出典(authority):フリー百科事典『ウィキペディア(Wikipedia)』「2016/08/22 14:30:01」(JST)
Thyroid | |
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The human thyroid as viewed from the front, with arteries visible.
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The thyroid as it may be seen from a posterior view, from behind the trachea
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Details | |
Precursor | Thyroid diverticulum (an extension of endoderm into 2nd pharyngeal arch) |
System | Endocrine system |
Artery | Superior, Inferior thyroid arteries |
Vein | Superior, middle, Inferior thyroid veins |
Identifiers | |
Latin | Glandula thyreoidea |
MeSH | A06.407.900 |
Dorlands /Elsevier |
Thyroid gland |
TA | A11.3.00.001 |
FMA | 9603 |
Anatomical terminology
[edit on Wikidata]
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The thyroid gland, or simply the thyroid /ˈθaɪrɔɪd/, is one of the largest endocrine glands in the body, and consists of two connected lobes. It is found in the anterior neck, below the laryngeal prominence (Adam's apple). The thyroid gland controls the metabolic rate, protein synthesis, and controls the body's sensitivity to other hormones. The thyroid hormones regulate the growth and rate of function of many other systems in the body. T3 and T4 are synthesized from iodine and tyrosine. The thyroid also produces calcitonin, which plays a role in calcium homeostasis.
Hormonal output from the thyroid is regulated by thyroid-stimulating hormone (TSH) produced by the anterior pituitary, which itself is regulated by thyrotropin-releasing hormone (TRH) produced by the hypothalamus.[1]
The thyroid may be affected by several diseases. Hyperthyroidism occurs when the gland produces excessive amounts of thyroid hormones, the most common cause being Graves' disease—an autoimmune disorder. In contrast, hypothyroidism is a state of insufficient thyroid hormone production. Worldwide, the most common cause is iodine deficiency. Thyroid hormones are important for development, and hypothyroidism secondary to iodine deficiency remains the leading cause of preventable intellectual disability.[2] In iodine-sufficient regions, the most common cause of hypothyroidism is Hashimoto's thyroiditis—also an autoimmune disease. In addition, the thyroid gland may also develop several types of nodules and cancer.
The thyroid gland is a butterfly-shaped organ and is composed of two lobes, one on the right and the left as the wings, and the connecting isthmus as the body.[3][4]The thyroid is one of the larger endocrine glands, weighing 2-3 grams in neonates[citation needed] and 25 grams in adults, and is increased in pregnancy.[3] Each lobe is about 5 cm long, 3 cm wide and 2 cm thick, with the isthmus about 1.25 cm in length.[3] The lobes though are asymmetrical with the right lobe usually larger. The gland itself is usually larger in women.[4] The thyroid sits near the front of the neck, lying against and around the larynx and trachea.[3] The top of the thyroid lies below the thyroid cartilage (just below the laryngeal prominence, or 'Adam's Apple'), and extends to the fifth or sixth tracheal ring. It is difficult to demarcate the gland's upper and lower border with vertebral levels because it moves position in relation to these during swallowing.[5] However it usually spans from C5 to C7.[4]
The thyroid gland is covered by a thin fibrous sheath, the capsule of the thyroid.[3] The external layer is anteriorly continuous with the pretracheal fascia and posterolaterally continuous with the carotid sheath.[citation needed] The capsule extrudes into the gland itself and forms the septae that divides the thyroid tissue into microscopic lobules.[3]
The gland is covered anteriorly with infrahyoid muscles and laterally with the sternocleidomastoid muscle also known as sternomastoid muscle. On the posterior side, the gland is fixed to the cricoid and tracheal cartilage and cricopharyngeus muscle by a thickening of the fascia to form the posterior suspensory ligament of thyroid gland also known as Berry's ligament.[6][7] The thyroid gland's firm attachment to the underlying trachea is the reason behind its movement with swallowing.[8]
In this region, the recurrent laryngeal nerve and the inferior thyroid artery pass next to or in the ligament and tubercle.[which?]
Two parathyroid glands usually lie on each side between the two layers of the capsule, at the back of the thyroid lobes.[3]
The thyroid is supplied with arterial blood from the superior thyroid artery, a branch of the external carotid artery, and the inferior thyroid artery, a branch of the thyrocervical trunk, and sometimes by an anatomical variant the thyroid ima artery, branching directly from the subclavian artery.[3] The superior thyroid artery splits into anterior and posterior branches supplying the thyroid, and the inferior thyroid artery splits into superior and inferior branches.[3] The venous blood is drained via superior and middle thyroid veins, which drain to the internal jugular vein, and via the inferior thyroid veins. The inferior thyroid veins originate in a network of veins and drain into the left and right brachiocephalic veins.[3]
Lymphatic drainage passes frequently the deep lateral cervical lymph nodes, and the pretracheal and paratracheal lymph nodes. The gland is supplied by parasympathetic nerve input from the superior laryngeal nerve and the recurrent laryngeal nerve.
There is quite often (28%-55% of population, mean 44.3%) a third lobe present called the pyramidal lobe of the thyroid gland.[9] It is cone-shaped and extends from the upper part of the isthmus, up across the thyroid cartilage to the hyoid bone. The pyramidal lobe is a remnant of the fetal thyroid stalk, or thyroglossal duct.[10] Sometimes the lobe is detached, or may be divided into two or more parts. The pyramidal lobe is also known as Lalouette's pyramid.[11]
The thyroid isthmus is variable in its situation and size and can also change in shape. It can encompass the pyramidal lobe (lobus or processus pyramidalis.[citation needed] In variable extent, the pyramidal lobe is present at the most anterior side of the lobe.
In the development of the embryo, at 3–4 weeks of gestation, the thyroid gland appears as an epithelial proliferation in the floor of the pharynx at the base of the tongue between the tuberculum impar and the copula linguae at a point later indicated by the foramen cecum. The thyroid then descends in front of the pharyngeal gut as a bilobed diverticulum through the thyroglossal duct. Over the next few weeks, it migrates to the base of the neck, passing anterior to the hyoid bone. During migration, the thyroid remains connected to the tongue by a narrow canal, the thyroglossal duct.
Thyrotropin-releasing hormone (TRH) and thyroid-stimulating hormone (TSH) start being secreted from the fetal hypothalamus and pituitary at 18-20 weeks of gestation, and fetal production of thyroxine (T4) reach a clinically significant level at 18–20 weeks.[12] Fetal triiodothyronine (T3) remains low (less than 15 ng/dL) until 30 weeks of gestation, and increases to 50 ng/dL at term.[12] Fetal self-sufficiency of thyroid hormones protects the fetus against (e.g., brain development abnormalities caused by maternal hypothyroidism).[13] However, preterm births can suffer neurodevelopmental disorders due to lack of maternal thyroid hormones due their own thyroid being insufficiently developed to meet their postnatal needs.[14]
While it was originally thought that the portion of the thyroid containing the parafollicular cells, also known as C cells, responsible for the production of calcitonin, are derived from neural crest, more recent research suggests that c-cells originate from pharyngeal endoderm. This is first seen as the ultimopharyngeal body, which begins in the ventral fourth pharyngeal pouch and joins the primordial thyroid gland during its descent to its final location in the anterior neck.
Aberrations in prenatal development can result in various forms of thyroid dysgenesis which can cause congenital hypothyroidism, and if untreated this can lead to cretinism.
At the microscopic level, there are three primary features of the thyroid—follicles, follicular cells, and parafollicular cells, first discovered by Geoffery Websterson in 1664.[15]
Follicles are small spherical groupings of cells 0.02-0.9mm in diameter that play the main role in thyroid function.[3] They consist of a rim that has a rich blood flow, nerve and lymphatic supply, that surrounds a core of colloid that consists mostly of thyroid hormone precursor proteins called thyroglobulin, an iodinated glycoprotein.[3][16]
The core of follicles is surrounded by a single layer of follicular cells. When stimulated by thyroid stimulating hormone (TSH), these secrete the thyroid hormones T3 and T4. They do this by transporting and metabolising the thyroglobulin contained in the colloid.[3] Follicular cells vary in shape from flat to cuboid to columnar, depending on how active they are.[3][16]
Scattered among follicular cells and in spaces between the spherical follicles are another type of thyroid cell, parafollicular cells.[3] These cells secrete calcitonin. Because the cytoplasm of these cells is clear, they are also called "C cells".[3]
The primary function of the thyroid is production of the thyroid hormones T3 and T4 and calcitonin. Up to 80% of the T4 is converted to T3 by organs such as the liver, kidney and spleen. T3 is several times more powerful than T4, which is largely a prohormone, perhaps four[17] or even ten times more active.[18]
T3 of particular physiological importance produced mainly in tissue after deiodination. It has calorigenic, cardiovascular, neural and other metabolic actions.
It increases oxygen consumption of all tissues except brain, uterus, testis (though it is important for normal fertility) lymph node, spleen, and its source, anterior pituitary, mainly by its action on sodium potassium pump and fat metabolism. It activates sodium potassium pump and increases sodium conductance, which further activating sodium potassium pump. It mobilises fatty acids from adipose tissue, resulting in decreased fat mass. Their increased catabolism increases O2 consumption.
It also increases O2 dissociation from haemoglobin by increasing red blood cell 2,3-BPG levels.
It increases body temperature, mainly by increasing metabolism and also activating uncoupler UCP-1 in inner mitochondrial membrane.
It can also increase blood glucose level, by increasing gluconeogenesis, and but same is utilised by increased uptake and glycolysis in tissue and increased insulin secretion.
It is helps in conversion of carotene into vitamin A in hepatic cells, therefore, hypothyroidism may lead to high levels of carotene in the blood, resulting in yellowish tint of only skin (and not the mucous membrane, like sclera) called as cartonemia. It increases vitamin requirements.
It increases growth and results in positive nitrogen usage in small quantities.
But high levels result in protein catabolism and negative nitrogen balance. Produced potassium due to catabolism appears in urine.
Decreased level of thyroid hormone result in retention of glycoproteins in the skin, which results in water retention (due to polyolic nature) and myxedema.
It also has significance in proper mentation. Increased levels results in irritability possibly due to activation of reticular system. Decreased levels results in poor mentation and increased protein level in CSF. It has significance in proper development of cochlea, basal ganglia and cerebral cortex. Hypothyroidism may lead to deaf-mutism, motor rigidity and mental retardation.
Many cardiovascular effects are reported. Decreased peripheral resistance, increased rate and force of heart beat occurs by effects of circulatory T3 .
It increases carbohydrate absorption from gastrointestinal system. It also increases gastrointestinal motility.
It is also reported to decrease cholesterol levels by up regulating LDL receptors on liver.
It is required for normal menstrual cycle in women.
It decreases reflex time.
Cells of the developing brain are a major target for the thyroid hormones T3 and T4. Thyroid hormones play a particularly crucial role in brain maturation during fetal development.[19] A transport protein that seems to be important for T4 transport across the blood–brain barrier (OATP1C1) has been identified.[20] A second transport protein (MCT8) is important for T3 transport across brain cell membranes.[20]
Non-genomic actions of T4 are those that are not initiated by liganding of the hormone to intranuclear thyroid receptor. These may begin at the plasma membrane or within cytoplasm. Plasma membrane-initiated actions begin at a receptor on the integrin alphaV beta3 that activates ERK1/2. This binding culminates in local membrane actions on ion transport systems such as the Na+/H+ exchanger or complex cellular events including cell proliferation. These integrins are concentrated on cells of the vasculature and on some types of tumor cells, which in part explains the proangiogenic effects of iodothyronines and proliferative actions of thyroid hormone on some cancers including gliomas. T4 also acts on the mitochondrial genome via imported isoforms of nuclear thyroid receptors to affect several mitochondrial transcription factors. Regulation of actin polymerization by T4 is critical to cell migration in neurons and glial cells and is important to brain development.
T3 can activate phosphatidylinositol 3-kinase by a mechanism that may be cytoplasmic in origin or may begin at integrin alpha V beta3.
In the blood, T4 and T3 are partially bound to thyroxine-binding globulin (TBG), transthyretin, and albumin. Only a very small fraction of the circulating hormone is free (unbound) - T4 0.03% and T3 0.3%. Only the free fraction has hormonal activity. As with the steroid hormones and retinoic acid, thyroid hormones cross the cell membrane and bind to intracellular receptors (α1, α2, β1 and β2), which act alone, in pairs or together with the retinoid X-receptor as transcription factors to modulate DNA transcription.[21]
Thyroxine (T4) is synthesised by the follicular cells from the tyrosine residues of the protein called thyroglobulin (Tg). It has 123 tyrosine residues, but only 4-6 are active. Iodine is captured with the "iodine trap" by the hydrogen peroxide generated by the enzyme thyroid peroxidase (TPO)[25] and linked to the 3' and 5' sites of the benzene ring of the tyrosine residues on Tg sequentially on tyrosine residue forming monoiodotyrosine (MIT) and then diiodotyrosine (DIT) (iodination). Two DIT can couple (coupling) to form T4 hormone attached to thyroglobulin releasing one alanine. Upon stimulation by the thyroid-stimulating hormone (TSH), the follicular cells reabsorb Tg and cleave the iodinated tyrosines from Tg in lysosomes, forming free T4, DIT, MIT, T3 and traces of RT3 (in T3 and RT3 has three iodine atom while T4 has four), and releasing T3 and T4 into the blood. Deiodinase releases the sequestred iodine from MIT and DIT. Deiodinase enzymes convert T4 to T3 and RT3, [26] which is a major source of both RT3 (95%) and T3 (87%) in peripheral tissues.[27] Thyroid hormone secreted from the gland is about 80-90% T4 and about 10-20% T3.[17][18]
Iodide—the ionized form of iodine—is essential for proper thyroid function. Iodide is taken up by follicular cells through the sodium-iodide symporter (NIS) present on the basolateral membrane, which transports two sodium cations and one iodide ion into the cell. It works against the iodide concentration gradient and uses energy of sodium gradient (maintained by the sodium-potassium pump) and therefore acts by secondary active transport. Thus, NIS help to maintain a 20- to 40-fold difference in iodide concentration across the membrane.[28] This iodide is transported to the follicular space through the apical membrane of the follicular cell with the help of the iodide-chloride antiporter pendrin. This iodide is then oxidized to iodine and attached to thyroglobulin by the enzyme thyroid peroxidase to form the precursors of thyroid hormones.[1]
The production of thyroxine and triiodothyronine is primarily regulated by thyroid-stimulating hormone (TSH), released by the anterior pituitary. The thyroid, and thyrotropes in the anterior pituitary, form a negative feedback loop: TSH production is suppressed when the free T4 levels are high. The negative feedback occurs on both the hypothalamus and the pituitary, but it is of particular importance at the level of the pituitary[29] The TSH production itself is modulated by thyrotropin-releasing hormone (TRH), which is produced by the hypothalamus. This is secreted at an increased rate in situations such as cold exposure (to stimulate thermogenesis) which is prominent in case of infants. TSH production is blunted by dopamine and somatostatin (SRIH) which act as local regulators at the level of the pituitary, in response to rising levels of glucocorticoids and sex hormones (estrogen and testosterone), and excessively high blood iodide concentration.
An additional hormone produced by the thyroid contributes to the regulation of blood calcium levels. Parafollicular cells produce calcitonin in response to hypercalcemia. Calcitonin stimulates movement of calcium into bone, in opposition to the effects of parathyroid hormone (PTH). However, calcitonin seems far less essential than PTH, as calcium metabolism remains clinically normal after removal of the thyroid (thyroidectomy), but not the parathyroids.
Thyroid disorders include
All these disorders may give rise to a goiter, that is, an enlarged thyroid.
In a healthy person the gland is not visible yet can be palpated as a soft mass. Examination of the thyroid gland includes the search for abnormal masses and the assessment of overall thyroid size.[30]
Test | Abbreviation | Normal ranges[31] |
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Serum thyrotropin/thyroid-stimulating hormone | TSH | 0.5–6.0 μU/ml |
Free thyroxine | FT4 | 7–18 ng/l = 0.7–1.8 ng/dl |
Serum triiodothyronine | T3 | 0.8–1.8 μg/l = 80–180 ng/dl |
Radioactive iodine-123 uptake | RAIU | 10–30% |
Radioiodine scan (gamma camera) | N/A | N/A - thyroid contrasted images |
Free thyroxine fraction | FT4F | 0.03–0.005% |
Serum thyroxine | T4 | 46–120 μg/l = 4.6–12.0 μg/dl |
Thyroid hormone binding ratio | THBR | 0.9–1.1 |
Free thyroxine index | FT4I | 4–11 |
Free triiodothyronine l | FT3 | 230–619 pg/d |
Free T3 Index | FT3I | 80–180 |
Thyroxine-binding globulin | TBG | 12–20 ug/dl T4 +1.8 μg |
TRH stimulation test | Peak TSH | 9–30 μIU/ml at 20–30 min. |
Serum thyroglobulin l | Tg | 0-30 ng/m |
Thyroid microsomal antibody titer | TMAb | Varies with method |
Thyroglobulin antibody titer | TgAb | Varies with method |
As of early 2015, in the United States, new guidelines for TSH levels have been implemented as endorsed by The American Association of Clinical Endocrinologists. The new range is a TSH of 0.45 to 4.12.[32]
Hyperthyroidism, or overactive thyroid, is defined as an overproduction of the thyroid hormones T3 and T4. This condition is most commonly caused by the development of Graves' disease, an autoimmune disease in which anomalous antibodies stimulate the thyroid to secrete excessive quantities of thyroid hormones.[33] The disease can progress to the formation of a toxic goiter as a result of thyroid growth in response to a lack of negative feedback mechanisms. It presents with symptoms such as a thyroid goiter, protruding eyes (exopthalmos), palpitations, excess sweating, diarrhea, weight loss, muscle weakness and unusual sensitivity to heat. The appetite is often increased.
Beta blockers can temporarily mitigate symptoms of hyperthyroidism such as increased heart rate, tremors, anxiety and heart palpitations, but long-term management of thyroid hormone levels may involve anti-thyroid drugs like methimazole and propylthiouracil, or radioactive iodine-131 treatment.[34] Radioactive iodine is selectively taken up by the thyroid, which over time destroys the cells involved in its uptake. Preferred first-line treatment varies by patient modality and country.[35]
Alternatively, the gland may be partially or entirely removed surgically, but this surgery is invasive and carries a risk of damage to the parathyroid glands and the nerves controlling the vocal cords. If the entire thyroid gland is removed, hypothyroidism results.[36]
Hypothyroidism is the underproduction of the thyroid hormones T3 and T4.
Hypothyroid disorders may occur as a result of
Typical symptoms are abnormal weight gain, tiredness, baldness, cold intolerance, and bradycardia. Hypothyroidism is treated with hormone replacement therapy, such as levothyroxine, which is typically required for the rest of the patient's life. Thyroid hormone treatment is given under the care of a physician and may take a few weeks to become effective.[37]
Negative feedback mechanisms result in growth of the thyroid gland when thyroid hormones are being produced in sufficiently low quantities, as a means of increasing the thyroid output; however, where hypothyroidism is caused by iodine insufficiency, the thyroid is unable to produce T3 and T4 and as a result, the thyroid may continue to grow to form a non-toxic goiter. It is termed non-toxic as it does not produce toxic quantities of thyroid hormones, despite its size.
Inflammation of the thyroid is called thyroiditis. There are two types of thyroiditis where initially hyperthyroidism presents which is followed by a period of hypothyroidism; (the overproduction of T3 and T4 followed by the underproduction of T3 and T4). These are Hashimoto's thyroiditis and postpartum thyroiditis.
Hashimoto's thyroiditis or Hashimoto's Disease is an autoimmune disorder whereby the body's own immune system reacts with the thyroid tissues in an attempt to destroy it. At the beginning, the gland may be overactive, and then becomes underactive as the gland is damaged resulting in too little thyroid hormone production or hypothyroidism. Some patients may experience "swings" in hormone levels that can progress rapidly from hyper-to-hypothyroid (sometimes mistaken as severe mood swings, or even being bipolar, before the proper clinical diagnosis is made). Some patients may experience these "swings" over a longer period of time, over days or weeks or even months. Hashimoto's is more common in females than males, usually appearing after the age of 30, and tends to run in families, meaning it can be seen as a genetic disease. Also more common in individuals with Hashimoto's thyroiditis are type 1 diabetes and celiac disease.[38]
Postpartum thyroiditis occurs in some females following the birth of a child. After delivery, the gland becomes inflamed and the condition initially presents with overactivity of the gland followed by underactivity. In some cases, the gland may recover with time and resume its functions. In others it may not. The etiology is not always known, but can sometimes be attributed to autoimmunity, such as Hashimoto's thyroiditis or Graves' disease.
There are other disorders that cause inflammation of the thyroid, and these include subacute thyroiditis, acute thyroiditis, silent thyroiditis and Riedel's thyroiditis.[39]
In most cases, thyroid cancer presents as a painless mass in the neck. It is very unusual for thyroid cancers to present with symptoms, unless they have been neglected. One may be able to feel a hard nodule in the neck. Diagnosis is made using a needle biopsy and various radiological studies.[40]
Thyroid nodules are often found on the gland. The majority of these nodules are benign (non cancerous), and their presence does not necessarily indicate disease. Most thyroid nodules do not cause any symptoms, and are mostly discovered on an incidental examination. Often there can be many nodules, which is termed a multinodular goiter. Doctors usually perform a needle aspiration biopsy of the thyroid to determine the status of the nodules. If the nodule is found to be non-cancerous, no other treatment is required. If the nodule is suspicious then surgery is recommended.
A persistent thyroglossal duct is the most common clinically significant congenital disorder of the thyroid gland. A persistent sinus tract may remain as a vestigial remnant of the tubular development of the thyroid gland. Parts of this tube may be obliterated, leaving small segments to form thyroglossal cysts. These occur at any age and might not become evident until adult life. Mucinous, clear secretions may collect within these cysts to form either spherical masses or fusiform swellings, rarely larger than 2 to 3 cm in diameter. These are present in the midline of the neck anterior to the trachea. Segments of the duct and cysts that occur high in the neck are lined by stratified squamous epithelium, which is essentially identical to that covering the posterior portion of the tongue in the region of the foramen cecum. The disorders that occur in the lower neck more proximal to the thyroid gland are lined by epithelium resembling the thyroidal acinar epithelium. Characteristically, next to the lining epithelium, there is an intense lymphocytic infiltrate. Superimposed infection may convert these lesions into abscess cavities, and rarely, give rise to cancers.[citation needed]
Another disorder is that of thyroid dysgenesis which can result in various presentations of one or more ectopic accessory thyroid glands. These can be asymptomatic.
In areas of the world where iodine is lacking in the diet, the thyroid gland can become considerably enlarged, a condition called endemic goiter. Pregnant women on a diet that is severely deficient of iodine can give birth to infants with thyroid hormone deficiency (congenital hypothyroidism), manifesting in problems of physical growth and development as well as brain development (a condition referred to as endemic cretinism). In many developed countries, newborns are routinely tested for congenital hypothyroidism as part of newborn screening. Children with congenital hypothyroidism are treated supplementally with levothyroxine, which facilitates normal growth and development.
Because the thyroid concentrates iodine, it also concentrates the various radioactive isotopes of iodine produced by nuclear fission. In the event of large accidental releases of such material into the environment, the uptake of radioactive iodine isotopes by the thyroid can, in theory, be blocked by saturating the uptake mechanism with a large surplus of non-radioactive iodine, taken in the form of potassium iodide tablets. One consequence of the Chernobyl disaster was an increase in thyroid cancers in children in the years following the accident.[42]
The use of iodised salt is an efficient way to add iodine to the diet. It has eliminated endemic cretinism in most developed countries, and some governments have made the iodination of flour, cooking oil, and salt mandatory. Potassium iodide and sodium iodide are typically used forms of supplemental iodine.
As with most substances, either too much or too little can cause problems. Recent studies on some populations are showing that excess iodine intake could cause an increased prevalence of autoimmune thyroid disease, resulting in permanent hypothyroidism.[43]
Historical references to what we now know as the thyroid gland arise early in medical history. In Ayurvedic medicine, the book Sushruta Samhita written about 1500 BC mentions the disease goitre as 'Galaganda' along with its treatment. In 1600 BC the Chinese were using burnt sponge and seaweed for the treatment of goitres (enlarged thyroid glands). Celsus first described a bronchoceole (a tumour of the neck) in 15 AD. Around this time Pliny referred to epidemics of goitre in the Alps and also mentioned the use of burnt seaweed in their treatment, in the same way as the Chinese had done 1600 years earlier. In 150 AD Galen, an instrumental figure in the transition from ancient to modern medicine, referred to 'spongia usta' (burnt sponge) for the treatment of goitre. He also suggested (incorrectly, as it turns out) that the role of the thyroid was to lubricate the larynx.
There are several findings that evidence a great interest for thyroid disorders just in the Medieval Medical School of Salerno (12th century). Rogerius Salernitanus, the Salernitan surgeon and author of "Post mundi fabricam" (around 1180) was considered at that time the surgical text par excellence all over Europe. In the chapter "De bocio" of his magnum opus, he describes several pharmacological and surgical cures, some of which nowadays are reappraised as scientifically effective.[44]
It was not until 1475 that Wang Hei anatomically described the thyroid gland and recommended that the treatment of goitre should be dried thyroid. Paracelsus, some fifty years later, attributed goitre to mineral impurities in the water.
In modern times, the thyroid was first identified in 1656 by the anatomist Thomas Wharton (whose name is also eponymised in Wharton's duct of the submandibular gland).[45] In 1656 Thomas Wharton named the gland the thyroid, meaning shield, as its shape resembled the shields commonly used in Ancient Greece.
In 1909, Theodor Kocher from Switzerland won the Nobel Prize in Medicine "for his work on the physiology, pathology and surgery of the thyroid gland".[46]
The English name thyroid gland[47] is derived from Latin glandula thyreoidea.[48] Glandula means gland in Latin,[49] and thyreoidea can be traced back to the Ancient Greek word θυρεοειδής, meaning shield-like/shield-shaped.[50]
The thyroid gland is found in all vertebrates. In fish, it is usually located below the gills and is not always divided into distinct lobes. However, in some teleosts, patches of thyroid tissue are found elsewhere in the body, associated with the kidneys, spleen, heart, or eyes.[51]
In tetrapods, the thyroid is always found somewhere in the neck region. In most tetrapod species, there are two paired thyroid glands - that is, the right and left lobes are not joined together. However, there is only ever a single thyroid gland in most mammals, and the shape found in humans is common to many other species.[51]
In larval lampreys, the thyroid originates as an exocrine gland, secreting its hormones into the gut, and associated with the larva's filter-feeding apparatus. In the adult lamprey, the gland separates from the gut, and becomes endocrine, but this path of development may reflect the evolutionary origin of the thyroid. For instance, the closest living relatives of vertebrates, the tunicates and Amphioxus, have a structure very similar to that of larval lampreys (the endostyle), and this also secretes iodine-containing compounds (albeit not thyroxine).[51]
Thyroxine is critical to the regulation of metabolism and growth throughout the animal kingdom. Among amphibians, for example, administering a thyroid-blocking agent such as propylthiouracil (PTU) can prevent tadpoles from metamorphosing into frogs; in contrast, administering thyroxine will trigger metamorphosis. In amphibian metamorphosis, thyroxine and iodine also exert a well-studied experimental model of apoptosis on the cells of gills, tail, and fins of tadpoles. Iodine, via iodolipids, has favored the evolution of terrestrial animal species and has likely played a crucial role in the evolution of the human brain. Iodine (and T4) trigger the amphibian metamorphosis that transforms the vegetarian aquatic tadpole into a carnivorous terrestrial adult frog, with better neurological, visuospatial, olfactory and cognitive abilities for hunting, as seen in other predatory animals. A similar phenomenon happens in the neotenic amphibian salamanders, which, without introducing iodine, don't transform into terrestrial adults, and live and reproduce in the larval form of aquatic axolotl.[52][53]
Thyroid and parathyroid.
Clearly visible pyramidal lobe of the thyroid
Thyroid gland
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Anatomy of the endocrine system
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