Histamine Receptor 1 and 2 Antagonists Alter Biodistribution of Radioiodine

Oliver Edwards; Ellen D Yakish; Li-Ming Wang; Qi Wu; John M Hoffman; Kathryn A Morton

doi:10.2967/jnmt.115.160697

Histamine Receptor 1 and 2 Antagonists Alter Biodistribution of Radioiodine

J Nucl Med Technol. 2015 Sep;43(3):214-9. doi: 10.2967/jnmt.115.160697. Epub 2015 Jun 25.

Authors

Oliver Edwards¹, Ellen D Yakish², Li-Ming Wang¹, Qi Wu¹, John M Hoffman¹, Kathryn A Morton³

Affiliations

¹ Department of Radiology, University of Utah, Salt Lake City, Utah; and.
² Intermountain Heart Center, Murray, Utah.
³ Department of Radiology, University of Utah, Salt Lake City, Utah; and Kathryn.morton@hsc.utah.edu.

PMID: 26111706
DOI: 10.2967/jnmt.115.160697

Abstract

Nuclear medicine technology assumes responsibility for examination-specific patient preparation procedures. This requires a clear understanding of the possible effects of medications on the outcome of examinations. There is evidence that common over-the-counter drugs, histamine 1 (H1) and histamine 2 (H2) receptor blockers and proton pump inhibitors, may directly or indirectly affect thyroid function. The objective was to determine whether short-term use of these drugs alters biodistribution of radioiodine in a rat model.

Methods: Rats received no drug (controls) or daily subcutaneous injections of H1 blocker (promethazine), H2 blocker (famotidine), or proton pump inhibitor (esomeprazole) commencing 1 d before a single intraperitoneal injection of 0.037 MBq (1 μCi) of (131)I (NaI) and continuing daily until euthanasia at either 1 d or 8 d after (131)I. Organ uptake of (131)I by control and drug-treated rats was compared by γ-well counting.

Results: Promethazine significantly increased uptake of (131)I by the thyroid (drug-treated-to-control ratios) both at 1 d (1.32) and 8 d (1.52) after (131)I. Both famotidine and promethazine (respectively) significantly increased salivary gland uptake of (131)I (drug-treated-to-control ratios) at 1 d (1.37, 1.40) and 8 d (4.52, 5.57) after (131)I. Promethazine significantly increased gastric (131)I uptake (drug-treated-to-control ratios) at 1 d (1.47) and 8 d (1.46) after (131)I. Famotidine and promethazine (respectively) significantly decreased uptake of (131)I by the liver (drug-treated-to-control ratios) at 1 d (0.60, 0.71) after (131)I but resulted in a marked increase over control levels (11.21, 9.28) at 8 d. Blood levels of (131)I were not altered by drug treatment. Esomeprazole did not affect radioiodine distribution.

Conclusion: H1 and H2 blockers alter the biodistribution of radioiodine in the rat. Although the findings remain to be confirmed in humans, these drugs could increase radiation exposure to nontarget tissues, particularly the stomach and salivary tissue, during (131)I therapy and consideration should be given toward avoiding the elective use of these drugs during radioiodine therapy.

Keywords: 131I; biodistribution; drugs; gastritis; radioiodine; rat; sialadenitis; xerostomia.

MeSH terms

Animals
Drug Interactions
Esomeprazole / administration & dosage
Famotidine / administration & dosage
Gastric Mucosa / metabolism*
Histamine Antagonists / administration & dosage*
Iodine Radioisotopes / pharmacokinetics*
Male
Organ Specificity / drug effects
Promethazine / administration & dosage
Proton Pump Inhibitors / administration & dosage*
Radiopharmaceuticals / pharmacokinetics*
Rats
Rats, Sprague-Dawley
Receptors, Histamine H1 / drug effects
Receptors, Histamine H2 / administration & dosage
Receptors, Histamine H2 / drug effects
Salivary Glands / metabolism*
Thyroid Gland / metabolism
Tissue Distribution / drug effects

Substances

Histamine Antagonists
Iodine Radioisotopes
Proton Pump Inhibitors
Radiopharmaceuticals
Receptors, Histamine H1
Receptors, Histamine H2
Famotidine
Promethazine
Esomeprazole