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Endocrine system

February 16, 2024

The endocrine system[1] is a messenger system in an organism comprising feedback loops of hormones that are released by internal glands directly into the circulatory system and that target and regulate distant organs. In vertebrates, the hypothalamus is the neural control center for all endocrine systems.

Endocrine system
Main glands of the human endocrine system
Details
Identifiers
Latinsystema endocrinum
MeSHD004703
FMA9668
Anatomical terminology
[edit on Wikidata]

In humans, the major endocrine glands are the thyroid, parathyroid, pituitary, pineal, and adrenal glands, and the (male) testicles and (female) ovaries. The hypothalamus, pancreas, and thymus also function as endocrine glands, among other functions. (The hypothalamus and pituitary glands are organs of the neuroendocrine system. One of the most important functions of the hypothalamus—it is located in the brain adjacent to the pituitary gland—is to link the endocrine system to the nervous system via the pituitary gland.) Other organs, such as the kidneys, also have roles within the endocrine system by secreting certain hormones. The study of the endocrine system and its disorders is known as endocrinology.[2]

Glands that signal each other in sequence are often referred to as an axis, such as the hypothalamic–pituitary–adrenal axis. In addition to the specialized endocrine organs mentioned above, many other organs that are part of other body systems have secondary endocrine functions, including bone, kidneys, liver, heart and gonads. For example, the kidney secretes the endocrine hormone erythropoietin. Hormones can be amino acid complexes, steroids, eicosanoids, leukotrienes, or prostaglandins.[3]

The endocrine system is contrasted both to exocrine glands, which secrete hormones to the outside of the body, and to the system known as paracrine signalling between cells over a relatively short distance. Endocrine glands have no ducts, are vascular, and commonly have intracellular vacuoles or granules that store their hormones. In contrast, exocrine glands, such as salivary glands, sweat glands, and glands within the gastrointestinal tract, tend to be much less vascular and have ducts or a hollow lumen. Endocrinology is a branch of internal medicine.[3]

Structure edit

Major endocrine systems edit

The human endocrine system consists of several systems that operate via feedback loops. Several important feedback systems are mediated via the hypothalamus and pituitary.[4]

Glands edit

Main article: Endocrine gland

Endocrine glands are glands of the endocrine system that secrete their products, hormones, directly into interstitial spaces where they are absorbed into blood rather than through a duct. The major glands of the endocrine system include the pineal gland, pituitary gland, pancreas, ovaries, testes, thyroid gland, parathyroid gland, hypothalamus and adrenal glands. The hypothalamus and pituitary gland are neuroendocrine organs.

The hypothalamus and the anterior pituitary are two out of the three endocrine glands that are important in cell signaling. They are both part of the HPA axis which is known to play a role in cell signaling in the nervous system.

Hypothalamus: The hypothalamus is a key regulator of the autonomic nervous system. The endocrine system has three sets of endocrine outputs[5] which include the magnocellular system, the parvocellular system, and autonomic intervention. The magnocellular is involved in the expression of oxytocin or vasopressin. The parvocellular is involved in controlling the secretion of hormones from the anterior pituitary.

Anterior Pituitary: The main role of the anterior pituitary gland is to produce and secrete tropic hormones.[6] Some examples of tropic hormones secreted by the anterior pituitary gland include TSH, ACTH, GH, LH, and FSH.

Cells edit

There are many types of cells that make up the endocrine system and these cells typically make up larger tissues and organs that function within and outside of the endocrine system.

Development edit

Main article: Development of the endocrine system

The fetal endocrine system is one of the first systems to develop during prenatal development.

Adrenal glands edit

The fetal adrenal cortex can be identified within four weeks of gestation. The adrenal cortex originates from the thickening of the intermediate mesoderm. At five to six weeks of gestation, the mesonephros differentiates into a tissue known as the genital ridge. The genital ridge produces the steroidogenic cells for both the gonads and the adrenal cortex. The adrenal medulla is derived from ectodermal cells. Cells that will become adrenal tissue move retroperitoneally to the upper portion of the mesonephros. At seven weeks of gestation, the adrenal cells are joined by sympathetic cells that originate from the neural crest to form the adrenal medulla. At the end of the eighth week, the adrenal glands have been encapsulated and have formed a distinct organ above the developing kidneys. At birth, the adrenal glands weigh approximately eight to nine grams (twice that of the adult adrenal glands) and are 0.5% of the total body weight. At 25 weeks, the adult adrenal cortex zone develops and is responsible for the primary synthesis of steroids during the early postnatal weeks.

Thyroid gland edit

The thyroid gland develops from two different clusterings of embryonic cells. One part is from the thickening of the pharyngeal floor, which serves as the precursor of the thyroxine (T4) producing follicular cells. The other part is from the caudal extensions of the fourth pharyngobranchial pouches which results in the parafollicular calcitonin-secreting cells. These two structures are apparent by 16 to 17 days of gestation. Around the 24th day of gestation, the foramen cecum, a thin, flask-like diverticulum of the median anlage develops. At approximately 24 to 32 days of gestation the median anlage develops into a bilobed structure. By 50 days of gestation, the medial and lateral anlage have fused together. At 12 weeks of gestation, the fetal thyroid is capable of storing iodine for the production of TRH, TSH, and free thyroid hormone. At 20 weeks, the fetus is able to implement feedback mechanisms for the production of thyroid hormones. During fetal development, T4 is the major thyroid hormone being produced while triiodothyronine (T3) and its inactive derivative, reverse T3, are not detected until the third trimester.

Parathyroid glands edit

A lateral and ventral view of an embryo showing the third (inferior) and fourth (superior) parathyroid glands during the 6th week of embryogenesis

Once the embryo reaches four weeks of gestation, the parathyroid glands begins to develop. The human embryo forms five sets of endoderm-lined pharyngeal pouches. The third and fourth pouch are responsible for developing into the inferior and superior parathyroid glands, respectively. The third pharyngeal pouch encounters the developing thyroid gland and they migrate down to the lower poles of the thyroid lobes. The fourth pharyngeal pouch later encounters the developing thyroid gland and migrates to the upper poles of the thyroid lobes. At 14 weeks of gestation, the parathyroid glands begin to enlarge from 0.1 mm in diameter to approximately 1 – 2 mm at birth. The developing parathyroid glands are physiologically functional beginning in the second trimester.

Studies in mice have shown that interfering with the HOX15 gene can cause parathyroid gland aplasia, which suggests the gene plays an important role in the development of the parathyroid gland. The genes, TBX1, CRKL, GATA3, GCM2, and SOX3 have also been shown to play a crucial role in the formation of the parathyroid gland. Mutations in TBX1 and CRKL genes are correlated with DiGeorge syndrome, while mutations in GATA3 have also resulted in a DiGeorge-like syndrome. Malformations in the GCM2 gene have resulted in hypoparathyroidism. Studies on SOX3 gene mutations have demonstrated that it plays a role in parathyroid development. These mutations also lead to varying degrees of hypopituitarism.

Pancreas edit

The human fetal pancreas begins to develop by the fourth week of gestation. Five weeks later, the pancreatic alpha and beta cells have begun to emerge. Reaching eight to ten weeks into development, the pancreas starts producing insulin, glucagon, somatostatin, and pancreatic polypeptide. During the early stages of fetal development, the number of pancreatic alpha cells outnumbers the number of pancreatic beta cells. The alpha cells reach their peak in the middle stage of gestation. From the middle stage until term, the beta cells continue to increase in number until they reach an approximate 1:1 ratio with the alpha cells. The insulin concentration within the fetal pancreas is 3.6 pmol/g at seven to ten weeks, which rises to 30 pmol/g at 16–25 weeks of gestation. Near term, the insulin concentration increases to 93 pmol/g. The endocrine cells have dispersed throughout the body within 10 weeks. At 31 weeks of development, the islets of Langerhans have differentiated.

While the fetal pancreas has functional beta cells by 14 to 24 weeks of gestation, the amount of insulin that is released into the bloodstream is relatively low. In a study of pregnant women carrying fetuses in the mid-gestation and near term stages of development, the fetuses did not have an increase in plasma insulin levels in response to injections of high levels of glucose. In contrast to insulin, the fetal plasma glucagon levels are relatively high and continue to increase during development. At the mid-stage of gestation, the glucagon concentration is 6 μg/g, compared to 2 μg/g in adult humans. Just like insulin, fetal glucagon plasma levels do not change in response to an infusion of glucose. However, a study of an infusion of alanine into pregnant women was shown to increase the cord blood and maternal glucagon concentrations, demonstrating a fetal response to amino acid exposure.

As such, while the fetal pancreatic alpha and beta islet cells have fully developed and are capable of hormone synthesis during the remaining fetal maturation, the islet cells are relatively immature in their capacity to produce glucagon and insulin. This is thought to be a result of the relatively stable levels of fetal serum glucose concentrations achieved via maternal transfer of glucose through the placenta. On the other hand, the stable fetal serum glucose levels could be attributed to the absence of pancreatic signaling initiated by incretins during feeding. In addition, the fetal pancreatic islets cells are unable to sufficiently produce cAMP and rapidly degrade cAMP by phosphodiesterase necessary to secrete glucagon and insulin.

During fetal development, the storage of glycogen is controlled by fetal glucocorticoids and placental lactogen. Fetal insulin is responsible for increasing glucose uptake and lipogenesis during the stages leading up to birth. Fetal cells contain a higher amount of insulin receptors in comparison to adults cells and fetal insulin receptors are not downregulated in cases of hyperinsulinemia. In comparison, fetal haptic glucagon receptors are lowered in comparison to adult cells and the glycemic effect of glucagon is blunted. This temporary physiological change aids the increased rate of fetal development during the final trimester. Poorly managed maternal diabetes mellitus is linked to fetal macrosomia, increased risk of miscarriage, and defects in fetal development. Maternal hyperglycemia is also linked to increased insulin levels and beta cell hyperplasia in the post-term infant. Children of diabetic mothers are at an increased risk for conditions such as: polycythemia, renal vein thrombosis, hypocalcemia, respiratory distress syndrome, jaundice, cardiomyopathy, congenital heart disease, and improper organ development.

Gonads edit

Main article: Development of the gonads

The reproductive system begins development at four to five weeks of gestation with germ cell migration. The bipotential gonad results from the collection of the medioventral region of the urogenital ridge. At the five-week point, the developing gonads break away from the adrenal primordium. Gonadal differentiation begins 42 days following conception.

Male gonadal development edit

For males, the testes form at six fetal weeks and the sertoli cells begin developing by the eight week of gestation. SRY, the sex-determining locus, serves to differentiate the Sertoli cells. The Sertoli cells are the point of origin for anti-Müllerian hormone. Once synthesized, the anti-Müllerian hormone initiates the ipsilateral regression of the Müllerian tract and inhibits the development of female internal features. At 10 weeks of gestation, the Leydig cells begin to produce androgen hormones. The androgen hormone dihydrotestosterone is responsible for the development of the male external genitalia.

The testicles descend during prenatal development in a two-stage process that begins at eight weeks of gestation and continues through the middle of the third trimester. During the transabdominal stage (8 to 15 weeks of gestation), the gubernacular ligament contracts and begins to thicken. The craniosuspensory ligament begins to break down. This stage is regulated by the secretion of insulin-like 3 (INSL3), a relaxin-like factor produced by the testicles, and the INSL3 G-coupled receptor, LGR8. During the transinguinal phase (25 to 35 weeks of gestation), the testicles descend into the scrotum. This stage is regulated by androgens, the genitofemoral nerve, and calcitonin gene-related peptide. During the second and third trimester, testicular development concludes with the diminution of the fetal Leydig cells and the lengthening and coiling of the seminiferous cords.

Female gonadal development edit

For females, the ovaries become morphologically visible by the 8th week of gestation. The absence of testosterone results in the diminution of the Wolffian structures. The Müllerian structures remain and develop into the fallopian tubes, uterus, and the upper region of the vagina. The urogenital sinus develops into the urethra and lower region of the vagina, the genital tubercle develops into the clitoris, the urogenital folds develop into the labia minora, and the urogenital swellings develop into the labia majora. At 16 weeks of gestation, the ovaries produce FSH and LH/hCG receptors. At 20 weeks of gestation, the theca cell precursors are present and oogonia mitosis is occurring. At 25 weeks of gestation, the ovary is morphologically defined and folliculogenesis can begin.

Studies of gene expression show that a specific complement of genes, such as follistatin and multiple cyclin kinase inhibitors are involved in ovarian development. An assortment of genes and proteins - such as WNT4, RSPO1, FOXL2, and various estrogen receptors - have been shown to prevent the development of testicles or the lineage of male-type cells.

Pituitary gland edit

The pituitary gland is formed within the rostral neural plate. The Rathke's pouch, a cavity of ectodermal cells of the oropharynx, forms between the fourth and fifth week of gestation and upon full development, it gives rise to the anterior pituitary gland. By seven weeks of gestation, the anterior pituitary vascular system begins to develop. During the first 12 weeks of gestation, the anterior pituitary undergoes cellular differentiation. At 20 weeks of gestation, the hypophyseal portal system has developed. The Rathke's pouch grows towards the third ventricle and fuses with the diverticulum. This eliminates the lumen and the structure becomes Rathke's cleft. The posterior pituitary lobe is formed from the diverticulum. Portions of the pituitary tissue may remain in the nasopharyngeal midline. In rare cases this results in functioning ectopic hormone-secreting tumors in the nasopharynx.

The functional development of the anterior pituitary involves spatiotemporal regulation of transcription factors expressed in pituitary stem cells and dynamic gradients of local soluble factors. The coordination of the dorsal gradient of pituitary morphogenesis is dependent on neuroectodermal signals from the infundibular bone morphogenetic protein 4 (BMP4). This protein is responsible for the development of the initial invagination of the Rathke's pouch. Other essential proteins necessary for pituitary cell proliferation are Fibroblast growth factor 8 (FGF8), Wnt4, and Wnt5. Ventral developmental patterning and the expression of transcription factors is influenced by the gradients of BMP2 and sonic hedgehog protein (SHH). These factors are essential for coordinating early patterns of cell proliferation.

Six weeks into gestation, the corticotroph cells can be identified. By seven weeks of gestation, the anterior pituitary is capable of secreting ACTH. Within eight weeks of gestation, somatotroph cells begin to develop with cytoplasmic expression of human growth hormone. Once a fetus reaches 12 weeks of development, the thyrotrophs begin expression of Beta subunits for TSH, while gonadotrophs being to express beta-subunits for LH and FSH. Male fetuses predominately produced LH-expressing gonadotrophs, while female fetuses produce an equal expression of LH and FSH expressing gonadotrophs. At 24 weeks of gestation, prolactin-expressing lactotrophs begin to emerge.

Function edit

See also: List of human endocrine organs and actions

Hormones edit

Main article: Hormone

A hormone is any of a class of signaling molecules produced by cells in glands in multicellular organisms that are transported by the circulatory system to target distant organs to regulate physiology and behaviour. Hormones have diverse chemical structures, mainly of 3 classes: eicosanoids, steroids, and amino acid/protein derivatives (amines, peptides, and proteins). The glands that secrete hormones comprise the endocrine system. The term hormone is sometimes extended to include chemicals produced by cells that affect the same cell (autocrine or intracrine signalling) or nearby cells (paracrine signalling).

Hormones are used to communicate between organs and tissues for physiological regulation and behavioral activities, such as digestion, metabolism, respiration, tissue function, sensory perception, sleep, excretion, lactation, stress, growth and development, movement, reproduction, and mood.[12][13]

Hormones affect distant cells by binding to specific receptor proteins in the target cell resulting in a change in cell function. This may lead to cell type-specific responses that include rapid changes to the activity of existing proteins, or slower changes in the expression of target genes. Amino acid–based hormones (amines and peptide or protein hormones) are water-soluble and act on the surface of target cells via signal transduction pathways; steroid hormones, being lipid-soluble, move through the plasma membranes of target cells to act within their nuclei.

Cell signalling edit

The typical mode of cell signalling in the endocrine system is endocrine signaling, that is, using the circulatory system to reach distant target organs. However, there are also other modes, i.e., paracrine, autocrine, and neuroendocrine signaling. Purely neurocrine signaling between neurons, on the other hand, belongs completely to the nervous system.

Autocrine edit

Main article: Autocrine signalling

Autocrine signaling is a form of signaling in which a cell secretes a hormone or chemical messenger (called the autocrine agent) that binds to autocrine receptors on the same cell, leading to changes in the cells.

Paracrine edit

Main article: Paracrine signalling

Some endocrinologists and clinicians include the paracrine system as part of the endocrine system, but there is not consensus. Paracrines are slower acting, targeting cells in the same tissue or organ. An example of this is somatostatin which is released by some pancreatic cells and targets other pancreatic cells.[3]

Juxtacrine edit

Main article: Juxtacrine signalling

Juxtacrine signaling is a type of intercellular communication that is transmitted via oligosaccharide, lipid, or protein components of a cell membrane, and may affect either the emitting cell or the immediately adjacent cells.[14]

It occurs between adjacent cells that possess broad patches of closely opposed plasma membrane linked by transmembrane channels known as connexons. The gap between the cells can usually be between only 2 and 4 nm.[15]

Clinical significance edit

Disease edit

 
Disability-adjusted life year for endocrine disorders per 100,000 inhabitants in 2002:[16]
  No data
  Less than 80
  80–160
  160–240
  240–320
  320–400
  400–480
  480–560
  560–640
  640–720
  720–800
  800–1000
  More than 1000
Main article: Endocrine diseases

Diseases of the endocrine system are common,[17] including conditions such as diabetes mellitus, thyroid disease, and obesity. Endocrine disease is characterized by misregulated hormone release (a productive pituitary adenoma), inappropriate response to signaling (hypothyroidism), lack of a gland (diabetes mellitus type 1, diminished erythropoiesis in chronic kidney failure), or structural enlargement in a critical site such as the thyroid (toxic multinodular goitre). Hypofunction of endocrine glands can occur as a result of loss of reserve, hyposecretion, agenesis, atrophy, or active destruction. Hyperfunction can occur as a result of hypersecretion, loss of suppression, hyperplastic or neoplastic change, or hyperstimulation.

Endocrinopathies are classified as primary, secondary, or tertiary. Primary endocrine disease inhibits the action of downstream glands. Secondary endocrine disease is indicative of a problem with the pituitary gland. Tertiary endocrine disease is associated with dysfunction of the hypothalamus and its releasing hormones.[18]

As the thyroid, and hormones have been implicated in signaling distant tissues to proliferate, for example, the estrogen receptor has been shown to be involved in certain breast cancers. Endocrine, paracrine, and autocrine signaling have all been implicated in proliferation, one of the required steps of oncogenesis.[19]

Other common diseases that result from endocrine dysfunction include Addison's disease, Cushing's disease and Graves' disease. Cushing's disease and Addison's disease are pathologies involving the dysfunction of the adrenal gland. Dysfunction in the adrenal gland could be due to primary or secondary factors and can result in hypercortisolism or hypocortisolism. Cushing's disease is characterized by the hypersecretion of the adrenocorticotropic hormone (ACTH) due to a pituitary adenoma that ultimately causes endogenous hypercortisolism by stimulating the adrenal glands.[20] Some clinical signs of Cushing's disease include obesity, moon face, and hirsutism.[21] Addison's disease is an endocrine disease that results from hypocortisolism caused by adrenal gland insufficiency. Adrenal insufficiency is significant because it is correlated with decreased ability to maintain blood pressure and blood sugar, a defect that can prove to be fatal.[22]

Graves' disease involves the hyperactivity of the thyroid gland which produces the T3 and T4 hormones.[21] Graves' disease effects range from excess sweating, fatigue, heat intolerance and high blood pressure to swelling of the eyes that causes redness, puffiness and in rare cases reduced or double vision.[15]

Other animals edit

A neuroendocrine system has been observed in all animals with a nervous system and all vertebrates have a hypothalamus–pituitary axis.[23] All vertebrates have a thyroid, which in amphibians is also crucial for transformation of larvae into adult form.[24][25] All vertebrates have adrenal gland tissue, with mammals unique in having it organized into layers.[26] All vertebrates have some form of a renin–angiotensin axis, and all tetrapods have aldosterone as a primary mineralocorticoid.[27][28]

Additional images edit

  •  
    Female endocrine system
  •  
    Male endocrine system

See also edit

References edit

  1. ^ "Anatomy of the Endocrine System". www.hopkinsmedicine.org. November 19, 2019. Retrieved June 14, 2022.
  2. ^ Gardner, Shoback (2017). Greenspan's Basic and Clinical Endocrinology (10th ed.). McGraw Hill / Medical. pp. 49–68. ISBN 978-1259589287.
  3. ^ a b c d Marieb E (2014). Anatomy & physiology. Glenview, IL: Pearson Education, Inc. ISBN 978-0-321-86158-0.
  4. ^ Sherwood, L. (1997). Human Physiology: From Cells to Systems. Wadsworth Pub Co. ISBN 978-0-495-39184-5.
  5. ^ Clifford B. Saper; Bradford B. Lowell (December 1, 2014). "The Hypothalamus". Current Biology. 24 (23): R1111-6. doi:10.1016/j.cub.2014.10.023. PMID 25465326. S2CID 18782796.
  6. ^ "Chapter 3. Anterior Pituitary Gland". Endocrine Physiology (4 ed.). McGraw Hill. 2013.
  7. ^ Quesada, Ivan (2008). "Physiology of the pancreatic α-cell and glucagon secretion: role in glucose homeostasis and diabetes". Journal of Endocrinology. 199 (1): 5–19. doi:10.1677/JOE-08-0290. PMID 18669612.
  8. ^ Patel, H.; Jessu, R.; Tiwari, V. (2021). "Physiology, Posterior Pituitary". How Does The Pancreas Work?. StatPearls. PMID 30252386. {{cite book}}: |website= ignored (help)
  9. ^ a b "267 Endocrine System Facts". Facts Legend. September 19, 2018.
  10. ^ Patel, H.; Jessu, R.; Tiwari, V. (2020). "Physiology, Posterior Pituitary". NCBI. StatPearls. PMID 30252386.
  11. ^ "Leydig cell | anatomy". Britannica. Retrieved June 14, 2022.
  12. ^ Neave N (2008). Hormones and behaviour: a psychological approach. Cambridge: Cambridge Univ. Press. ISBN 978-0-521-69201-4.
    • Claire L. Gibson (Winter 2010). "Hormones and Behaviour: A Psychological Approach". Perspectives in Biology and Medicine (Review). 53 (1): 152–155. doi:10.1353/pbm.0.0141. S2CID 72100830.
  13. ^ "Hormones". MedlinePlus. U.S. National Library of Medicine.
  14. ^ Gilbert F (2000). "Juxtacrine Signaling". Developmental Biology (6th ed.). Sunderland, MA: Sinauer Associates. ISBN 0-87893-243-7.
  15. ^ a b Vander A (2008). Vander's Human Physiology: the mechanisms of body function. Boston: McGraw-Hill Higher Education. pp. 332–333. ISBN 978-0-07-304962-5.
  16. ^ "Mortality and Burden of Disease Estimates for WHO Member States in 2002" (xls). World Health Organization. 2002.
  17. ^ Kasper DL, Harrison TR (2005). Harrison's Principles of Internal Medicine. McGraw Hill. pp. 2074. ISBN 978-0-07-139140-5.
  18. ^ Macksey LF (2012). Surgical procedures and anesthetic implications: a handbook for nurse anesthesia practice. Sudbury, MA: Jones & Bartlett Learning. p. 479. ISBN 978-0-7637-8057-9. OCLC 632070527.
  19. ^ Bhowmick NA, Chytil A, Plieth D, Gorska AE, Dumont N, Shappell S, Washington MK, Neilson EG, Moses HL (February 2004). "TGF-beta signaling in fibroblasts modulates the oncogenic potential of adjacent epithelia". Science. 303 (5659): 848–51. Bibcode:2004Sci...303..848B. doi:10.1126/science.1090922. PMID 14764882. S2CID 1703215.
  20. ^ Buliman A, Tataranu LG, Paun DL, Mirica A, Dumitrache C (2016). "Cushing's disease: a multidisciplinary overview of the clinical features, diagnosis, and treatment". Journal of Medicine and Life. 9 (1): 12–18. PMC 5152600. PMID 27974908.
  21. ^ a b Vander A (2008). Vander's Human Physiology: the mechanisms of body function. Boston: McGraw-Hill Higher Education. pp. 345–347. ISBN 978-0-07-304962-5.
  22. ^ Inder WJ, Meyer C, Hunt PJ (June 2015). "Management of hypertension and heart failure in patients with Addison's disease". Clinical Endocrinology. 82 (6): 789–92. doi:10.1111/cen.12592. PMID 25138826. S2CID 13552007.
  23. ^ Hartenstein V (September 2006). "The neuroendocrine system of invertebrates: a developmental and evolutionary perspective". The Journal of Endocrinology. 190 (3): 555–70. doi:10.1677/joe.1.06964. PMID 17003257.
  24. ^ Dickhoff WW, Darling DS (1983). "Evolution of Thyroid Function and Its Control in Lower Vertebrates". American Zoologist. 23 (3): 697–707. doi:10.1093/icb/23.3.697. JSTOR 3882951.
  25. ^ Galton VA (January 1, 1988). "The Role of Thyroid Hormone in Amphibian Development". Integrative and Comparative Biology. 28 (2): 309–18. doi:10.1093/icb/28.2.309. JSTOR 3883279.
  26. ^ Pohorecky LA, Wurtman RJ (March 1971). "Adrenocortical control of epinephrine synthesis". Pharmacological Reviews. 23 (1): 1–35. PMID 4941407.
  27. ^ Wilson JX (1984). "The renin-angiotensin system in nonmammalian vertebrates". Endocrine Reviews. 5 (1): 45–61. doi:10.1210/edrv-5-1-45. PMID 6368215.
  28. ^ Colombo L, Dalla Valle L, Fiore C, Armanini D, Belvedere P (April 2006). "Aldosterone and the conquest of land". Journal of Endocrinological Investigation. 29 (4): 373–9. doi:10.1007/bf03344112. PMID 16699307. S2CID 25316873.

External links edit

 
The Wikibook Human Physiology has a page on the topic of: The endocrine system
 
The Wikibook Anatomy and Physiology of Animals has a page on the topic of: Endocrine System
  •   Media related to Endocrine system at Wikimedia Commons

February 16, 2024
endocrine, system, endocrine, system, messenger, system, organism, comprising, feedback, loops, hormones, that, released, internal, glands, directly, into, circulatory, system, that, target, regulate, distant, organs, vertebrates, hypothalamus, neural, control. The endocrine system 1 is a messenger system in an organism comprising feedback loops of hormones that are released by internal glands directly into the circulatory system and that target and regulate distant organs In vertebrates the hypothalamus is the neural control center for all endocrine systems Endocrine systemMain glands of the human endocrine systemDetailsIdentifiersLatinsystema endocrinumMeSHD004703FMA9668Anatomical terminology edit on Wikidata In humans the major endocrine glands are the thyroid parathyroid pituitary pineal and adrenal glands and the male testicles and female ovaries The hypothalamus pancreas and thymus also function as endocrine glands among other functions The hypothalamus and pituitary glands are organs of the neuroendocrine system One of the most important functions of the hypothalamus it is located in the brain adjacent to the pituitary gland is to link the endocrine system to the nervous system via the pituitary gland Other organs such as the kidneys also have roles within the endocrine system by secreting certain hormones The study of the endocrine system and its disorders is known as endocrinology 2 Glands that signal each other in sequence are often referred to as an axis such as the hypothalamic pituitary adrenal axis In addition to the specialized endocrine organs mentioned above many other organs that are part of other body systems have secondary endocrine functions including bone kidneys liver heart and gonads For example the kidney secretes the endocrine hormone erythropoietin Hormones can be amino acid complexes steroids eicosanoids leukotrienes or prostaglandins 3 The endocrine system is contrasted both to exocrine glands which secrete hormones to the outside of the body and to the system known as paracrine signalling between cells over a relatively short distance Endocrine glands have no ducts are vascular and commonly have intracellular vacuoles or granules that store their hormones In contrast exocrine glands such as salivary glands sweat glands and glands within the gastrointestinal tract tend to be much less vascular and have ducts or a hollow lumen Endocrinology is a branch of internal medicine 3 Contents 1 Structure 1 1 Major endocrine systems 1 2 Glands 1 3 Cells 2 Development 2 1 Adrenal glands 2 2 Thyroid gland 2 3 Parathyroid glands 2 4 Pancreas 2 5 Gonads 2 5 1 Male gonadal development 2 5 2 Female gonadal development 2 6 Pituitary gland 3 Function 3 1 Hormones 3 2 Cell signalling 3 2 1 Autocrine 3 2 2 Paracrine 3 2 3 Juxtacrine 4 Clinical significance 4 1 Disease 5 Other animals 6 Additional images 7 See also 8 References 9 External linksStructure editMajor endocrine systems edit The human endocrine system consists of several systems that operate via feedback loops Several important feedback systems are mediated via the hypothalamus and pituitary 4 TRH TSH T3 T4 GnRH LH FSH sex hormones CRH ACTH cortisol Renin angiotensin aldosterone leptin vs GhrelinGlands edit Main article Endocrine gland Endocrine glands are glands of the endocrine system that secrete their products hormones directly into interstitial spaces where they are absorbed into blood rather than through a duct The major glands of the endocrine system include the pineal gland pituitary gland pancreas ovaries testes thyroid gland parathyroid gland hypothalamus and adrenal glands The hypothalamus and pituitary gland are neuroendocrine organs The hypothalamus and the anterior pituitary are two out of the three endocrine glands that are important in cell signaling They are both part of the HPA axis which is known to play a role in cell signaling in the nervous system Hypothalamus The hypothalamus is a key regulator of the autonomic nervous system The endocrine system has three sets of endocrine outputs 5 which include the magnocellular system the parvocellular system and autonomic intervention The magnocellular is involved in the expression of oxytocin or vasopressin The parvocellular is involved in controlling the secretion of hormones from the anterior pituitary Anterior Pituitary The main role of the anterior pituitary gland is to produce and secrete tropic hormones 6 Some examples of tropic hormones secreted by the anterior pituitary gland include TSH ACTH GH LH and FSH Cells edit There are many types of cells that make up the endocrine system and these cells typically make up larger tissues and organs that function within and outside of the endocrine system Hypothalamus Anterior pituitary gland Pineal gland Posterior pituitary gland The posterior pituitary gland is a section of the pituitary gland This organ does not produce any hormone but stores and secretes hormones such as antidiuretic hormone ADH which is synthesized by supraoptic nucleus of hypothalamus and oxytocin which is synthesized by paraventricular nucleus of hypothalamus ADH functions to help the body to retain water this is important in maintaining a homeostatic balance between blood solutions and water Oxytocin functions to induce uterine contractions stimulate lactation and allows for ejaculation 7 8 Thyroid gland follicular cells of the thyroid gland produce and secrete T3 and T4 in response to elevated levels of TRH produced by the hypothalamus and subsequent elevated levels of TSH produced by the anterior pituitary gland which further regulates the metabolic activity and rate of all cells including cell growth and tissue differentiation Parathyroid gland Epithelial cells of the parathyroid glands are richly supplied with blood from the inferior and superior thyroid arteries and secrete parathyroid hormone PTH PTH acts on bone the kidneys and the GI tract to increase calcium reabsorption and phosphate excretion In addition PTH stimulates the conversion of Vitamin D to its most active variant 1 25 dihydroxyvitamin D3 which further stimulates calcium absorption in the GI tract 3 Thymus Gland Adrenal glands Adrenal cortex Adrenal medulla Pancreas Pancreas contain nearly 1 to 2 million islets of Langerhans a tissue which consists cells that secrete hormones and acini Acini secretes digestive enzymes 9 Alpha cells The alpha cells of the pancreas secrete hormones to maintain homeostatic blood sugar Insulin is produced and excreted to lower blood sugar to normal levels Glucagon another hormone produced by alpha cells is secreted in response to low blood sugar levels glucagon stimulates glycogen stores in the liver to release sugar into the bloodstream to raise blood sugar to normal levels 10 Beta cells 60 of the cells present in islet of Langerhans are beta cells Beta cells secrete insulin Along with glucagon insulin helps in maintaining glucose levels in our body Insulin decreases blood glucose level a hypoglycemic hormone whereas glucagon increases blood glucose level 9 Delta cells F Cells Ovaries Granulosa cells Testis Leydig cells 11 Development editMain article Development of the endocrine system The fetal endocrine system is one of the first systems to develop during prenatal development Adrenal glands edit The fetal adrenal cortex can be identified within four weeks of gestation The adrenal cortex originates from the thickening of the intermediate mesoderm At five to six weeks of gestation the mesonephros differentiates into a tissue known as the genital ridge The genital ridge produces the steroidogenic cells for both the gonads and the adrenal cortex The adrenal medulla is derived from ectodermal cells Cells that will become adrenal tissue move retroperitoneally to the upper portion of the mesonephros At seven weeks of gestation the adrenal cells are joined by sympathetic cells that originate from the neural crest to form the adrenal medulla At the end of the eighth week the adrenal glands have been encapsulated and have formed a distinct organ above the developing kidneys At birth the adrenal glands weigh approximately eight to nine grams twice that of the adult adrenal glands and are 0 5 of the total body weight At 25 weeks the adult adrenal cortex zone develops and is responsible for the primary synthesis of steroids during the early postnatal weeks Thyroid gland edit The thyroid gland develops from two different clusterings of embryonic cells One part is from the thickening of the pharyngeal floor which serves as the precursor of the thyroxine T4 producing follicular cells The other part is from the caudal extensions of the fourth pharyngobranchial pouches which results in the parafollicular calcitonin secreting cells These two structures are apparent by 16 to 17 days of gestation Around the 24th day of gestation the foramen cecum a thin flask like diverticulum of the median anlage develops At approximately 24 to 32 days of gestation the median anlage develops into a bilobed structure By 50 days of gestation the medial and lateral anlage have fused together At 12 weeks of gestation the fetal thyroid is capable of storing iodine for the production of TRH TSH and free thyroid hormone At 20 weeks the fetus is able to implement feedback mechanisms for the production of thyroid hormones During fetal development T4 is the major thyroid hormone being produced while triiodothyronine T3 and its inactive derivative reverse T3 are not detected until the third trimester Parathyroid glands edit A lateral and ventral view of an embryo showing the third inferior and fourth superior parathyroid glands during the 6th week of embryogenesisOnce the embryo reaches four weeks of gestation the parathyroid glands begins to develop The human embryo forms five sets of endoderm lined pharyngeal pouches The third and fourth pouch are responsible for developing into the inferior and superior parathyroid glands respectively The third pharyngeal pouch encounters the developing thyroid gland and they migrate down to the lower poles of the thyroid lobes The fourth pharyngeal pouch later encounters the developing thyroid gland and migrates to the upper poles of the thyroid lobes At 14 weeks of gestation the parathyroid glands begin to enlarge from 0 1 mm in diameter to approximately 1 2 mm at birth The developing parathyroid glands are physiologically functional beginning in the second trimester Studies in mice have shown that interfering with the HOX15 gene can cause parathyroid gland aplasia which suggests the gene plays an important role in the development of the parathyroid gland The genes TBX1 CRKL GATA3 GCM2 and SOX3 have also been shown to play a crucial role in the formation of the parathyroid gland Mutations in TBX1 and CRKL genes are correlated with DiGeorge syndrome while mutations in GATA3 have also resulted in a DiGeorge like syndrome Malformations in the GCM2 gene have resulted in hypoparathyroidism Studies on SOX3 gene mutations have demonstrated that it plays a role in parathyroid development These mutations also lead to varying degrees of hypopituitarism Pancreas edit The human fetal pancreas begins to develop by the fourth week of gestation Five weeks later the pancreatic alpha and beta cells have begun to emerge Reaching eight to ten weeks into development the pancreas starts producing insulin glucagon somatostatin and pancreatic polypeptide During the early stages of fetal development the number of pancreatic alpha cells outnumbers the number of pancreatic beta cells The alpha cells reach their peak in the middle stage of gestation From the middle stage until term the beta cells continue to increase in number until they reach an approximate 1 1 ratio with the alpha cells The insulin concentration within the fetal pancreas is 3 6 pmol g at seven to ten weeks which rises to 30 pmol g at 16 25 weeks of gestation Near term the insulin concentration increases to 93 pmol g The endocrine cells have dispersed throughout the body within 10 weeks At 31 weeks of development the islets of Langerhans have differentiated While the fetal pancreas has functional beta cells by 14 to 24 weeks of gestation the amount of insulin that is released into the bloodstream is relatively low In a study of pregnant women carrying fetuses in the mid gestation and near term stages of development the fetuses did not have an increase in plasma insulin levels in response to injections of high levels of glucose In contrast to insulin the fetal plasma glucagon levels are relatively high and continue to increase during development At the mid stage of gestation the glucagon concentration is 6 mg g compared to 2 mg g in adult humans Just like insulin fetal glucagon plasma levels do not change in response to an infusion of glucose However a study of an infusion of alanine into pregnant women was shown to increase the cord blood and maternal glucagon concentrations demonstrating a fetal response to amino acid exposure As such while the fetal pancreatic alpha and beta islet cells have fully developed and are capable of hormone synthesis during the remaining fetal maturation the islet cells are relatively immature in their capacity to produce glucagon and insulin This is thought to be a result of the relatively stable levels of fetal serum glucose concentrations achieved via maternal transfer of glucose through the placenta On the other hand the stable fetal serum glucose levels could be attributed to the absence of pancreatic signaling initiated by incretins during feeding In addition the fetal pancreatic islets cells are unable to sufficiently produce cAMP and rapidly degrade cAMP by phosphodiesterase necessary to secrete glucagon and insulin During fetal development the storage of glycogen is controlled by fetal glucocorticoids and placental lactogen Fetal insulin is responsible for increasing glucose uptake and lipogenesis during the stages leading up to birth Fetal cells contain a higher amount of insulin receptors in comparison to adults cells and fetal insulin receptors are not downregulated in cases of hyperinsulinemia In comparison fetal haptic glucagon receptors are lowered in comparison to adult cells and the glycemic effect of glucagon is blunted This temporary physiological change aids the increased rate of fetal development during the final trimester Poorly managed maternal diabetes mellitus is linked to fetal macrosomia increased risk of miscarriage and defects in fetal development Maternal hyperglycemia is also linked to increased insulin levels and beta cell hyperplasia in the post term infant Children of diabetic mothers are at an increased risk for conditions such as polycythemia renal vein thrombosis hypocalcemia respiratory distress syndrome jaundice cardiomyopathy congenital heart disease and improper organ development Gonads edit Main article Development of the gonads The reproductive system begins development at four to five weeks of gestation with germ cell migration The bipotential gonad results from the collection of the medioventral region of the urogenital ridge At the five week point the developing gonads break away from the adrenal primordium Gonadal differentiation begins 42 days following conception Male gonadal development edit For males the testes form at six fetal weeks and the sertoli cells begin developing by the eight week of gestation SRY the sex determining locus serves to differentiate the Sertoli cells The Sertoli cells are the point of origin for anti Mullerian hormone Once synthesized the anti Mullerian hormone initiates the ipsilateral regression of the Mullerian tract and inhibits the development of female internal features At 10 weeks of gestation the Leydig cells begin to produce androgen hormones The androgen hormone dihydrotestosterone is responsible for the development of the male external genitalia The testicles descend during prenatal development in a two stage process that begins at eight weeks of gestation and continues through the middle of the third trimester During the transabdominal stage 8 to 15 weeks of gestation the gubernacular ligament contracts and begins to thicken The craniosuspensory ligament begins to break down This stage is regulated by the secretion of insulin like 3 INSL3 a relaxin like factor produced by the testicles and the INSL3 G coupled receptor LGR8 During the transinguinal phase 25 to 35 weeks of gestation the testicles descend into the scrotum This stage is regulated by androgens the genitofemoral nerve and calcitonin gene related peptide During the second and third trimester testicular development concludes with the diminution of the fetal Leydig cells and the lengthening and coiling of the seminiferous cords Female gonadal development edit For females the ovaries become morphologically visible by the 8th week of gestation The absence of testosterone results in the diminution of the Wolffian structures The Mullerian structures remain and develop into the fallopian tubes uterus and the upper region of the vagina The urogenital sinus develops into the urethra and lower region of the vagina the genital tubercle develops into the clitoris the urogenital folds develop into the labia minora and the urogenital swellings develop into the labia majora At 16 weeks of gestation the ovaries produce FSH and LH hCG receptors At 20 weeks of gestation the theca cell precursors are present and oogonia mitosis is occurring At 25 weeks of gestation the ovary is morphologically defined and folliculogenesis can begin Studies of gene expression show that a specific complement of genes such as follistatin and multiple cyclin kinase inhibitors are involved in ovarian development An assortment of genes and proteins such as WNT4 RSPO1 FOXL2 and various estrogen receptors have been shown to prevent the development of testicles or the lineage of male type cells Pituitary gland edit The pituitary gland is formed within the rostral neural plate The Rathke s pouch a cavity of ectodermal cells of the oropharynx forms between the fourth and fifth week of gestation and upon full development it gives rise to the anterior pituitary gland By seven weeks of gestation the anterior pituitary vascular system begins to develop During the first 12 weeks of gestation the anterior pituitary undergoes cellular differentiation At 20 weeks of gestation the hypophyseal portal system has developed The Rathke s pouch grows towards the third ventricle and fuses with the diverticulum This eliminates the lumen and the structure becomes Rathke s cleft The posterior pituitary lobe is formed from the diverticulum Portions of the pituitary tissue may remain in the nasopharyngeal midline In rare cases this results in functioning ectopic hormone secreting tumors in the nasopharynx The functional development of the anterior pituitary involves spatiotemporal regulation of transcription factors expressed in pituitary stem cells and dynamic gradients of local soluble factors The coordination of the dorsal gradient of pituitary morphogenesis is dependent on neuroectodermal signals from the infundibular bone morphogenetic protein 4 BMP4 This protein is responsible for the development of the initial invagination of the Rathke s pouch Other essential proteins necessary for pituitary cell proliferation are Fibroblast growth factor 8 FGF8 Wnt4 and Wnt5 Ventral developmental patterning and the expression of transcription factors is influenced by the gradients of BMP2 and sonic hedgehog protein SHH These factors are essential for coordinating early patterns of cell proliferation Six weeks into gestation the corticotroph cells can be identified By seven weeks of gestation the anterior pituitary is capable of secreting ACTH Within eight weeks of gestation somatotroph cells begin to develop with cytoplasmic expression of human growth hormone Once a fetus reaches 12 weeks of development the thyrotrophs begin expression of Beta subunits for TSH while gonadotrophs being to express beta subunits for LH and FSH Male fetuses predominately produced LH expressing gonadotrophs while female fetuses produce an equal expression of LH and FSH expressing gonadotrophs At 24 weeks of gestation prolactin expressing lactotrophs begin to emerge Function editSee also List of human endocrine organs and actions Hormones edit Main article Hormone A hormone is any of a class of signaling molecules produced by cells in glands in multicellular organisms that are transported by the circulatory system to target distant organs to regulate physiology and behaviour Hormones have diverse chemical structures mainly of 3 classes eicosanoids steroids and amino acid protein derivatives amines peptides and proteins The glands that secrete hormones comprise the endocrine system The term hormone is sometimes extended to include chemicals produced by cells that affect the same cell autocrine or intracrine signalling or nearby cells paracrine signalling Hormones are used to communicate between organs and tissues for physiological regulation and behavioral activities such as digestion metabolism respiration tissue function sensory perception sleep excretion lactation stress growth and development movement reproduction and mood 12 13 Hormones affect distant cells by binding to specific receptor proteins in the target cell resulting in a change in cell function This may lead to cell type specific responses that include rapid changes to the activity of existing proteins or slower changes in the expression of target genes Amino acid based hormones amines and peptide or protein hormones are water soluble and act on the surface of target cells via signal transduction pathways steroid hormones being lipid soluble move through the plasma membranes of target cells to act within their nuclei Cell signalling edit The typical mode of cell signalling in the endocrine system is endocrine signaling that is using the circulatory system to reach distant target organs However there are also other modes i e paracrine autocrine and neuroendocrine signaling Purely neurocrine signaling between neurons on the other hand belongs completely to the nervous system Autocrine edit Main article Autocrine signalling Autocrine signaling is a form of signaling in which a cell secretes a hormone or chemical messenger called the autocrine agent that binds to autocrine receptors on the same cell leading to changes in the cells Paracrine edit Main article Paracrine signalling Some endocrinologists and clinicians include the paracrine system as part of the endocrine system but there is not consensus Paracrines are slower acting targeting cells in the same tissue or organ An example of this is somatostatin which is released by some pancreatic cells and targets other pancreatic cells 3 Juxtacrine edit Main article Juxtacrine signalling Juxtacrine signaling is a type of intercellular communication that is transmitted via oligosaccharide lipid or protein components of a cell membrane and may affect either the emitting cell or the immediately adjacent cells 14 It occurs between adjacent cells that possess broad patches of closely opposed plasma membrane linked by transmembrane channels known as connexons The gap between the cells can usually be between only 2 and 4 nm 15 Clinical significance editDisease edit nbsp Disability adjusted life year for endocrine disorders per 100 000 inhabitants in 2002 16 No data Less than 80 80 160 160 240 240 320 320 400 400 480 480 560 560 640 640 720 720 800 800 1000 More than 1000Main article Endocrine diseases Diseases of the endocrine system are common 17 including conditions such as diabetes mellitus thyroid disease and obesity Endocrine disease is characterized by misregulated hormone release a productive pituitary adenoma inappropriate response to signaling hypothyroidism lack of a gland diabetes mellitus type 1 diminished erythropoiesis in chronic kidney failure or structural enlargement in a critical site such as the thyroid toxic multinodular goitre Hypofunction of endocrine glands can occur as a result of loss of reserve hyposecretion agenesis atrophy or active destruction Hyperfunction can occur as a result of hypersecretion loss of suppression hyperplastic or neoplastic change or hyperstimulation Endocrinopathies are classified as primary secondary or tertiary Primary endocrine disease inhibits the action of downstream glands Secondary endocrine disease is indicative of a problem with the pituitary gland Tertiary endocrine disease is associated with dysfunction of the hypothalamus and its releasing hormones 18 As the thyroid and hormones have been implicated in signaling distant tissues to proliferate for example the estrogen receptor has been shown to be involved in certain breast cancers Endocrine paracrine and autocrine signaling have all been implicated in proliferation one of the required steps of oncogenesis 19 Other common diseases that result from endocrine dysfunction include Addison s disease Cushing s disease and Graves disease Cushing s disease and Addison s disease are pathologies involving the dysfunction of the adrenal gland Dysfunction in the adrenal gland could be due to primary or secondary factors and can result in hypercortisolism or hypocortisolism Cushing s disease is characterized by the hypersecretion of the adrenocorticotropic hormone ACTH due to a pituitary adenoma that ultimately causes endogenous hypercortisolism by stimulating the adrenal glands 20 Some clinical signs of Cushing s disease include obesity moon face and hirsutism 21 Addison s disease is an endocrine disease that results from hypocortisolism caused by adrenal gland insufficiency Adrenal insufficiency is significant because it is correlated with decreased ability to maintain blood pressure and blood sugar a defect that can prove to be fatal 22 Graves disease involves the hyperactivity of the thyroid gland which produces the T3 and T4 hormones 21 Graves disease effects range from excess sweating fatigue heat intolerance and high blood pressure to swelling of the eyes that causes redness puffiness and in rare cases reduced or double vision 15 Other animals editA neuroendocrine system has been observed in all animals with a nervous system and all vertebrates have a hypothalamus pituitary axis 23 All vertebrates have a thyroid which in amphibians is also crucial for transformation of larvae into adult form 24 25 All vertebrates have adrenal gland tissue with mammals unique in having it organized into layers 26 All vertebrates have some form of a renin angiotensin axis and all tetrapods have aldosterone as a primary mineralocorticoid 27 28 Additional images edit nbsp Female endocrine system nbsp Male endocrine systemSee also editEndocrine disease Endocrinology List of human endocrine organs and actions Neuroendocrinology Nervous system Paracrine signalling Releasing hormones Tropic hormoneReferences edit Anatomy of the Endocrine System www hopkinsmedicine org November 19 2019 Retrieved June 14 2022 Gardner Shoback 2017 Greenspan s Basic and Clinical Endocrinology 10th ed McGraw Hill Medical pp 49 68 ISBN 978 1259589287 a b c d Marieb E 2014 Anatomy amp physiology Glenview IL Pearson Education Inc ISBN 978 0 321 86158 0 Sherwood L 1997 Human Physiology From Cells to Systems Wadsworth Pub Co ISBN 978 0 495 39184 5 Clifford B Saper Bradford B Lowell December 1 2014 The Hypothalamus Current Biology 24 23 R1111 6 doi 10 1016 j cub 2014 10 023 PMID 25465326 S2CID 18782796 Chapter 3 Anterior Pituitary Gland Endocrine Physiology 4 ed McGraw Hill 2013 Quesada Ivan 2008 Physiology of the pancreatic a cell and glucagon secretion role in glucose homeostasis and diabetes Journal of Endocrinology 199 1 5 19 doi 10 1677 JOE 08 0290 PMID 18669612 Patel H Jessu R Tiwari V 2021 Physiology Posterior Pituitary How Does The Pancreas Work StatPearls PMID 30252386 a href Template Cite book html title Template Cite book cite book a website ignored help a b 267 Endocrine System Facts Facts Legend September 19 2018 Patel H Jessu R Tiwari V 2020 Physiology Posterior Pituitary NCBI StatPearls PMID 30252386 Leydig cell anatomy Britannica Retrieved June 14 2022 Neave N 2008 Hormones and behaviour a psychological approach Cambridge Cambridge Univ Press ISBN 978 0 521 69201 4 Claire L Gibson Winter 2010 Hormones and Behaviour A Psychological Approach Perspectives in Biology and Medicine Review 53 1 152 155 doi 10 1353 pbm 0 0141 S2CID 72100830 Hormones MedlinePlus U S National Library of Medicine Gilbert F 2000 Juxtacrine Signaling Developmental Biology 6th ed Sunderland MA Sinauer Associates ISBN 0 87893 243 7 a b Vander A 2008 Vander s Human Physiology the mechanisms of body function Boston McGraw Hill Higher Education pp 332 333 ISBN 978 0 07 304962 5 Mortality and Burden of Disease Estimates for WHO Member States in 2002 xls World Health Organization 2002 Kasper DL Harrison TR 2005 Harrison s Principles of Internal Medicine McGraw Hill pp 2074 ISBN 978 0 07 139140 5 Macksey LF 2012 Surgical procedures and anesthetic implications a handbook for nurse anesthesia practice Sudbury MA Jones amp Bartlett Learning p 479 ISBN 978 0 7637 8057 9 OCLC 632070527 Bhowmick NA Chytil A Plieth D Gorska AE Dumont N Shappell S Washington MK Neilson EG Moses HL February 2004 TGF beta signaling in fibroblasts modulates the oncogenic potential of adjacent epithelia Science 303 5659 848 51 Bibcode 2004Sci 303 848B doi 10 1126 science 1090922 PMID 14764882 S2CID 1703215 Buliman A Tataranu LG Paun DL Mirica A Dumitrache C 2016 Cushing s disease a multidisciplinary overview of the clinical features diagnosis and treatment Journal of Medicine and Life 9 1 12 18 PMC 5152600 PMID 27974908 a b Vander A 2008 Vander s Human Physiology the mechanisms of body function Boston McGraw Hill Higher Education pp 345 347 ISBN 978 0 07 304962 5 Inder WJ Meyer C Hunt PJ June 2015 Management of hypertension and heart failure in patients with Addison s disease Clinical Endocrinology 82 6 789 92 doi 10 1111 cen 12592 PMID 25138826 S2CID 13552007 Hartenstein V September 2006 The neuroendocrine system of invertebrates a developmental and evolutionary perspective The Journal of Endocrinology 190 3 555 70 doi 10 1677 joe 1 06964 PMID 17003257 Dickhoff WW Darling DS 1983 Evolution of Thyroid Function and Its Control in Lower Vertebrates American Zoologist 23 3 697 707 doi 10 1093 icb 23 3 697 JSTOR 3882951 Galton VA January 1 1988 The Role of Thyroid Hormone in Amphibian Development Integrative and Comparative Biology 28 2 309 18 doi 10 1093 icb 28 2 309 JSTOR 3883279 Pohorecky LA Wurtman RJ March 1971 Adrenocortical control of epinephrine synthesis Pharmacological Reviews 23 1 1 35 PMID 4941407 Wilson JX 1984 The renin angiotensin system in nonmammalian vertebrates Endocrine Reviews 5 1 45 61 doi 10 1210 edrv 5 1 45 PMID 6368215 Colombo L Dalla Valle L Fiore C Armanini D Belvedere P April 2006 Aldosterone and the conquest of land Journal of Endocrinological Investigation 29 4 373 9 doi 10 1007 bf03344112 PMID 16699307 S2CID 25316873 External links edit nbsp The Wikibook Human Physiology has a page on the topic of The endocrine system nbsp The Wikibook Anatomy and Physiology of Animals has a page on the topic of Endocrine System nbsp Media related to Endocrine system at Wikimedia Commons Retrieved from https en wikipedia org w index php title Endocrine system amp oldid 1189643607, wikipedia, wiki, book, books, library,

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