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Journal ArticleDOI

Hydrochlorothiazide‐Induced 131I Excretion Facilitated by Salt and Water

TLDR
Thiazide administration in customary clinical dosage twice a day with substantial sodium chloride and water for the first two days after exposure to 131I, should facilitate the safe excretion of 131I.
Abstract
Salt intake is restricted under clinical conditions for which thiazide diuretics are customarily used. Dietary iodide intake offsets any effect of thiazide on iodide loss. However, our correlation coefficients relating Na+ to Cl− to l− excretion indicate that as thiazide administration or sodium chloride intake increases renal Na+ and Cl− excretion, l− reabsorption by the nephron coordinately decreases. Increased sodium chloride and water intake by the dog doubled l−excretion rates. Hydrochlorothiazide increased the sodium chloride and water enhanced l−excretion rate as much as eight-fold. Without added NaCl, hydrochlorothiazide increased the excretion rate of 131I by three- to eightfold, acutely. Within five to seven days after 131I oral administration, hydrochlorothiazide (1 or 2 mg/kg twice daily) doubled the rate of 131I disappearance from plasma, reduced the fecal output of 131I, and increased its rate of renal excretion. When hydrochlorothiazide was administered, as much 131I was excreted in the first 24 hours as occurred in 48 hours when sodium chloride and water were given without hydrochlorothiazide. Thiazide administration in customary clinical dosage twice a day with substantial sodium chloride and water for the first two days after exposure to 131I, should therefore facilitate the safe excretion of 131I. This accelerated removal of 131I might be enhanced even more if thyroid uptake of 131I is blocked by administration of potassium iodide, as judged by the greater 131I recovery from thyroidectomized dogs.

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Citations
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Journal ArticleDOI

Radioiodine Therapy in Benign Thyroid Diseases: Effects, Side Effects, and Factors Affecting Therapeutic Outcome

TL;DR: Radioiodine ((131)I) therapy of benign thyroid diseases was introduced 70 yr ago, and the patients treated since then are probably numbered in the millions, but results have been conflicting due to differences in design, sample size, patient selection, and dose calculation.

Toxicological profile for iodine

J. Risher
TL;DR: This edition supersedes any previously released draft or final profile and reflects a comprehensive and extensive evaluation, summary, and interpretation of available toxicologic and epidemiologic information on a substance.
Journal ArticleDOI

Transfer of Inhaled Cannabis Into Human Breast Milk.

TL;DR: Delta-9-tetrahydrocannabinol was transferred into mother's milk such that exclusively breastfeeding infants ingested an estimated mean of 2.5% of the maternal dose (the calculated relative infant dose=2.5%, range 0.4-8.7%).
Journal ArticleDOI

Clinical features and management of intoxication due to hallucinogenic drugs.

TL;DR: Hallucinogenic drugs are unique in that they produce the desired hallucinogenic effects at what are considered non-toxic doses and management of the intoxicated patient is dependent on the specific behavioural manifestation elicited by the drug.
References
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Journal ArticleDOI

Metabolites of Thyroxine.

TL;DR: It is suggested that thyroxine is metabolized to yield at least the two compounds Nos. 1 and 4 as well as iodide, which are likewise found in organs and excreta taken from intact mice and rats injected 48 hours previously with radio-iodide.
Journal Article

The distribution of administered iodide and thiocyanate in comparison with chloride, and their relation to body fluids

TL;DR: In this paper, the distribution of iodide in various tissues of the body was determined and compared to that of thiocyanate and chloride, and the relative concentration in terms of blood-tissue ratio was alike for the three substances in the organs examined, with the exception of the brain, in which the chloride was in much larger amounts than the other two.
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