Jay H. Bauman scite author profile

Propylthiouracil discontinued 4-7 days before radioiodine dosing is associated with a significant increase in the failure rate of a single dose of radioiodine. Discontinuation of the propylthiouracil for at least a week before radioiodine administration is associated with a higher, although not statistically significant, radioiodine failure rate. In patients that require treatment with propylthiouracil before radioiodine therapy, a higher total serum thyroxine level at diagnosis is associated with an increased rate of radioiodine failure. Consideration should be given to increasing empirically the dose of radioiodine administered to Graves' disease patients that have received propylthiouracil within a week of radioiodine administration in an effort to decrease the radioiodine failure rate to an acceptable level.

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Cimetidine as an Inhibitor of Drug Metabolism: Therapeutic Implications and Review of the Literature

Bauman¹,

Kimelblatt²

1982

Drug Intelligence & Clinical Pharmacy

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Cimetidine has been reported to decrease the biotransformation of drugs metabolized by the MFOE system. Additionally, cimetidine decreases liver blood flow and increases the bioavailability of drugs with high hepatic extraction ratios. Patients receiving cimetidine in conjunction with drugs known to interact with cimetidine in conjunction with drugs known to interact with cimetidine are at risk of experiencing toxicity. When appropriate, reducing the dosage of these agents or switching to an alternative drug will minimize the incidence of side effects. Clinicians should be suspicious if patients experience exaggerated drug effects when cimetidine therapy is begun.

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Evaluation and Effectiveness of a Pharmaceutical-Based Drug Information Service

Bauman

Bettenhausen

1994

Drug Information Journal

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Ranitidine Hydrochloride

Gaginella¹,

Bauman²

1983

Drug Intelligence & Clinical Pharmacy

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Ranitidine is a selective, competitive histamine H2-receptor antagonist recently approved by the Food and Drug Administration for use in the short-term treatment of active duodenal ulcers and gastric hypersecretory conditions. Ranitidine is four to ten times more potent than cimetidine on a molar basis in inhibiting stimulated gastric acid secretion. Clinical studies have demonstrated that ranitidine is as effective as cimetidine and is similarly well tolerated. Based on available literature (approximately 700 publications), this article reviews the pharmacology, safety profile, and clinical efficacy of ranitidine in duodenal ulcers and gastric hypersecretory conditions.

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Comment on Effect of Cimetidine on Theophylline Clearance

Bauman¹,

Kimelblatt

1981

Drug Intelligence & Clinical Pharmacy

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Jay H. Bauman

The effect of propylthiouracil on subsequent radioactive iodine therapy in Graves' disease

Cimetidine as an Inhibitor of Drug Metabolism: Therapeutic Implications and Review of the Literature

Evaluation and Effectiveness of a Pharmaceutical-Based Drug Information Service

Ranitidine Hydrochloride

Comment on Effect of Cimetidine on Theophylline Clearance

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