Thyroid Hormone Kinetics – Processes and Relevance
Thyroid hormone kinetics describes how thyroid hormones are absorbed, distributed, converted, and eliminated in the body. It is essential for diagnosing and treating thyroid disorders.
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Thyroid hormone kinetics describes how thyroid hormones are absorbed, distributed, converted, and eliminated in the body. It is essential for diagnosing and treating thyroid disorders.
What Is Thyroid Hormone Kinetics?
Thyroid hormone kinetics is a branch of physiology and pharmacology that describes the time-dependent processes governing the production, secretion, transport, cellular uptake, conversion, and elimination of the thyroid hormones thyroxine (T4) and triiodothyronine (T3). A thorough understanding of these processes is essential for correctly interpreting laboratory values and for the appropriate dosing of thyroid medications.
Production and Secretion
Under the stimulation of thyroid-stimulating hormone (TSH) released by the pituitary gland, the thyroid gland produces mainly T4 (approximately 80–90 %) and a smaller proportion of T3 (approximately 10–20 %). T4 functions primarily as a storage and transport form of the hormone, while T3 is the biologically far more potent form. In healthy adults, daily production amounts to approximately 80–100 µg of T4 and 25–35 µg of T3.
Transport in the Blood
Once released into the bloodstream, more than 99 % of thyroid hormones are bound to carrier proteins. The most important binding proteins are:
- Thyroxine-binding globulin (TBG) – carries approximately 70–75 % of circulating hormones
- Transthyretin (TTR) – carries approximately 10–15 %
- Albumin – carries approximately 15–20 %
Only the very small fraction of free T4 (fT4) and free T3 (fT3) is biologically active and able to enter target cells. These free fractions are therefore particularly relevant for laboratory diagnostics.
Half-Lives and Volume of Distribution
A central concept in hormone kinetics is the half-life – the time it takes for the concentration of a hormone to decrease to half of its initial value. Reference values for thyroid hormones are:
- T4: half-life approximately 6–8 days, reflecting strong protein binding and a large volume of distribution
- T3: half-life approximately 1–2 days, due to lower protein binding and faster turnover
These long half-lives explain why changes in blood hormone concentrations and adjustments to medication dosages do not reach their full effect until several weeks later.
Peripheral Conversion: T4 to T3
One of the most important steps in thyroid hormone kinetics is peripheral deiodination. In various tissues – particularly the liver, kidneys, muscle, and brain – T4 is converted to T3 by enzymes called deiodinases (types I, II, and III). This conversion supplies the majority of circulating T3 (approximately 80 % of T3 in the bloodstream originates from peripheral conversion rather than direct thyroid secretion). In addition to active T3, this process also produces the biologically inactive reverse T3 (rT3), levels of which can be elevated during stress, serious illness, or fasting.
Cellular Uptake and Mechanism of Action
Free hormone fractions are actively transported into target cells via specific membrane transporter proteins (e.g., MCT8, OATP1C1). Inside the cell nucleus, they bind to thyroid hormone receptors (TR-alpha, TR-beta), which act as transcription factors regulating the expression of numerous enzymes and structural proteins. Through this mechanism, thyroid hormones control basal metabolic rate, heart rate, body temperature, growth, bone maturation, and cognitive function.
Metabolism and Elimination
Inactivation of thyroid hormones occurs mainly through deiodination (removal of iodine atoms), sulfation, and glucuronidation, primarily in the liver and intestine. Conjugated metabolites are excreted via bile into the intestine, where intestinal bacteria can partially cleave and reabsorb them through the enterohepatic circulation. The remainder is excreted in the feces, while a small proportion leaves the body via the urine.
Clinical Relevance
Understanding thyroid hormone kinetics is indispensable in several clinical situations:
- In hypothyroidism, levothyroxine (synthetic T4) must be dosed to achieve stable fT4 and TSH levels. Due to the long half-life of T4, once-daily administration is sufficient, but follow-up measurements should not be performed before 4–6 weeks after a dose adjustment.
- In hyperthyroidism, kinetic principles help predict how quickly antithyroid drugs will lower hormone levels and when normal values can be expected.
- Certain medications (e.g., amiodarone, glucocorticoids, propylthiouracil) and disease states significantly affect deiodinase activity and thus the conversion of T4 to T3.
- Pregnancy, liver cirrhosis, and kidney disease alter the concentration of binding proteins, thereby affecting total hormone measurements.
References
- Bianco, A. C. et al. (2019): American Thyroid Association Guide to Investigating Thyroid Hormone Economy and Action in Rodent and Cell Models. Thyroid, 24(1): 88–168. PubMed PMID: 24001314.
- Larsen, P. R. et al. (2016): Williams Textbook of Endocrinology. 13th ed. Elsevier, Philadelphia.
- World Health Organization (WHO) (2023): Thyroid disorders – Fact sheets. Geneva: WHO. Available at: https://www.who.int
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