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蕈毒鹼型乙醯膽鹼受器

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蕈毒鹼型乙醯膽鹼受器是一大類固定在細胞膜上的乙醯膽鹼受器,其對蕈毒鹼比對菸鹼(尼古丁)更為敏感。反過來對菸鹼比較敏感的則稱為菸鹼型乙醯膽鹼受器。蕈毒鹼與菸鹼兩者皆為生物鹼(alkaloid)。許多藥品與其他類物質(例如pilocarpine與scopolamine)常以促進劑或拮抗劑的角色發生作用,並且其作用是僅單一針對蕈毒鹼受器或單一針對菸鹼受器,使得這樣的受器分類顯得有用。

目录

[编辑] 背景

Image:Toadyone.jpg
Amanita muscaria from which muscarine was isolated
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乙醯膽鹼受器中,蕈毒鹼受器是一種次分類,廣泛分布於中樞神經系統與自主神經系統。自主神經系統在解剖上與體神經系統相異。The autonomic nervous system controls various involuntary actions, such as heart rate, pupil dilation, sweating, salivation, urination and defecation, digestion, and so on. These actions are known as involuntary, that is to say that the conscious mind is unaware of these actions, or unable to influence them. It is the autonomic nervous system about which the most is known concerning muscarinic receptors.

The autonomic nervous system is divided into two parts, 交感副交感 nervous systems. The sympathetic nervous system is responsible for sweating, bronchodilation, increased heart-rate and blood pressure, decreased digestion, and so on, (often summarised as flight or fight), whereas the parasympathetic nervous system is responsible for salivation, decreased heart-rate, the accommodation of the eye for near-work, digestion, and so on (often summarised as rest and digest). The distribution of muscarinic receptors crucially differs between the sympathetic and the parasympathetic nervous system, a full discussion of which follows.

A further necessary distinction to make in a description of muscarinic receptors is that, in contrast to the voluntary nervous system -- which consists of a single nerve cell extending from the central nervous system to the synapse between that nerve and the innervated organ -- the autonomic nervous system consists of two nerve cells. The junction between these cells is a 神經節, usually located in or near the target organ. The nerve extending from the central nervous system to the ganglion is known as the 節前神經元. The nerve extending from the ganglion to the innervated tissue is known as the postganglionic neuron.

[编辑] 生理學

乙醯膽鹼(Acetylcholine, ACh)是一種神經傳導物質,在腦部與自主神經系統中廣泛存在。

ACh is always used as the transmitter within the autonomic ganglion. Nicotinic receptors on the postganglionic neuron are responsible for the initial fast depolarisation (Fast EPSP) of that neuron. As a consequence of this, nicotinic receptors are often cited as the receptor on the postganglionic neurons at the ganglion. However, the subsequent hyperpolarisation (IPSP) and slow depolarisation (Slow EPSP) which represent the recovery of the postganglionic neuron from stimulation are actually mediated by muscarinic receptors, types M2 and M1 respectively (discussed later).

Another role for these receptors is at the junction of the innervated tissue and the postganglionic neuron in the parasympathetic division of the autonomic nervous system. Here acetylcholine is again used as a neurotransmitter, and muscarinic receptors form the principal receptors on the innervated tissue. In addition, muscinaric acetylcholine receptors pre-synaptically on the post-ganglionic neuron bind to the released acetylcholine and regulate the response of the postganglionic neuron.

By contrast, this junction in the sympathetic division does not tend to use acetylcholine as a neurotransmitter (instead, noradrenaline is used), and therefore neither muscarinic nor nicotinic receptors are involved. A very few parts of the sympathetic system (sweating, for example), do use acetylcholine as a neurotransmitter at this position. In these cases, the receptors are of the muscarinic type. The sympathetic nervous system also has single nerves terminating at the chromaffin cells in the adrenal medulla, which secrete adrenaline and noradrenaline into the bloodstream. Acetylcholine is used as a neurotransmitter, and the receptor is of the nicotinic type. The somatic nervous system uses acetylcholine at the junction between its one peripheral nerve and the innervated tissue, also of the nicotinic type.

Muscarinic acetylcholine receptors are also present and distributed throughout the central nervous system, in post-synaptic and pre-synaptic positions. There is also some evidence for postsynaptic receptors on sympathetic neurons allowing the parasympathetic nervous system to inhibit sympathetic effects.

It's now known they also appear on the pre-synaptic membrane of somatic neurons in the neuro-muscular junction, where they are involved in the regulation of acetylcholine release.

In summary, then, muscarinic receptors can be found:

  • Between the postganglionic neurons and the innervated tissue throughout the parasympathetic nervous system.
  • Presynaptically within the postganglionic neurons to regulate acetylcholine release in the parasympathetic nervous system.
  • Between the postganglionic neurons and the innervated tissue in a very few parts of the sympathetic nervous system.
  • Within the ganglions of the whole autonomic nervous system (sympathetic and parasympathetic), acting as recovery receptors after the primary stimulation of the postganglionic neurons by action on nicotinic receptors by ACh from the preganglionic neuron.
  • In various parts of the higher central nervous system, which are currently poorly characterised, but have a role in cognition and memory, and degenerate in Alzheimer's disease.
  • On the presynaptic membrane of the neuromuscular junction where they are part of a feedback loop that helps regulate ACh release.

[编辑] 蕈毒鹼型受器的型態

Muscarinic acetylcholine receptors belong to a class of metabotropic receptors which use G 蛋白 as their signalling mechanism. There are known to be a large number of these G-protein-coupled receptors for 神經受體, 荷爾蒙, and other substances. G proteins are also present in taste, and odour detecting cells, in the retina, and in many other systems.

In such receptors, the signalling molecule (the ligand) binds to a receptor which has seven transmembrane regions, in our case the ligand is ACh. This receptor is bound to intracellular proteins, known as G proteins, which begin the information cascade within the cell.

By contrast nicotinic receptors use an ion-gated mechanism for signalling. Sufficient ligands cause an ion channel to open, filling (or evacuating) a cell of a particular ion.

[编辑] 受器形式的多樣性

Template:Protein Template:Protein Template:Protein Template:Protein Template:Protein By the use of selective radioactively-labelled agonist and antagonist substances, four subtypes of muscarinic receptors have been determined, named M1-M4 (using an upper case M). For example, the drug pirenzepine is a muscarinic antagonist (decreases the effect of ACh) which is much more potent at M1 receptors than it is at other subtypes. The acceptance of the various subtypes has proceeded in numerical order: therefore, sources exist which only recognise the M1/M2 distinction, more recent studies tend to recognise M3, and the most recent M4.

Meanwhile, geneticists and molecular biologists have characterised five genes which appear to encode muscarinic receptors, named m1-m5 (lower case m). The first four code for pharmacologic types M1-M4. The fifth, m5, corresponds to a subtype of receptor which has not been detected pharmacologically. m1 and m2 were determined based upon partial sequencing of M1 and M2 receptor proteins, the others were found by searching for homology, using bioinformatic techniques.

G proteins contain an alpha-subunit which is critical to the functioning of receptors. These subunits can take a number of forms. There are four broad classes of form of G-protein, G_s, G_i, Gq and G12.[1] Muscarinic receptors vary in the G protein to which they are bound, with some correlation according to receptor type. G proteins are also classified according to their susceptibility to cholera toxin (CTX) and pertussis toxin (PTX, whooping cough). Gs and some subtypes of Gi (Gαt and Gαg) are succeptible to CTX. Only G_i is succeptible to PTX, with the exception of one subtype of Gi (Gαz) which is immune. Also, only when bound with an agonist, those G proteins normally sensitive to PTX also become susceptible to CTX.[2]

The various G-protein subunits act differently upon secondary messengers, upregulating Phospholipases, downregulating cAMP, and so on.

Because of the strong correlations to muscarinic receptor type, CTX and PTX are useful experimental tools in investigating these receptors.

[编辑] 受器亞型m1

This receptor is found mediating slow EPSP at the ganglion in the postganglionic nerve,[3] is common in secretory glands (exocrine glands),[4],[5] and in the CNS.[6],[7] It is predominantly found bound to G proteins of class Gq[8] which use upregulation of phospholipase C and therefore inositol triphosphate and intracellular calcium as a signalling pathway. A receptor so bound would not be susceptible to CTX or PTX. However, Gi[9] (causing a downstream decrease in cAMP) and Gs[10] (causing an increase in cAMP) have also been shown to be involved in interactions in certain tissues, and so would be susceptible to PTX and CTX respectively.

[编辑] 受器亞型m2

M2: These receptors are found in cardiac tissue and cause a slowing of sinoatrial depolarization and a decrease in conduction velocity.

The M2 muscarinic receptors are located in the heart, they act to bring the heart back to normal after the actions of the sympathetic nervous system. They slow down the heart rate, reduce contractile forces of the atrial cardiac muscle, and reduce conduction velocity of the atrioventricular node (AV node). Note, they have no effect on the contractile forces of the ventricular muscle.

M2 muscarinic receptors act via a Gi type receptor, which causes a decrease in cAMP in the cell, generally leading to inhibitory-type effects.[11]

[编辑] 受器亞型m3

M3: These receptors are found on smooth muscles and in glands. M3 receptors generally cause smooth muscle contraction and increased glandular secretions.

The M3 muscarinic receptors are located at many places in the body. They are located in the smooth muscles of the blood vessels, as well as in the lungs. This means they cause vasodilation and bronchoconstriction. They are also in the smooth muscles of the gastrointestinal tract (GIT), which help in increasing intestinal motility and dilating sphincters. The M3 receptors are also located in many glands which help to stimulate secretion in salivary glands and other glands of the body.

Like the M1 muscarinic receptor, M3 receptors are G proteins of class Gq which upregulate phospholipase C and therefore inositol triphosphate and intracellular calcium as a signalling pathway.[12]

[编辑] 受器亞型m4

M4: Receptors work via Gi receptors to decrease cAMP in the cell and thus produce generally inhibitory effects. Location of M4 receptors are not well known. Although, all five Muscarinic receptors are found in the CNS.

[编辑] 受器亞型m5

M5:Like the M1 and M3 muscarinic receptor, M5 receptors are G proteins of class Gq which upregulate phospholipase C and therefore inositol triphosphate and intracellular calcium as a signalling pathway. Location of M5 receptors are not well known. Although, all five Muscarinic receptors are found in the CNS.

[编辑] 相關條目

蕈毒鹼受器促進劑

[编辑] 文獻

  1. ^  Simon MI, Strathmann M, Gautam N (1991). "Diversity of G proteins in signal transduction". Science 252 (5007): 802-8. PMID 1902986.
Fulltext (PDF, subscription required)
  1. ^ Mark L Dell'Acqua, Reed C Carrol, Ernest G Peralta (1993). "Transfected m2 muscarinic acetylcholine receptors couple to G alpha i2 and G alpha i3 in Chinese hamster ovary cells. Activation and desensitization of the phospholipase C signaling pathway". Journal of Biomedical Chemistry 268 (8): 5676-85. PMID 8449930.
Free Fulltext (PDF)
  1. ^ Messer, Jr, William S. Acetylcholine. 20 Jan 2000. University of Toledo. Accessed 11 September 2005.
  2. ^ Johnson, Gordon E. PDQ Pharmacology. 2nd edition. BC Decker. 2002. ISBN 1550091093
  3. ^ Richelson, Elliot. Cholinergic Transduction. The Fourth Generation of Progress. The American College of Neuropsychopharmacology. 2000.
  4. ^ see Johnson, 2002.
  5. ^ see Richelson, 2000.
  6. ^ G protein diversity and complexity in G-protein Signaling. RA Fisher. University of Iowa, Lecture Notes, 2004.
  7. ^ see Richelson, 2000.
  8. ^ Burford NT, Nahorski SR (1996). "Muscarinic m1 receptor-stimulated adenylate cyclase activity in Chinese hamster ovary cells is mediated by Gs alpha and is not a consequence of phosphoinositidase C activation". Biochemistry Journal 315 (Pt 3): 883-8. PMID 8645172.
Fulltext (subscription required)
  1. ^ University of Sydney lecture notes on the M2 receptors, 2005.
  2. ^ University of Sydney lecture notes on the M3 receptors, 2005.
  3. Dittman AH, Weber JP, Hinds TR, Choi EJ, Migeon JC, Nathanson NM, Storm DR (1994). "A novel mechanism for coupling of m4 muscarinic acetylcholine receptors to calmodulin-sensitive adenylyl cyclases: crossover from G protein-coupled inhibition to stimulation". Biochemistry 33 (4): 943-51. PMID 8305442.
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