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A prostaglandin is any member of a group of lipid molecules that are derived from fatty acids and have important functions in the animal body. Every prostaglandin contains 20 carbon atoms, including a 5 carbon ring. They are mediators and have a variety of strong physiological effects; although they are technically hormones they are rarely classified as such.
The prostaglandins together with the thromboxanes from the prostanoid class of fatty acid derivatives; the prostanoid class is a subclass of eicosanoids.
The name prostaglandin comes from the prostate gland. When prostaglandin was first isolated from seminal fluid in 1936, it was believed to have been added from the prostate. In 1971, it was determined that aspirin-like drugs could inhibit the synthesis of prostaglandins. The biochemists Sune K. Bergström, Bengt I. Samuelsson and John R. Vane jointly received the 1982 Nobel Prize in Physiology or Medicine for their research on prostaglandins.
Prostaglandins are found in vitually all tissues and organs. They are autocrine and paracrine lipid mediators which act upon platelet, endothelium, uterine and mast cells among others. They are synthesized in the cell from arachidonate acid created by phospholipase A2. The intermediate is then passed into one of either the cyclooxygenase or lipoxygenase pathways to form either prostaglandin and thromboxane or leukotriene. The cyclooxygenase pathway produces thromboxane, prostacyclin and prostaglandin D, E and F. The lipoxygenase pathway is active in leukocytes and in macrophages and synthesises leukotrines. Prostagladins are released through the prostaglandin transporter on the cell's plasma membrane.
Prostaglandins are produced from arachidonic acid by cycloxygenases (COX-1 and COX-2). COX-1 is responsible for the baseline levels of prostaglandins while COX-2 produces prostaglandins through stimulation. While COX-1 is located in the blood vessels, stomach and the kidneys, prostaglandin level are induced by COX-2 in scenarios of inflammation. The recent development of COX-2 inhibitors, known as coxibs, allow the circumvention of the negative gastrointestinal effects while effectively reducing inflammation.
There are currently nine known receptors of prostaglandins on various cell types. Prostaglandins thus act on a variety of cells such as vascular smooth muscle cells causing constriction or dilation, on platelets causing aggregation or disaggregation and on spinal neurons causing pain. Prostagladins act principally on subfamily of G protein coupled receptors. Most of these GPCRs are located at the periphery of target cells at the plasma membrane, however, a few exist within the cell at the nuclear envelope. They may also act upon peroxisome proliferator-activated receptors. Prostaglandins have a wide variety of actions but most cause muscular constriction and mediate inflammation. Other effects can be calcium movement, hormone regulation and cell growth control. Thromboxane is created in platelets and causes vascular constriction and platelet aggregation. Prostacyclin comes from cells in the blood vessel walls and is antagonistic to thromboxane.
Prostaglandins are potent but have a short half-life before being inactivated and excreted.
15-deoxy-Δ12,14-PGJ2 (15d-PGJ2) is a PGD2 derivative that acts on PPAR intracellular receptors.
NSAIDs inhibit cyclooxygenase and reduce prostaglandin sysnthesis. Corticosteroids inhibit phospholipase A2 production by boosting production of lipocortin, an inhibitor protein. Relatively new drugs, known as childbirth (PGE2 or PGF2, with mifepristone);
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