sucralfate. In addition, antacids or other aluminum-containing agents should be used cautiously with sucralfate in patients with chronic renal failure due to the aluminum content of sucralfate and the potential for aluminum toxicity.
Aluminum Hydroxide; Magnesium Hydroxide; Simethicone: (Moderate) Antacids can interfere with the binding capacity of sucralfate to the GI mucosa, decreasing its effectiveness. Antacids should not be administered within 30 minutes of sucralfate. In addition, antacids or other aluminum-containing agents should be used cautiously with sucralfate in patients with chronic renal failure due to the aluminum content of sucralfate and the potential for aluminum toxicity.
Aluminum Hydroxide; Magnesium Trisilicate: (Moderate) Antacids can interfere with the binding capacity of sucralfate to the GI mucosa, decreasing its effectiveness. Antacids should not be administered within 30 minutes of sucralfate. In addition, antacids or other aluminum-containing agents should be used cautiously with sucralfate in patients with chronic renal failure due to the aluminum content of sucralfate and the potential for aluminum toxicity.
Amoxicillin; Clarithromycin; Omeprazole: (Minor) Proton pump inhibitors should be taken at least 30 minutes prior to sucralfate. Sucralfate has been shown to delay absorption and reduce the bioavailability of omeprazole by about 16%.
Antacids: (Moderate) Antacids can interfere with the binding capacity of sucralfate to the GI mucosa, decreasing its effectiveness. Antacids should not be administered within 30 minutes of sucralfate. In addition, antacids or other aluminum-containing agents should be used cautiously with sucralfate in patients with chronic renal failure due to the aluminum content of sucralfate and the potential for aluminum toxicity.
Aspirin, ASA; Citric Acid; Sodium Bicarbonate: (Major) Antacids can interfere with the binding capacity of sucralfate to the GI mucosa, decreasing its effectiveness. Antacids should not be administered within 30 minutes of sucralfate.
Aspirin, ASA; Omeprazole: (Minor) Proton pump inhibitors should be taken at least 30 minutes prior to sucralfate. Sucralfate has been shown to delay absorption and reduce the bioavailability of omeprazole by about 16%.
Bictegravir; Emtricitabine; Tenofovir Alafenamide: (Moderate) Concomitant administration of bictegravir and sucralfate may result in decreased bictegravir plasma concentrations. The chemical structure of sucralfate contains aluminum, which can bind bictegravir in the GI tract, resulting in reduced bioavailability of bictegravir. Caution and close monitoring are advised if these drugs are used together.
Bismuth Subcitrate Potassium; Metronidazole; Tetracycline: (Moderate) Sucralfate should be given 2 hours before or after the oral administration of tetracyclines. Divalent or trivalent cations readily chelate with tetracycline antibiotics, forming insoluble compounds. The oral absorption of these antibiotics will be significantly reduced by other orally administered compounds that contain aluminum salts, calcium salts, iron salts, magnesium salts, and/or zinc salts. Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with tetracyclines in the GI tract, reducing the bioavailability of these agents.
Bismuth Subsalicylate; Metronidazole; Tetracycline: (Moderate) Sucralfate should be given 2 hours before or after the oral administration of tetracyclines. Divalent or trivalent cations readily chelate with tetracycline antibiotics, forming insoluble compounds. The oral absorption of these antibiotics will be significantly reduced by other orally administered compounds that contain aluminum salts, calcium salts, iron salts, magnesium salts, and/or zinc salts. Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with tetracyclines in the GI tract, reducing the bioavailability of these agents.
Calcium Acetate: (Moderate) Oral antacids, including calcium salts, potentially interfere with gastric mucosal binding of sucralfate. This interaction can be minimized by staggering the doses of these agents as much as possible.
Calcium Carbonate: (Moderate) Oral antacids, including calcium carbonate, potentially interfere with gastric mucosal binding of sucralfate. This interaction can be minimized by staggering the doses of these agents as much as possible.
Calcium Carbonate; Famotidine; Magnesium Hydroxide: (Moderate) Oral antacids, including calcium carbonate, potentially interfere with gastric mucosal binding of sucralfate. This interaction can be minimized by staggering the doses of these agents as much as possible.
Calcium Carbonate; Magnesium Hydroxide: (Moderate) Oral antacids, including calcium carbonate, potentially interfere with gastric mucosal binding of sucralfate. This interaction can be minimized by staggering the doses of these agents as much as possible.
Calcium Carbonate; Magnesium Hydroxide; Simethicone: (Moderate) Oral antacids, including calcium carbonate, potentially interfere with gastric mucosal binding of sucralfate. This interaction can be minimized by staggering the doses of these agents as much as possible.
Calcium Carbonate; Simethicone: (Moderate) Oral antacids, including calcium carbonate, potentially interfere with gastric mucosal binding of sucralfate. This interaction can be minimized by staggering the doses of these agents as much as possible.
Calcium Chloride: (Moderate) Calcium salts potentially interfere with gastric mucosal binding of sucralfate. This interaction can be minimized by staggering the doses of these agents as much as possible.
Calcium Gluconate: (Moderate) Oral antacids, including calcium salts, potentially interfere with gastric mucosal binding of sucralfate. This interaction can be minimized by staggering the doses of these agents as much as possible.
Calcium; Vitamin D: (Moderate) Oral antacids, including calcium carbonate, potentially interfere with gastric mucosal binding of sucralfate. This interaction can be minimized by staggering the doses of these agents as much as possible.
Ciprofloxacin: (Moderate) Administer oral ciprofloxacin at least 2 hours before or 6 hours after sucralfate. Ciprofloxacin absorption may be reduced as quinolone antibiotics can chelate with sucralfate. This interaction appears to be the result of chelation by the aluminum content of sucralfate.
Delafloxacin: (Major) Administer oral delafloxacin at least 2 hours before or 6 hours after sucralfate. Delafloxacin absorption may be reduced as quinolone antibiotics can chelate with sucralfate. This interaction appears to be the result of chelation by the aluminum content of sucralfate.
Demeclocycline: (Moderate) Sucralfate should be given 2 hours before or after the oral administration of tetracyclines. Divalent or trivalent cations readily chelate with tetracycline antibiotics, forming insoluble compounds. The oral absorption of these antibiotics will be significantly reduced by other orally administered compounds that contain aluminum salts, calcium salts, iron salts, magnesium salts, and/or zinc salts. Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with tetracyclines in the GI tract, reducing the bioavailability of these agents.
Dexlansoprazole: (Moderate) Sucralfate has been shown to delay the absorption and reduce the bioavailability of oral lansoprazole by about 17%. Dexlansoprazole should be taken no less than 30 minutes before sucralfate if these drugs are to be used concomitantly. Concurrent administration of oral dexlansoprazole and antacids may reduce the bioavailability of dexlansoprazole; except when the antacids are given at least 30 minutes to one hour before dexlansoprazole administration.
Digoxin: (Moderate) Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with digoxin in the GI tract, reducing its bioavailability. Sucralfate should be given 2 hours before or after the oral administration of digoxin. In addition, the manufacturer of digoxin recommends measuring serum digoxin concentrations prior to initiation of sucralfate. Continue monitoring during concomitant treatment and increase the digoxin dose by 20 to 40% as necessary.
Diphenhydramine; Naproxen: (Moderate) Separate sucralfate and naproxen administration by at least 2 hours. Concomitant administration of sucralfate and enteric-coated or delayed-release naproxen tablets can delay the absorption of naproxen.
Dolutegravir: (Moderate) Administer dolutegravir 2 hours before or 6 hours after taking sucralfate. The chemical structure of sucralfate contains aluminum, which can bind dolutegravir in the GI tract. Taking these drugs simultaneously may result in reduced bioavailability of dolutegravir.
Dolutegravir; Lamivudine: (Moderate) Administer dolutegravir 2 hours before or 6 hours after taking sucralfate. The chemical structure of sucralfate contains aluminum, which can bind dolutegravir in the GI tract. Taking these drugs simultaneously may result in reduced bioavailability of dolutegravir.
Dolutegravir; Rilpivirine: (Moderate) Administer dolutegravir 2 hours before or 6 hours after taking sucralfate. The chemical structure of sucralfate contains aluminum, which can bind dolutegravir in the GI tract. Taking these drugs simultaneously may result in reduced bioavailability of dolutegravir.
Doxycycline: (Moderate) Sucralfate should be given 2 hours before or after the oral administration of tetracyclines. Divalent or trivalent cations readily chelate with tetracycline antibiotics, forming insoluble compounds. The oral absorption of these antibiotics will be significantly reduced by other orally administered compounds that contain aluminum salts, calcium salts, iron salts, magnesium salts, and/or zinc salts. Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with tetracyclines in the GI tract, reducing the bioavailability of these agents.
Elvitegravir; Cobicistat; Emtricitabine; Tenofovir Alafenamide: (Moderate) Separate administration of elvitegravir and sucralfate by at least 2 hours. Due to the formation of ionic complexes in the gastrointestinal tract, simultaneous administration results in lower elvitegravir plasma concentrations.
Elvitegravir; Cobicistat; Emtricitabine; Tenofovir Disoproxil Fumarate: (Moderate) Separate administration of elvitegravir and sucralfate by at least 2 hours. Due to the formation of ionic complexes in the gastrointestinal tract, simultaneous administration results in lower elvitegravir plasma concentrations.
Enteral Feedings: (Minor) The risk of bezoar formation may be increased when sucralfate is combined with enteral feedings; additionally, continuous enteral feedings have been reported to interfere with the therapeutic efficacy of sucralfate for selected indications. When sucralfate is given via a feeding tube, careful attention to proper administration technique is recommended. In patients receiving continuous enteral feedings, the selection of an alternative agent to sucralfate may be warranted.
Esomeprazole: (Minor) Sucralfate may delay absorption and reduce the bioavailability of lansoprazole. Lansoprazole should be taken no less than 30 minutes before sucralfate. This interaction is theoretical and is based on the interaction between sucralfate and lansoprazole; sucralfate has been shown to delay absorption and reduce the bioavailability of lansoprazole by about 17%. No information is available to determine if a similar interaction occurs with esomeprazole.
Ethotoin: (Major) The oral absorption of ethotoin may be reduced by sucralfate. Although the magnitude of this interactions is not great, an occasional patient may be affected and the interaction may lead to subtherapeutic ethotoin concentrations. Sucralfate should be given 2 hours before or after the ethotoin.
Furosemide: (Moderate) Separate the administration of oral furosemide and sucralfate by at least 2 hours. Simultaneous coadministration may reduce furosemide efficacy.
Gemifloxacin: (Major) Administer sucralfate at least 3 hours before or 2 hours after gemifloxacin. Gemifloxacin absorption may be reduced as quinolone antibiotics can chelate with sucralfate. This interaction appears to be the result of chelation by the aluminum content of sucralfate.
Ibritumomab Tiuxetan: (Moderate) Serum phosphorus should be checked routinely in patients treated chronically with sucralfate; sucralfate may cause hypophosphatemia and some patients may require phosphorus repletion. This nutrient interaction should be considered in patients receiving phosphates for dietary supplementation. It appears that sucralfate chelates phosphorus in the gut, forming nonabsorbable complexes. Because of sucralfate's therapeutic effect, this interaction may not be prevented by separating times of oral administration.
Ketoconazole: (Moderate) Avoid use of sucralfate with ketoconazole. If concomitant use is necessary, separate administration of ketoconazole and sucralfate by at least 2 hours. Sucralfate is expected to impair ketoconazole absorption. Coadministration of sucralfate decreased ketoconazole bioavailability by approximately 20%.
Lansoprazole: (Moderate) Sucralfate has been shown to delay absorption and reduce the bioavailability of lansoprazole by about 17%. Lansoprazole should be taken no less than 30 minutes before sucralfate if these drugs are to be used concomitantly.
Lansoprazole; Amoxicillin; Clarithromycin: (Moderate) Sucralfate has been shown to delay absorption and reduce the bioavailability of lansoprazole by about 17%. Lansoprazole should be taken no less than 30 minutes before sucralfate if these drugs are to be used concomitantly.
Lanthanum Carbonate: (Major) Oral compounds known to interact with antacids, like sucralfate, should not be taken within 2 hours of dosing with lanthanum carbonate. If these agents are used concomitantly, space the dosing intervals appropriately. Monitor serum concentrations and clinical condition.
Levofloxacin: (Moderate) Administer sucralfate at least 2 hours before or 2 hours after orally administered levofloxacin. Levofloxacin absorption may be reduced as quinolone antibiotics can chelate with sucralfate. This interaction appears to be the result of chelation by the aluminum content of sucralfate. Chelation of divalent cations with levofloxacin is less than with other quinolones.
Levoketoconazole: (Moderate) Avoid use of sucralfate with ketoconazole. If concomitant use is necessary, separate administration of ketoconazole and sucralfate by at least 2 hours. Sucralfate is expected to impair ketoconazole absorption. Coadministration of sucralfate decreased ketoconazole bioavailability by approximately 20%.
Levothyroxine: (Moderate) Administer levothyroxine at least 4 hours apart from a dose of sucralfate. Patients treated concomitantly with these drugs should be monitored for changes in thyroid function. Consider an alternative to sucralfate, if appropriate. Concurrent use of sucralfate may reduce the efficacy of levothyroxine and other thyroid hormones by binding and delaying or preventing oral absorption, potentially resulting in hypothyroidism.
Levothyroxine; Liothyronine (Porcine): (Moderate) Administer levothyroxine at least 4 hours apart from a dose of sucralfate. Patients treated concomitantly with these drugs should be monitored for changes in thyroid function. Consider an alternative to sucralfate, if appropriate. Concurrent use of sucralfate may reduce the efficacy of levothyroxine and other thyroid hormones by binding and delaying or preventing oral absorption, potentially resulting in hypothyroidism.
Levothyroxine; Liothyronine (Synthetic): (Moderate) Administer levothyroxine at least 4 hours apart from a dose of sucralfate. Patients treated concomitantly with these drugs should be monitored for changes in thyroid function. Consider an alternative to sucralfate, if appropriate. Concurrent use of sucralfate may reduce the efficacy of levothyroxine and other thyroid hormones by binding and delaying or preventing oral absorption, potentially resulting in hypothyroidism.
Liothyronine: (Moderate) Administer levothyroxine at least 4 hours apart from a dose of sucralfate. Patients treated concomitantly with these drugs should be monitored for changes in thyroid function. Consider an alternative to sucralfate, if appropriate. Concurrent use of sucralfate may reduce the efficacy of levothyroxine and other thyroid hormones by binding and delaying or preventing oral absorption, potentially resulting in hypothyroidism.
Magnesium Hydroxide: (Moderate) Antacids can interfere with the binding capacity of sucralfate to the GI mucosa, decreasing its effectiveness. Antacids should not be administered within 30 minutes of sucralfate. In addition, antacids or other aluminum-containing agents should be used cautiously with sucralfate in patients with chronic renal failure due to the aluminum content of sucralfate and the potential for aluminum toxicity.
Magnesium Salts: (Moderate) Antacids can interfere with the binding capacity of sucralfate to the GI mucosa, decreasing its effectiveness. Antacids should not be administered within 30 minutes of sucralfate. In addition, antacids or other aluminum-containing agents should be used cautiously with sucralfate in patients with chronic renal failure due to the aluminum content of sucralfate and the potential for aluminum toxicity.
Minocycline: (Moderate) Sucralfate should be given 2 hours before or after the oral administration of tetracyclines. Divalent or trivalent cations readily chelate with tetracycline antibiotics, forming insoluble compounds. The oral absorption of these antibiotics will be significantly reduced by other orally administered compounds that contain aluminum salts, calcium salts, iron salts, magnesium salts, and/or zinc salts. Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with tetracyclines in the GI tract, reducing the bioavailability of these agents.
Moxifloxacin: (Major) Administer oral moxifloxacin at least 4 hours before or 8 hours after sucralfate. Moxifloxacin absorption may be reduced as quinolone antibiotics can chelate with sucralfate. This interaction appears to be the result of chelation by the aluminum content of sucralfate.
Naproxen: (Moderate) Separate sucralfate and naproxen administration by at least 2 hours. Concomitant administration of sucralfate and enteric-coated or delayed-release naproxen tablets can delay the absorption of naproxen.
Naproxen; Esomeprazole: (Moderate) Separate sucralfate and naproxen administration by at least 2 hours. Concomitant administration of sucralfate and enteric-coated or delayed-release naproxen tablets can delay the absorption of naproxen. (Minor) Sucralfate may delay absorption and reduce the bioavailability of lansoprazole. Lansoprazole should be taken no less than 30 minutes before sucralfate. This interaction is theoretical and is based on the interaction between sucralfate and lansoprazole; sucralfate has been shown to delay absorption and reduce the bioavailability of lansoprazole by about 17%. No information is available to determine if a similar interaction occurs with esomeprazole.
Naproxen; Pseudoephedrine: (Moderate) Separate sucralfate and naproxen administration by at least 2 hours. Concomitant administration of sucralfate and enteric-coated or delayed-release naproxen tablets can delay the absorption of naproxen.
Ofloxacin: (Moderate) Administer sucralfate at least 2 hours before or 2 hours after ofloxacin. Ofloxacin absorption may be reduced as quinolone antibiotics can chelate with sucralfate. This interaction appears to be the result of chelation by the aluminum content of sucralfate.
Omadacycline: (Moderate) Sucralfate should be given 2 hours before or after the oral administration of tetracyclines. Divalent or trivalent cations readily chelate with tetracycline antibiotics, forming insoluble compounds. The oral absorption of these antibiotics will be significantly reduced by other orally administered compounds that contain aluminum salts, calcium salts, iron salts, magnesium salts, and/or zinc salts. Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with tetracyclines in the GI tract, reducing the bioavailability of these agents.
Omeprazole: (Minor) Proton pump inhibitors should be taken at least 30 minutes prior to sucralfate. Sucralfate has been shown to delay absorption and reduce the bioavailability of omeprazole by about 16%.
Omeprazole; Amoxicillin; Rifabutin: (Minor) Proton pump inhibitors should be taken at least 30 minutes prior to sucralfate. Sucralfate has been shown to delay absorption and reduce the bioavailability of omeprazole by about 16%.
Omeprazole; Sodium Bicarbonate: (Major) Antacids can interfere with the binding capacity of sucralfate to the GI mucosa, decreasing its effectiveness. Antacids should not be administered within 30 minutes of sucralfate. (Minor) Proton pump inhibitors should be taken at least 30 minutes prior to sucralfate. Sucralfate has been shown to delay absorption and reduce the bioavailability of omeprazole by about 16%.
Phenytoin: (Moderate) Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with certain drugs in the GI tract, including phenytoin, reducing the bioavailability of these agents. Sucralfate should be given 2 hours before or after the oral administration of these agents. Be alert to altered clinical response to phenytoin and monitor blood concentrations as clinically indicated.
Phosphorated Carbohydrate Solution: (Moderate) Serum phosphorus should be checked routinely in patients treated chronically with sucralfate; sucralfate may cause hypophosphatemia and some patients may require phosphorus repletion. This nutrient interaction should be considered in patients receiving phosphates for dietary supplementation. It appears that sucralfate chelates phosphorus in the gut, forming nonabsorbable complexes. Because of sucralfate's therapeutic effect, this interaction may not be prevented by separating times of oral administration.
Phosphorus: (Moderate) Serum phosphorus should be checked routinely in patients treated chronically with sucralfate; sucralfate may cause hypophosphatemia and some patients may require phosphorus repletion. This nutrient interaction should be considered in patients receiving phosphates for dietary supplementation. It appears that sucralfate chelates phosphorus in the gut, forming nonabsorbable complexes. Because of sucralfate's therapeutic effect, this interaction may not be prevented by separating times of oral administration.
Posaconazole: (Major) The manufacturer suggests drugs that increase gastric pH, such as sucralfate, may decrease the absorption of posaconazole. The manufacturer recommends monitoring patients for breakthrough fungal infections.
Potassium Phosphate: (Moderate) Serum phosphorus should be checked routinely in patients treated chronically with sucralfate; sucralfate may cause hypophosphatemia and some patients may require phosphorus repletion. This nutrient interaction should be considered in patients receiving phosphates for dietary supplementation. It appears that sucralfate chelates phosphorus in the gut, forming nonabsorbable complexes. Because of sucralfate's therapeutic effect, this interaction may not be prevented by separating times of oral administration.
Potassium Phosphate; Sodium Phosphate: (Moderate) Serum phosphorus should be checked routinely in patients treated chronically with sucralfate; sucralfate may cause hypophosphatemia and some patients may require phosphorus repletion. This nutrient interaction should be considered in patients receiving phosphates for dietary supplementation. It appears that sucralfate chelates phosphorus in the gut, forming nonabsorbable complexes. Because of sucralfate's therapeutic effect, this interaction may not be prevented by separating times of oral administration.
Sarecycline: (Moderate) Sucralfate should be given 2 hours before or after the oral administration of tetracyclines. Divalent or trivalent cations readily chelate with tetracycline antibiotics, forming insoluble compounds. The oral absorption of these antibiotics will be significantly reduced by other orally administered compounds that contain aluminum salts, calcium salts, iron salts, magnesium salts, and/or zinc salts. Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with tetracyclines in the GI tract, reducing the bioavailability of these agents.
Sodium Bicarbonate: (Major) Antacids can interfere with the binding capacity of sucralfate to the GI mucosa, decreasing its effectiveness. Antacids should not be administered within 30 minutes of sucralfate.
Sumatriptan; Naproxen: (Moderate) Separate sucralfate and naproxen administration by at least 2 hours. Concomitant administration of sucralfate and enteric-coated or delayed-release naproxen tablets can delay the absorption of naproxen.
Tetracycline: (Moderate) Sucralfate should be given 2 hours before or after the oral administration of tetracyclines. Divalent or trivalent cations readily chelate with tetracycline antibiotics, forming insoluble compounds. The oral absorption of these antibiotics will be significantly reduced by other orally administered compounds that contain aluminum salts, calcium salts, iron salts, magnesium salts, and/or zinc salts. Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with tetracyclines in the GI tract, reducing the bioavailability of these agents.
Tetracyclines: (Moderate) Sucralfate should be given 2 hours before or after the oral administration of tetracyclines. Divalent or trivalent cations readily chelate with tetracycline antibiotics, forming insoluble compounds. The oral absorption of these antibiotics will be significantly reduced by other orally administered compounds that contain aluminum salts, calcium salts, iron salts, magnesium salts, and/or zinc salts. Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with tetracyclines in the GI tract, reducing the bioavailability of these agents.
Theophylline, Aminophylline: (Major) Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with certain drugs in the GI tract, including aminophylline, reducing its bioavailability. Sucralfate should be given 2 hours before or after the oral administration of aminophylline. (Major) Sucralfate, because it contains aluminum in its structure and due to its mechanism of action, can bind with certain drugs in the GI tract, including theophylline, reducing its bioavailability. Sucralfate should be given 2 hours before or after the oral administration of theophylline.
Thyroid hormones: (Moderate) Administer levothyroxine at least 4 hours apart from a dose of sucralfate. Patients treated concomitantly with these drugs should be monitored for changes in thyroid function. Consider an alternative to sucralfate, if appropriate. Concurrent use of sucralfate may reduce the efficacy of levothyroxine and other thyroid hormones by binding and delaying or preventing oral absorption, potentially resulting in hypothyroidism.
Warfarin: (Moderate) Sucralfate has been reported to interfere with warfarin absorption. While isolated reports have shown that sucralfate can inhibit warfarin oral absorption, other studies have shown no clinical effect.
Sucralfate exerts its action locally rather than systemically and its effect on gastric acid is negligible with a low acid-neutralizing capacity (14-16 mEq/dose). Sucralfate reacts with hydrochloric acid in the stomach to form an adherent, paste-like substance capable of acting as an acid buffer. Subsequently, sucralfate adheres electrostatically to proteins on the surface of an ulcer, such as albumin and fibrinogen, forming insoluble, stable complexes. These ulcer-bound complexes act as a protective barrier at the ulcer site, which facilitates recovery by shielding the ulcer from the ulcerogenic properties of pepsin, acid, and bile. Sucralfate predominantly binds to damaged GI mucosa, although binding to normal mucosa occurs to a minimal extent. This agent also inhibits back-diffusion of hydrogen ions, and adsorbs both pepsin and bile acids. In vivo, recommended doses of sucralfate inhibit pepsin activity in gastric juice by 32%. Recent data indicate that production of prostaglandin E2 and gastric mucus may be increased. Sucralfate also absorbs bile salts in vitro.
Pharmacokinetics:
Sucralfate is administered orally. Sucralfate predominantly acts locally, with the duration of action dependent upon the length of contact at the ulcer site. Binding to ulcer sites has been demonstrated for up to 6 hours. Animal studies indicate that the majority of an oral dose (> 90%) is excreted in the feces within 48 hours. Any systemically absorbed drug is excreted primarily in the urine.
-Route-Specific Pharmacokinetics
Oral Route
Following oral administration, minimal amounts of sucralfate are absorbed systemically (3-5%).
-Special Populations
Renal Impairment
Small amounts of aluminum can be absorbed following oral administration of sucralfate. Aluminum is cleared by the kidneys in patients with normal renal function; however, patients with renal failure or those receiving dialysis can develop aluminum accumulation due to impaired excretion. Aluminum does not cross dialysis membranes because of high plasma protein binding. Aluminum intoxication in the form of aluminum osteodystrophy, osteomalacia, or encephalopathy has been described in patients with renal impairment.