B. Marchant scite author profile

Flurbiprofen was rapidly absorbed in all species studied. 2. Half-lives of elimination measured 0 to 12 h after a single dose were: mouse 3.4 h, rat 2.5 h, dog 10.1 h, baboon 3.1 h and man 3.9 h. A second phase of elimination was seen in the dog. Flurbiprofen accumulated in the circulation of the dog on repeated dosing. 3. After dosing with [14C]flurbiprofen, tissue levels of radioactivity in dog and baboon were similar to that in plasma. In the rat, levels were slightly elevated in liver, kidney, large intestine and thyroid after repeated dosing. 4. The dog excreted equal amounts of radioactivity in urine and faeces. In other species renal excretion was the more important route. 5. Six metabolites have been detected, the most important being: 2-(2-fluoro-4'-hydroxy-4-biphenylyl)propionic acid (metabolite 1), 2-(i-fluoro-3',4'-dihydroxy-4-biphenylyl)propionic acid (metabolite 2) and 2-(2-fluoro-3'-hydroxy-4'-methoxy-4-biphenylyl)propionic acid (metabolite 3). The proportions of the metabolites and the extents of their conjugation varied among the species. 6. Metabolites were detected in the circulation of rat, mouse and baboon but not in dog and man. 7. Flurbiprofen did not affect the hepatic drug-metabolizing enzyme system of rat. 8. Flurbiprofen was extensively bound to serum protein of rat, dog, baboon and man.

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The Placental Transfer of Propylthiouracil, Methimazole and Carbimazole

Marchant

Brownlie

Hart

et al. 1977

The Journal of Clinical Endocrinology & Metabolism

163

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The placental transfer of 35S-labelled methimazole (MMI), carbimazole and propylthiouracil (PTU) has been examined in the rat in late pregnancy and in patients undergoing therapeutic abortion. Although rapid equilibrium of fetal and maternal serum radioactivity (FS:MS ratio 1:1) occurred after iv administration of 35S-carbimazole or 35S-MMI in rats, a persistent fetal to maternal ratio of less than one was observed after 35S-PTU administration. Results from human studies after a single oral dose indicate that, as in the rat, the placenta appeared to be more permeable to 35S-MMI than to 35S-PTU as shown by the marked difference in fetal serum:maternal serum ratios and amounts accumulated in the fetus. Localization of radioactivity in the human fetal thyroid was also observed after administration of 35S-labelled MMI, carbimazole or PTU.

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Antithyroid drugs

Marchant¹,

Lees²,

Alexander³

1978

Pharmacology & Therapeutics. Part B: General and Systematic

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The Accumulation of³⁵S-Antithyroid Drugs by the Thyroid Gland

Marchant¹,

Alexander²,

Lazarus³

et al. 1972

The Journal of Clinical Endocrinology & Metabolism

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Concentration of 35S-propylthiouracil by the thyroid gland and its relationship to anion trapping mechanism

et al. 1971

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B. Marchant

The Disposition and Metabolism of Flurbiprofen in Several Species Including Man

The Placental Transfer of Propylthiouracil, Methimazole and Carbimazole

Antithyroid drugs

The Accumulation of³⁵S-Antithyroid Drugs by the Thyroid Gland

Concentration of 35S-propylthiouracil by the thyroid gland and its relationship to anion trapping mechanism

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About

B. Marchant

The Disposition and Metabolism of Flurbiprofen in Several Species Including Man

The Placental Transfer of Propylthiouracil, Methimazole and Carbimazole

Antithyroid drugs

The Accumulation of35S-Antithyroid Drugs by the Thyroid Gland

Concentration of 35S-propylthiouracil by the thyroid gland and its relationship to anion trapping mechanism

Contact Info

Product

Resources

About

The Accumulation of³⁵S-Antithyroid Drugs by the Thyroid Gland