Endocrine system
Endocrine system | |
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Main glands of the endocrine system | |
Details | |
Identifiers | |
Latin | Systema endocrinum |
FMA | 9668 |
The endocrine system refers to the collection of glands of an organism that secrete hormones directly into the circulatory system to be carried towards distant target organs. The major endocrine glands include the pineal gland, pituitary gland, pancreas, ovaries, testes, thyroid gland, parathyroid gland, hypothalamus, gastrointestinal tract and adrenal glands. The endocrine system is in contrast to the exocrine system, which secretes its hormones to the outside of the body using ducts. The endocrine system is an information signal system like the nervous system, yet its effects and mechanism are classifiably different. The endocrine system's effects are slow to initiate, and prolonged in their response, lasting from a few hours up to weeks. The nervous system sends information very quickly, and responses are generally short lived. In vertebrates, the hypothalamus is the neural control center for all endocrine systems. The field of study dealing with the endocrine system and its disorders is endocrinology, a branch of internal medicine.[1] Special features of endocrine glands are, in general, their ductless nature, their vascularity, and commonly the presence of 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.
In addition to the specialized endocrine organs mentioned above, many other organs that are part of other body systems, such as bone, kidney, liver, heart and gonads, have secondary endocrine functions. For example, the kidney secretes endocrine hormones such as erythropoietin and renin. Hormones can consist of either amino acid complexes, steroids, eicosanoids, leukotrienes, or prostaglandins.[1]
A number of glands that signal each other in sequence are usually referred to as an axis, for example, the hypothalamic-pituitary-adrenal axis.
As opposed to endocrine factors that travel considerably longer distances via the circulatory system, other signaling molecules, such as paracrine factors involved in paracrine signalling diffuse over a relatively short distance.
The word endocrine derives from the Greek words ἐνδο- endo- "inside, within," and κρίνειν krinein "to separate, distinguish".
Endocrine organs and known secreted hormones
Hypothalamus
Pineal body (epiphysis)
Secreted hormone | From cells | Effect |
---|---|---|
Melatonin | Pinealocytes | Antioxidant Monitors the circadian rhythm including induction of drowsiness and lowering of the core body temperature |
Pituitary gland (hypophysis)
The pituitary gland (or hypophysis) is an endocrine gland about the size of a pea and weighing 0.5 grams (0.018 oz) in humans. It is a protrusion off the bottom of the hypothalamus at the base of the brain, and rests in a small, bony cavity (sella turcica) covered by a dural fold (diaphragma sellae). The pituitary is functionally connected to the hypothalamus by the median eminence via a small tube called the infundibular stem or pituitary stalk. The pituitary fossa, in which the pituitary gland sits, is situated in the sphenoid bone in the middle cranial fossa at the base of the brain. The pituitary gland secretes nine hormones that regulate homeostasis and the secretion of other hormones.
Anterior pituitary lobe (adenohypophysis)
Secreted hormone | Abbreviation | From cells | Effect |
---|---|---|---|
Growth hormone (somatotropin) |
GH | Somatotrophs | Stimulates growth and cell reproduction Stimulates Insulin-like growth factor 1 release from liver |
Thyroid-stimulating hormone (thyrotropin) |
TSH | Thyrotrophs | Stimulates thyroxine (T4) and triiodothyronine (T3) synthesis and release from thyroid gland Stimulates iodine absorption by thyroid gland |
Adrenocorticotropic hormone (corticotropin) |
ACTH | Corticotrophs | Stimulates corticosteroid (glucocorticoid and mineralcorticoid) and androgen synthesis and release from adrenocortical cells |
Beta-endorphin | – | Corticotrophs | Inhibits perception of pain |
Follicle-stimulating hormone | FSH | Gonadotrophs | In females: Stimulates maturation of ovarian follicles in ovary In males: Stimulates maturation of seminiferous tubules In males: Stimulates spermatogenesis In males: Stimulates production of androgen-binding protein from Sertoli cells of the testes |
Luteinizing hormone | LH | Gonadotrophs | In females: Stimulates ovulation In females: Stimulates formation of corpus luteum In males: Stimulates testosterone synthesis from Leydig cells (interstitial cells) |
Prolactin | PRL | Lactotrophs | Stimulates milk synthesis and release from mammary glands Mediates sexual gratification |
Melanocyte-stimulating hormone | MSH | Melanotropes in the Pars intermedia of the Anterior Pituitary | Stimulates melanin synthesis and release from skin/hair melanocytes |
Posterior pituitary lobe (neurohypophysis)
Stored hormone | Abbreviation | From cells | Effect |
---|---|---|---|
Oxytocin | Magnocellular neurosecretory cells | In females: uterine contraction during birthing, lactation (letdown reflex) when nursing | |
Vasopressin (antidiuretic hormone) |
ADH or AVP | Parvocellular neurosecretory neurons | Increases water permeability in the distal convoluted tubule and collecting duct of nephrons, thus promoting water reabsorption and increasing blood volume |
Oxytocin and anti-diuretic hormone are not secreted in the posterior lobe, merely stored.
Thyroid
Secreted hormone | Abbreviation | From cells | Effect |
---|---|---|---|
Triiodothyronine | T3 | Thyroid epithelial cell | (More potent form of thyroid hormone) Stimulates body oxygen and energy consumption, thereby increasing the basal metabolic rate Stimulates RNA polymerase I and II, thereby promoting protein synthesis |
Thyroxine (tetraiodothyronine) |
T4 | Thyroid epithelial cells | (Less active form of thyroid hormone) (Acts as a prohormone to triiodothyronine) Stimulates body oxygen and energy consumption, thereby increasing the basal metabolic rate Stimulates RNA polymerase I and II, thereby promoting protein synthesis |
Calcitonin | Parafollicular cells | Stimulates osteoblasts and thus bone construction Inhibits Ca2+ release from bone, thereby reducing blood Ca2+ |
Digestive system
Stomach
Secreted hormone | Abbreviation | From cells | Effect |
---|---|---|---|
Gastrin (Primarily) | G cells | Secretion of gastric acid by parietal cells | |
Ghrelin | P/D1 cells | Stimulate appetite. | |
Neuropeptide Y | NPY | Increased food intake and decreased physical activity. It can be associated with obesity. | |
Somatostatin | D cells | Suppress release of gastrin, cholecystokinin (CCK), secretin, motilin, vasoactive intestinal peptide (VIP), gastric inhibitory polypeptide (GIP), enteroglucagon
Lowers rate of gastric emptying Reduces smooth muscle contractions and blood flow within the intestine.[2] | |
Histamine | ECL cells | stimulate gastric acid secretion | |
Endothelin | X cells | Smooth muscle contraction of stomach[3] |
Duodenum (small intestine)
Secreted hormone | From cells | Effect |
---|---|---|
Secretin | S cells | Secretion of bicarbonate from liver, pancreas and duodenal Brunner's glands
Enhances effects of cholecystokinin, stops production of gastric juice |
Cholecystokinin | I cells | Release of digestive enzymes from pancreas
Release of bile from gallbladder, hunger suppressant |
Liver
Secreted hormone | Abbreviation | From cells | Effect |
---|---|---|---|
Insulin-like growth factor (or somatomedin) (Primarily) | IGF | Hepatocytes | insulin-like effects
regulate cell growth and development |
Angiotensinogen and angiotensin | Hepatocytes | vasoconstriction
release of aldosterone from adrenal cortex dipsogen. | |
Thrombopoietin | THPO | Hepatocytes | stimulates megakaryocytes to produce platelets[4] |
Hepcidin | Hepatocytes | inhibits intestinal iron absorption and iron release by macrophages |
Pancreas
The pancreas is a mixocrine gland and it secretes both enzymes and hormones.
Secreted hormone | From cells | Effect |
---|---|---|
Insulin (Primarily) | β Islet cells | Intake of glucose, glycogenesis and glycolysis in liver and muscle from blood.
Intake of lipids and synthesis of triglycerides in adipocytes. Other anabolic effects |
Glucagon (Also Primarily) | α Islet cells | Glycogenolysis and gluconeogenesis in liver.
Increases blood glucose level. |
Somatostatin | δ Islet cells | Inhibit release of insulin[5]
Inhibit release of glucagon[5] Suppress the exocrine secretory action of pancreas. |
Pancreatic polypeptide | PP cells | Self regulate the pancreas secretion activities and effect the hepatic glycogen levels. |
Kidney
Secreted hormone | From cells | Effect |
---|---|---|
Renin (Primarily) | Juxtaglomerular cells | Activates the renin-angiotensin system by producing angiotensin I of angiotensinogen |
Erythropoietin (EPO) | Extraglomerular mesangial cells | Stimulate erythrocyte production |
Calcitriol (1,25-dihydroxyvitamin D3) | Active form of vitamin D3
Increase absorption of calcium and phosphate from gastrointestinal tract and kidneys inhibit release of PTH | |
Thrombopoietin | stimulates megakaryocytes to produce platelets[4] |
Adrenal glands
Adrenal cortex
Secreted hormone | From cells | Effect |
---|---|---|
Glucocorticoids (chiefly cortisol) | zona fasciculata and zona reticularis cells | Stimulates gluconeogenesis Stimulates fat breakdown in adipose tissue Inhibits protein synthesis Inhibits glucose uptake in muscle and adipose tissue Inhibits immunological responses (immunosuppressive) Inhibits inflammatory responses (anti-inflammatory) |
Mineralocorticoids (chiefly aldosterone) | Zona glomerulosa cells | Stimulates active sodium reabsorption in kidneys Stimulates passive water reabsorption in kidneys, thus increasing blood volume and blood pressure Stimulates potassium and H+ secretion into nephron of kidney and subsequent excretion |
Androgens (including DHEA and testosterone) | Zona fasciculata and Zona reticularis cells | In males: Relatively small effect compared to androgens from testes In females: masculinizing effects |
Adrenal medulla
Secreted hormone | From cells | Effect |
---|---|---|
Adrenaline (epinephrine) (Primarily) | Chromaffin cells | Fight-or-flight response:
|
Noradrenaline (norepinephrine) | Chromaffin cells | Fight-or-flight response:
|
Dopamine | Chromaffin cells | Increase heart rate and blood pressure |
Enkephalin | Chromaffin cells | Regulate pain |
Reproductive
Testes
Secreted hormone | From cells | Effect |
---|---|---|
Androgens (chiefly testosterone) | Leydig cells | Anabolic: growth of muscle mass and strength, increased bone density, growth and strength,
Virilizing: maturation of sex organs, formation of scrotum, deepening of voice, growth of beard and axillary hair. |
Estradiol | Sertoli cells | Prevent apoptosis of germ cells[6] |
Inhibin | Sertoli cells | Inhibit production of FSH |
Ovarian follicle and corpus luteum
Secreted hormone | From cells | Effect |
---|---|---|
Progesterone | Granulosa cells, theca cells | Support pregnancy:[7]
Other:
|
Androstenedione | Theca cells | Substrate for estrogen |
Estrogens (mainly estradiol) | Granulosa cells | Structural:
Protein synthesis:
Fluid balance:
Gastrointestinal tract:
Melanin:
Cancer:
Lung function: |
Inhibin | Granulosa cells | Inhibit production of FSH from anterior pituitary |
Placenta (when pregnant)
Secreted hormone | Abbreviation | From cells | Effect |
---|---|---|---|
Progesterone (Primarily) | Support pregnancy:[7]
Other effects on mother similar to ovarian follicle-progesterone | ||
Estrogens (mainly Estriol) (Also Primarily) | Effects on mother similar to ovarian follicle estrogen | ||
Human chorionic gonadotropin | HCG | Syncytiotrophoblast | Promote maintenance of corpus luteum during beginning of pregnancy
Inhibit immune response, towards the human embryo. |
Human placental lactogen | HPL | Syncytiotrophoblast | Increase production of insulin and IGF-1
Increase insulin resistance and carbohydrate intolerance |
Inhibin | Fetal Trophoblasts | Suppress FSH |
Uterus (when pregnant)
Secreted hormone | Abbreviation | From cells | Effect |
---|---|---|---|
Prolactin | PRL | Decidual cells | milk production in mammary glands |
Relaxin | Decidual cells | Unclear in humans and animals |
Calcium regulation
Parathyroid
Secreted hormone | Abbreviation | From cells | Effect |
---|---|---|---|
Parathyroid hormone | PTH | Parathyroid chief cell | Calcium:
|
Skin
Secreted hormone | From cells | Effect |
---|---|---|
Calcidiol (25-hydroxyvitamin D3) | Inactive form of vitamin D3 |
Targets
Heart
Secreted hormone | Abbreviation | From cells | Effect |
---|---|---|---|
Atrial-natriuretic peptide | ANP | Cardiac myocytes | Reduce blood pressure by:
reducing systemic vascular resistance, reducing blood water, sodium and fats |
Brain natriuretic peptide | BNP | Cardiac myocytes | (To a lesser degree than ANP) reduce blood pressure by:
reducing systemic vascular resistance, reducing blood water, sodium and fats |
Bone marrow
Secreted hormone | From cells | Effect |
---|---|---|
Thrombopoietin | liver and kidney cells | stimulates megakaryocytes to produce platelets[4] |
Skeletal muscle
In 1998, skeletal muscle was identified as an endocrine organ[12] due to its now well-established role in the secretion of myokines.[12][13] The use of the term myokine to describe cytokines and other peptides produced by muscle as signalling molecules was proposed in 2003.[14]
Adipose tissue
Signalling molecules released by adipose tissue are referred to as adipokines.
Secreted hormone | From cells | Effect |
---|---|---|
Leptin (Primarily) | Adipocytes | decrease of appetite and increase of metabolism. |
Estrogens[15] (mainly Estrone) | Adipocytes |
Major endocrine systems
The human endocrine system consists of several systems that operate via feedback loops. Several important feedback systems are mediated via the hypothalamus and pituitary.[16]
- TRH – TSH – T3/T4
- GnRH – LH/FSH – sex hormones
- CRH – ACTH – cortisol
- Renin – angiotensin – aldosterone
- leptin vs. insulin
Physiology
Interaction with immune system
Extensive bidirectional interactions exist between the endocrine system and the immune system.[17] Cortisol has major immunosuppressive effects,[18][19] and dopamine has immunomodulatory functions.[20] On the other hand, cytokines produced during inflammation activate the HPA axis at all three levels, sensible to negative feedback.[21] Moreover, cytokines stimulate hepcidin release from the liver, which is eventually responsible for the anemia of chronic disease.[22]
Other types of signalling
The typical mode of cell signaling in the endocrine system is endocrine signaling. 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
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
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 target other pancreatic cells.[1]
Juxtacrine
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.
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.
Unlike other types of cell signaling (such as paracrine and endocrine), juxtacrine signaling requires physical contact between the two cells involved.
Juxtacrine signaling has been observed for some growth factors, cytokine and chemokine cellular signals.
Diseases
Diseases of the endocrine system are common,[24] including conditions such as diabetes mellitus, thyroid disease, and obesity. Endocrine disease is characterized by irregulated hormone release (a productive pituitary adenoma), inappropriate response to signaling (hypothyroidism), lack of a gland (diabetes mellitus type 1, diminished erythropoiesis in chronic renal 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.
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.[25]
Other animals
A neuroendocrine system has been observed in all animals with a nervous system and all vertebrates have an hypothalamus-pituitary axis.[26] All vertebrates have a thyroid, which in amphibians is also crucial for transformation of larvae into adult form.[27][28] All vertebrates have adrenal gland tissue, with mammals unique in having it organized into layers.[29] All vertebrates have some form of renin-angiotensin axis, and all tetrapods have aldosterone as primary mineralocorticoid.[30][31]
Additional images
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Female endocrine system.
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Male endocrine system
See also
References
- 1 2 3 Marieb, Elaine (2014). Anatomy & physiology. Glenview, IL: Pearson Education, Inc. ISBN 978-0321861580.
- ↑ Colorado State University – Biomedical Hypertextbooks – Somatostatin
- ↑ Endo K, Matsumoto T, Kobayashi T, Kasuya Y, Kamata K (2005). "Diabetes-related changes in contractile responses of stomach fundus to endothelin-1 in streptozotocin-induced diabetic rats". J Smooth Muscle Res 41 (1): 35–47. doi:10.1540/jsmr.41.35. PMID 15855738.
- 1 2 3 Kaushansky K (May 2006). "Lineage-specific hematopoietic growth factors". N Engl J Med. 354 (19): 2034–45. doi:10.1056/NEJMra052706. PMID 16687716.
- 1 2 Physiology: 5/5ch4/s5ch4_17 - Essentials of Human Physiology
- ↑ Pentikäinen V, Erkkilä K, Suomalainen L, Parvinen M, Dunkel L (2000). "Estradiol acts as a germinal cell survival factor in the human testis in vitro". J Clin Endocrinol Metab. 85 (5): 2057–67. doi:10.1210/jcem.85.5.6600. PMID 10843196.
- 1 2 3 4 Bowen, R. (August 6, 2000) Placental Hormones. Colorado State University
- ↑ Physiology: 5/5ch9/s5ch9_13 - Essentials of Human Physiology
- ↑ Hould F, Fried G, Fazekas A, Tremblay S, Mersereau W (1988). "Progesterone receptors regulate gallbladder motility". J Surg Res 45 (6): 505–12. doi:10.1016/0022-4804(88)90137-0. PMID 3184927.
- ↑ Hormonal Therapy
- ↑ Massaro D, Massaro GD (2004). "Estrogen regulates pulmonary alveolar formation, loss, and regeneration in mice". American Journal of Physiology. Lung Cellular and Molecular Physiology 287 (6): L1154–9. doi:10.1152/ajplung.00228.2004. PMID 15298854.
- 1 2 Pedersen BK, Febbraio MA (October 2008). "Muscle as an endocrine organ: focus on muscle-derived interleukin-6". Physiological Reviews 88 (4): 1379–406. doi:10.1152/physrev.90100.2007. PMID 18923185.
- ↑ Ostrowski K, Hermann C, Bangash A, Schjerling P, Nielsen JN, Pedersen BK (December 1998). "A trauma-like elevation of plasma cytokines in humans in response to treadmill running". The Journal of Physiology 513 (3): 889–94. doi:10.1111/j.1469-7793.1998.889ba.x. PMC 2231318. PMID 9824725.
- ↑ Pedersen BK, Steensberg A, Fischer C; et al. (2003). "Searching for the exercise factor: is IL-6 a candidate?". Journal of Muscle Research and Cell Motility 24 (2-3): 113–9. doi:10.1023/A:1026070911202. PMID 14609022.
- ↑ Frühbeck G (July 2004). "The adipose tissue as a source of vasoactive factors". Curr Med Chem Cardiovasc Hematol Agents 2 (3): 197–208. doi:10.2174/1568016043356255. PMID 15320786.
- ↑ Sherwood, L. (1997). "Human Physiology: From Cells to Systems". Wadsworth Pub Co. ISBN 0495391840.
- ↑ Turnbull AV, Rivier CL (January 1999). "Regulation of the hypothalamic-pituitary-adrenal axis by cytokines: actions and mechanisms of action". Physiological Reviews 79 (1): 1–71. PMID 9922367.
- ↑ O'Connor TM, O'Halloran DJ, Shanahan F (June 2000). "The stress response and the hypothalamic-pituitary-adrenal axis: from molecule to melancholia". QJM 93 (6): 323–33. doi:10.1093/qjmed/93.6.323. PMID 10873181.
- ↑ Tsigos C, Chrousos GP (October 2002). "Hypothalamic-pituitary-adrenal axis, neuroendocrine factors and stress". Journal of Psychosomatic Research 53 (4): 865–71. doi:10.1016/S0022-3999(02)00429-4. PMID 12377295.
- ↑ Sarkar C, Basu B, Chakroborty D, Dasgupta PS, Basu S (May 2010). "The immunoregulatory role of dopamine: an update". Brain, Behavior, and Immunity 24 (4): 525–8. doi:10.1016/j.bbi.2009.10.015. PMC 2856781. PMID 19896530.
- ↑ Silverman MN, Pearce BD, Biron CA, Miller AH (2005). "Immune modulation of the hypothalamic-pituitary-adrenal (HPA) axis during viral infection". Viral Immunology 18 (1): 41–78. doi:10.1089/vim.2005.18.41. PMC 1224723. PMID 15802953.
- ↑ Andrews NC (May 2004). "Anemia of inflammation: the cytokine-hepcidin link". The Journal of Clinical Investigation 113 (9): 1251–3. doi:10.1172/JCI21441. PMC 398435. PMID 15124013.
- ↑ "Mortality and Burden of Disease Estimates for WHO Member States in 2002" (xls). World Health Organization. 2002.
- ↑ Kasper (2005). Harrison's Principles of Internal Medicine. McGraw Hill. p. 2074. ISBN 0-07-139140-1.
- ↑ Bhowmick NA, Chytil A, Plieth D, Gorska AE, Dumont N, Shappell S, Washington MK, Neilson EG, Moses HL (2004). "TGF-beta signaling in fibroblasts modulates the oncogenic potential of adjacent epithelia". Science 303 (5659): 848–51. doi:10.1126/science.1090922. PMID 14764882.
- ↑ 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, Walton W.; Darling, Douglas S. (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, Valerie Anne (1 January 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.
External links
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 |
Library resources about Endocrine system |
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