Pharmacokinetics and dynamics of famotidine in patients with renal failure.

Gladziwa, U.; Klotz, Ulrich; Krishna, D. R.; Schmitt, H.; Glöckner, W. M.; Mann, H.

doi:10.1111/j.1365-2125.1988.tb05282.x

Cited by 33 publications

(20 citation statements)

References 12 publications

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“…Depending on the degree of renal dysfunction the t1/, of famotidine was prolonged from 3 to 27h, with a simultaneous and parallel decrease in CL and CLR (Gladziwa et al 1988a;Hachisu et al 1988;Inotsume et al 1989;Lin et al 1988;Takabatake et al 1985). Thus, depending on the extent of renal impairment, dosage should be reduced by 50 to 75%.…”

Section: In Renal Insufficiencymentioning

confidence: 94%

“…In addition, no clear association between the individual pharmacokinetic and pharmacodynamic data was discernible (Gladziwa et al I 988a). This might be due to a higher acid secretion in patients with renal insufficiency (Gladziwa et al 1988a(Gladziwa et al , 1991Goldstein et al 1967;Milito et al 1983Milito et al , 1985Ritz et al 1971;Shepherd et al 1973;Venkateswaran et al 1972). Moreover, an abnormal gastric emptying time and an impaired drainage of gastric acid might play a role (Gladziwa et al 1991a).…”

Section: H2-antagonists and Bloodmentioning

confidence: 97%

“…Haemodialysis with polysulphone membranes seems to be most effective, as it removes 16.4% of the dose. However, supplementation during or after any form of blood purification procedure is not necessary (Gladziwa et al 1988a;Langtry et al 1989). Reducing the dosage to one-third of the normal dose of 40mg orally or 20mg intravenously is recommended in patients with severe renal failure who 327 are undergoing blood purification procedures (Gladziwa et al 1988a;Inotsume et al 1990).…”

Section: During Blood Purification Proceduresmentioning

confidence: 98%

“…Ebihara et (1977); 400-600 Larsson et al (1979Larsson et al ( , 1981Larsson et al ( . 1982 Famotidine Gladziwa et al (1988a); 15-20 Lin et al (1988) Hachisu et al (1988 60/week Takabatake et al (1986) 40 20 10 Hachisu et al (1992) 75 tiw Lameire et al (1988b) 75 q24h 40 q24h Takabatake et al (1986) 75 q8h 75 q24h 75 q48h a ml/min/1.48m 2 .…”

Section: In Renal Insufficiencymentioning

confidence: 98%

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Pharmacokinetics and Pharmacodynamics of H2-Receptor Antagonists in Patients with Renal Insufficiency

Gladziwa

Klotz

1993

Clinical Pharmacokinetics

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H2-receptor antagonists are frequently used in patients with renal insufficiency to treat hyperacidity and resultant peptic ulceration. All H2-antagonists are mainly eliminated by the renal route (glomerular filtration and tubular secretion). Since it is dependent on creatinine clearance (CLCR), elimination will be impaired in renal insufficiency. Protein binding and volumes of distribution (Vd) of H2-antagonists are not significantly altered in patients with renal impairment. Bioavailability (F) is similar in patients with and without renal insufficiency, except for nizatidine, which has an F that is lower in uraemic patients. When given in similar doses, mean peak concentrations (Cmax) and area under the concentration-time curve (AUC) are higher in patients with renal insufficiency than in those with normal renal function. Thus, maintenance doses of H2-antagonists should be reduced in line with reductions in CLCR. The time to reach Cmax is similar for all drugs except ranitidine, which has a delayed Cmax. Due to the decreased renal clearance (CLR), elimination half-life (t1/2) is prolonged 3- to 8-fold depending upon the degree of renal failure and the particular drug. H2-antagonists are removed by various dialysis procedures in insignificant amounts. Thus, no dosage supplementation is necessary after any type of dialysis therapy. By means of intragastric long term pH-metry it has been shown that inhibition of gastric acid secretion is prolonged in patients with renal insufficiency.

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Section: In Renal Insufficiencymentioning

confidence: 94%

Section: H2-antagonists and Bloodmentioning

confidence: 97%

Section: During Blood Purification Proceduresmentioning

confidence: 98%

Section: In Renal Insufficiencymentioning

confidence: 98%

See 2 more Smart Citations

Pharmacokinetics and Pharmacodynamics of H2-Receptor Antagonists in Patients with Renal Insufficiency

Gladziwa

Klotz

1993

Clinical Pharmacokinetics

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“…Therefore, dose reduction is recommended for all 4 H2-antagonists based on creatinine clearance (table I). All H2-antagonists are minimally cleared by dialysis (both haemodialysis and peritoneal dialysis) and do not need to be supplemented after dialysis (Aronoff et al 1988;Garg et al 1985;Gladziwa et al 1988;Somogyi & Gugler 1983). However, with newer more permeable membranes and increased use of continuous arteriovenous haemofiltration in the intensive care unit setting, there is the potential for increased drug loss with dialysis, although there are few data to support this.…”

Section: H2-antagonistsmentioning

confidence: 95%

Renal Effects of Peptic Ulcer Therapy

Burgess

Muruve

1992

Drug Safety

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Drugs used in the treatment of peptic ulcer disease may interact with the renal system in a variety of ways. Since many agents are eliminated by renal excretion, clearance of these agents may be reduced and half-life extended in the presence of renal insufficiency. The histamine H2-receptor antagonists may interfere with renal tubular excretion of creatinine and cationic drugs, resulting in elevated serum concentrations and reduced renal clearance. The prostaglandin E1 analogue misoprostol is used as a cytoprotective agent but has renal effects. The renal effects differ between systems studied. In the rat, misoprostol reduces cyclosporin-induced renal tubular toxicity, whereas in humans it has been shown to attenuate renal allograft rejection. Sucralfate is the aluminium salt of sucrose octasulfate. It permits the absorption of aluminium in amounts similar to aluminium-containing antacids, and toxicity has been demonstrated in the presence of renal insufficiency. Bismuth compounds are used increasingly to treat peptic ulcer disease, and bismuth toxicity has been described in association with renal insufficiency. Aluminium-, calcium- and magnesium-containing antacids are used as oral phosphate binders in patients with renal insufficiency in addition to their usual indications. Cation absorption and accumulation with all of these antacid preparations has been described and may lead to toxicity.

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Hemofiltrability of H₂‐Receptor Antagonist, Famotidine, in Renal Failure Patients

Saima

Echizen

Yoshimoto

et al. 1990

The Journal of Clinical Pharma

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To determine if a new H2-receptor antagonist, famotidine, would be significantly removed by arteriovenous hemofiltration, we measured plasma concentrations and amounts of the drug recovered in ultrafiltrate during 18 sessions of an intermittent hemofiltration performed in five patients with renal failure receiving the repeated intravenous dosings of the drug (5-20 mg/day). Plasma and ultrafiltrate drug concentrations were determined by using a high performance liquid chromatography with fluorescent detection. The mean (+/- SD) amount of the drug removed by the procedure, which was performed at the mean ultrafiltration rate of 19.0 +/- 6.0 ml/min over the mean duration of 212 +/- 168 min, corresponded to 4.1 +/- 2.2% of the daily maintenance doses. There was a significant (r = 0.90, P less than .01) linear relationship between the hemofiltration clearance and the ultrafiltration rate, indicating that the sieving coefficient, an index filtration efficiency, for the drug was largely constant (i.e., 0.73 +/- 0.10) over the ranging filtration rates (i.e., 3.9-29.5 mL/min) employed in the present study. When the mean filtration efficiency of 0.73 obtained from the study is extrapolated into a 24-hour continuous arteriovenous hemofiltration performed at commonly used filtration rates (i.e., 6-12 ml/min), the 24-hour hemofiltration clearances are estimated to range from 4 to 9 ml/min. These clearance values are found to correspond to only 10 to 25% of the mean total body clearance (about 35 ml/min) reported from anuric patients.(ABSTRACT TRUNCATED AT 250 WORDS)

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Pharmacokinetics and dynamics of famotidine in patients with renal failure.

Cited by 33 publications

References 12 publications

Pharmacokinetics and Pharmacodynamics of H2-Receptor Antagonists in Patients with Renal Insufficiency

Pharmacokinetics and Pharmacodynamics of H2-Receptor Antagonists in Patients with Renal Insufficiency

Renal Effects of Peptic Ulcer Therapy

Hemofiltrability of H₂‐Receptor Antagonist, Famotidine, in Renal Failure Patients

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Pharmacokinetics and dynamics of famotidine in patients with renal failure.

Cited by 33 publications

References 12 publications

Pharmacokinetics and Pharmacodynamics of H2-Receptor Antagonists in Patients with Renal Insufficiency

Pharmacokinetics and Pharmacodynamics of H2-Receptor Antagonists in Patients with Renal Insufficiency

Renal Effects of Peptic Ulcer Therapy

Hemofiltrability of H2‐Receptor Antagonist, Famotidine, in Renal Failure Patients

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Product

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Hemofiltrability of H₂‐Receptor Antagonist, Famotidine, in Renal Failure Patients