Hypothalamic–pituitary–thyroid axis

From Wikipedia, the free encyclopedia
Short overview of thyroid homeostasis.[1]

The hypothalamic–pituitary–thyroid axis (HPT axis for short, a.k.a. thyroid homeostasis or thyrotropic feedback control) is part of the neuroendocrine system responsible for the regulation of metabolism and also responds to stress.

As its name suggests, it depends upon the hypothalamus, the pituitary gland, and the thyroid gland.

The hypothalamus senses low circulating levels of thyroid hormone (Triiodothyronine (T3) and Thyroxine (T4)) and responds by releasing thyrotropin-releasing hormone (TRH). The TRH stimulates the anterior pituitary to produce thyroid-stimulating hormone (TSH). The TSH, in turn, stimulates the thyroid to produce thyroid hormone until levels in the blood return to normal. Thyroid hormone exerts negative feedback control over the hypothalamus as well as anterior pituitary, thus controlling the release of both TRH from hypothalamus and TSH from anterior pituitary gland.[2]

The HPA, HPG, and HPT axes are three pathways in which the hypothalamus and pituitary direct neuroendocrine function.

Physiology[edit]

Thyrotropic feedback control on a more detailed and quantitative level.[3]

Thyroid homeostasis results from a multi-loop feedback system that is found in virtually all higher vertebrates. Proper function of thyrotropic feedback control is indispensable for growth, differentiation, reproduction and intelligence. Very few animals (e.g. axolotls and sloths) have impaired thyroid homeostasis that exhibits a very low set-point that is assumed to underlie the metabolic and ontogenetic anomalies of these animals.

The pituitary gland secretes thyrotropin (TSH; Thyroid Stimulating Hormone) that stimulates the thyroid to secrete thyroxine (T4) and, to a lesser degree, triiodothyronine (T3). The major portion of T3, however, is produced in peripheral organs, e.g. liver, adipose tissue, glia and skeletal muscle by deiodination from circulating T4. Deiodination is controlled by numerous hormones and nerval signals including TSH, vasopressin and catecholamines.

Both peripheral thyroid hormones (iodothyronines) inhibit thyrotropin secretion from the pituitary (negative feedback). Consequently, equilibrium concentrations for all hormones are attained.

TSH secretion is also controlled by thyrotropin releasing hormone (thyroliberin, TRH), whose secretion itself is again suppressed by plasma T4 and T3 in CSF (long feedback, Fekete–Lechan loop).[4] Additional feedback loops are ultrashort feedback control of TSH secretion (Brokken-Wiersinga-Prummel loop)[5] and linear feedback loops controlling plasma protein binding.

Recent research suggested the existence of an additional feedforward motif linking TSH release to deiodinase activity in humans.[6][7][8] The existence of this TSH-T3 shunt could explain why deiodinase activity is higher in hypothyroid patients and why a minor fraction of affected individuals may benefit from substitution therapy with T3.[9]

Convergence of multiple afferent signals in the control of TSH release including but not limited to T3,[10] cytokines[11][12] and TSH receptor antibodies[13] may be the reason for the observation that the relation between free T4 concentration and TSH levels deviates[14][15][16][17] from a pure loglinear relation that has previously been proposed.[18] Recent research suggests that ghrelin also plays a role in the stimulation of T4 production and the subsequent suppression of TSH directly and by negative feedback.[19]

Functional states of thyrotropic feedback control[edit]

Diagnostics[edit]

Standard procedures cover the determination of serum levels of the following hormones:

  • TSH (thyrotropin, thyroid stimulating hormone)
  • Free T4
  • Free T3

For special conditions the following assays and procedures may be required:

See also[edit]

References[edit]

  1. ^ References used in overview figure are found in image article in Commons: References.
  2. ^ Dietrich JW, Landgrafe G, Fotiadou EH (2012). "TSH and Thyrotropic Agonists: Key Actors in Thyroid Homeostasis". Journal of Thyroid Research. 2012: 1–29. doi:10.1155/2012/351864. PMC 3544290. PMID 23365787.
  3. ^ References used in detailed figure are found in image article in Commons: References.
  4. ^ Lechan, Ronald M.; Fekete, C (2004). "Feedback regulation of thyrotropin-releasing hormone (TRH): mechanisms for the non-thyroidal illness syndrome". Journal of Endocrinological Investigation. 27 (6 Suppl): 105–19. PMID 15481810.
  5. ^ Prummel MF, Brokken LJ, Wiersinga WM (2004). "Ultra short-loop feedback control of thyrotropin secretion". Thyroid. 14 (10): 825–9. doi:10.1089/thy.2004.14.825. PMID 15588378.
  6. ^ Hoermann R, Midgley JE, Giacobino A, Eckl WA, Wahl HG, Dietrich JW, Larisch R (2014). "Homeostatic equilibria between free thyroid hormones and pituitary thyrotropin are modulated by various influences including age, body mass index and treatment". Clinical Endocrinology. 81 (6): 907–15. doi:10.1111/cen.12527. PMID 24953754. S2CID 19341039.
  7. ^ Dietrich, JW; Midgley, JE; Larisch, R; Hoermann, R (December 2015). "Of rats and men: thyroid homeostasis in rodents and human beings". The Lancet Diabetes & Endocrinology. 3 (12): 932–933. doi:10.1016/S2213-8587(15)00421-0. PMID 26590684.
  8. ^ Hoermann, R; Midgley, JE; Larisch, R; Dietrich, JW (2015). "Homeostatic Control of the Thyroid-Pituitary Axis: Perspectives for Diagnosis and Treatment". Frontiers in Endocrinology. 6: 177. doi:10.3389/fendo.2015.00177. PMC 4653296. PMID 26635726.
  9. ^ Hoermann R, Midgley JE, Larisch R, Dietrich JW (2015). "Integration of Peripheral and Glandular Regulation of Triiodothyronine Production by Thyrotropin in Untreated and Thyroxine-Treated Subjects". Hormone and Metabolic Research. 47 (9): 674–80. doi:10.1055/s-0034-1398616. PMID 25750078. S2CID 9824656.
  10. ^ Hoermann, R; Midgley, JEM; Dietrich, JW; Larisch, R (June 2017). "Dual control of pituitary thyroid stimulating hormone secretion by thyroxine and triiodothyronine in athyreotic patients". Therapeutic Advances in Endocrinology and Metabolism. 8 (6): 83–95. doi:10.1177/2042018817716401. PMC 5524252. PMID 28794850.
  11. ^ Fliers, E; Kalsbeek, A; Boelen, A (November 2014). "Beyond the fixed setpoint of the hypothalamus-pituitary-thyroid axis" (PDF). European Journal of Endocrinology. 171 (5): R197–208. doi:10.1530/EJE-14-0285. PMID 25005935.
  12. ^ a b Chatzitomaris, Apostolos; Hoermann, Rudolf; Midgley, John E.; Hering, Steffen; Urban, Aline; Dietrich, Barbara; Abood, Assjana; Klein, Harald H.; Dietrich, Johannes W. (20 July 2017). "Thyroid Allostasis–Adaptive Responses of Thyrotropic Feedback Control to Conditions of Strain, Stress, and Developmental Programming". Frontiers in Endocrinology. 8: 163. doi:10.3389/fendo.2017.00163. PMC 5517413. PMID 28775711.
  13. ^ Brokken LJ, Wiersinga WM, Prummel MF (2003). "Thyrotropin receptor autoantibodies are associated with continued thyrotropin suppression in treated euthyroid Graves' disease patients". Journal of Clinical Endocrinology & Metabolism. 88 (9): 4135–4138. doi:10.1210/jc.2003-030430. PMID 12970276.
  14. ^ Hoermann R, Eckl W, Hoermann C, Larisch R (2010). "Complex relationship between free thyroxine and TSH in the regulation of thyroid function". European Journal of Endocrinology. 162 (6): 1123–9. doi:10.1530/EJE-10-0106. PMID 20299491.
  15. ^ Clark PM, Holder RL, Haque SM, Hobbs FD, Roberts LM, Franklyn JA (2012). "The relationship between serum TSH and free T4 in older people". Journal of Clinical Pathology. 65 (5): 463–5. doi:10.1136/jclinpath-2011-200433. PMID 22287691. S2CID 43886378.
  16. ^ Hoermann R, Midgley JE, Larisch R, Dietrich JW (2012). "Is pituitary TSH an adequate measure of thyroid hormone-controlled homoeostasis during thyroxine treatment?". European Journal of Endocrinology. 168 (2): 271–80. doi:10.1530/EJE-12-0819. PMID 23184912.
  17. ^ Midgley JE, Hoermann R, Larisch R, Dietrich JW (2013). "Physiological states and functional relation between thyrotropin and free thyroxine in thyroid health and disease: In vivo and in silico data suggest a hierarchical model". Journal of Clinical Pathology. 66 (4): 335–42. doi:10.1136/jclinpath-2012-201213. PMID 23423518. S2CID 46291947.
  18. ^ Reichlin S, Utiger RD (1967). "Regulation of the pituitary-thyroid axis in man: Relationship of TSH concentration to concentration of free and total thyroxine in plasma". The Journal of Clinical Endocrinology and Metabolism. 27 (2): 251–5. doi:10.1210/jcem-27-2-251. PMID 4163614.
  19. ^ Kluge M, et al. (2010). "Ghrelin affects the hypothalamus–pituitary–thyroid axis in humans by increasing free thyroxine and decreasing TSH in plasma". European Journal of Endocrinology. 162 (6): 1059–1065. doi:10.1530/EJE-10-0094. PMID 20423986. S2CID 5237852.
  20. ^ Liu S, Ren J, Zhao Y, Han G, Hong Z, Yan D, Chen J, Gu G, Wang G, Wang X, Fan C, Li J (2013). "Nonthyroidal illness syndrome: Is it far away from Crohn's disease?". Journal of Clinical Gastroenterology. 47 (2): 153–9. doi:10.1097/MCG.0b013e318254ea8a. PMID 22874844. S2CID 35344744.
  21. ^ a b Dietrich, J. W. (2002). Der Hypophysen-Schilddrüsen-Regelkreis. Berlin, Germany: Logos-Verlag Berlin. ISBN 978-3-89722-850-4. OCLC 50451543. OL 24586469M. 3897228505.
  22. ^ Jostel A, Ryder WD, Shalet SM (2009). "The use of thyroid function tests in the diagnosis of hypopituitarism: Definition and evaluation of the TSH Index". Clinical Endocrinology. 71 (4): 529–34. doi:10.1111/j.1365-2265.2009.03534.x. PMID 19226261. S2CID 10827131.

Further reading[edit]