Autonomic nervous system
| Autonomic nervous system | |
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| The autonomic nervous system Blue = parasympathetic Red = sympathetic |
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| Latin | divisio autonomica systematis nervosi peripherici |
The autonomic nervous system (ANS or visceral nervous system) is the part of the peripheral nervous system that acts as a control system functioning largely below the level of consciousness, and controls visceral functions.[1] The ANS affects heart rate, digestion, respiration rate, salivation, perspiration, diameter of the pupils, micturition (urination), and sexual arousal. Whereas most of its actions are involuntary, some, such as breathing, work in tandem with the conscious mind.
It is classically divided into two subsystems: the parasympathetic nervous system and sympathetic nervous system.[1][2] Relatively recently, a third subsystem of neurons that have been named 'non-adrenergic and non-cholinergic' neurons (because they use nitric oxide as a neurotransmitter) have been described and found to be integral in autonomic function, particularly in the gut and the lungs.
With regard to function, the ANS is usually divided into sensory (afferent) and motor (efferent) subsystems. Within these systems, however, there are inhibitory and excitatory synapses between neurones.
The enteric nervous system is sometimes considered part of the autonomic nervous system, and sometimes considered an independent system.
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Anatomy
The sympathetic nervous trunk consists of sympathetic ganglia running directly adjacent to the spinal column. The adrenal medulla can be considered a sympathetic ganglion; although separate from the main trunk, the sympathetic fibers run through the sympathetic trunk before synapsing in the adrenal medulla. The parasympathetic division consists of a sacral and cranial part. In the cranium the PSN originate from cranial nerves CN III (oculomotor nerve), CN VII (facial nerve), CN IX (glossopharyngeal nerve) and CN X (vagus nerve). In the sacral region of the body the PSN is derived from spinal nerves S2, S3 and S4, commonly referred to as the pelvic splanchnics. The reflex arcs of the ANS comprise a sensory (afferent) arm, and a motor (efferent or effector) arm. Only the latter is shown in the illustration.
Sensory neurons
The sensory arm is made of “primary visceral sensory neurons” found in the peripheral nervous system (PNS), in “cranial sensory ganglia”: the geniculate, petrosal and nodose ganglia, appended respectively to cranial nerves VII, IX and X. These sensory neurons monitor the levels of carbon dioxide, oxygen and sugar in the blood, arterial pressure and the chemical composition of the stomach and gut content. (They also convey the sense of taste, a conscious perception). Blood oxygen and carbon dioxide are in fact directly sensed by the carotid body, a small collection of chemosensors at the bifurcation of the carotid artery, innervated by the petrosal (IXth) ganglion. Primary sensory neurons project (synapse) onto “second order” or relay visceral sensory neurons located in the medulla oblongata, forming the nucleus of the solitary tract (nTS), that integrates all visceral information. The nTS also receives input from a nearby chemosensory center, the area postrema, that detects toxins in the blood and the cerebrospinal fluid and is essential for chemically induced vomiting or conditional taste aversion (the memory that ensures that an animal which has been poisoned by a food never touches it again). All these visceral sensory informations constantly and unconsciously modulate the activity of the motor neurons of the ANS
Motor neurons
Motor neurons of the ANS are also located in ganglia of the PNS, called “autonomic ganglia”. They belong to three categories with different effects on their target organs (see below “Function”): sympathetic, parasympathetic and enteric.
Sympathetic ganglia are located in two sympathetic chains close to the spinal cord: the prevertebral and pre-aortic chains. Parasympathetic ganglia, in contrast, are located in close proximity to the target organ: the submandibular ganglion close to salivary glands, paracardiac ganglia close to the heart etc... Enteric ganglia, which as their name implies innervate the digestive tube, are located inside its walls and collectively contain as many neurons as the entire spinal cord, including local sensory neurons, motor neurons and interneurons. It is the only truly autonomous part of the ANS and the digestive tube can function surprisingly well even in isolation. For that reason the enteric nervous system has been called “the second brain”.
The activity of autonomic ganglionic neurons is modulated by “preganglionic neurons” (also called improperly but classically "visceral motoneurons") located in the central nervous system. Preganglionic sympathetic neurons are in the spinal cord, at thoraco-lumbar levels. Preganglionic parasympathetic neurons are in the medulla oblongata (forming visceral motor nuclei: the dorsal motor nucleus of the vagus nerve (dmnX), the nucleus ambiguus, and salivatory nuclei) and in the sacral spinal cord. Enteric neurons are also modulated by input from the CNS, from preganglionic neurons located, like parasympathetic ones, in the medulla oblongata (in the dmnX).
The feedback from the sensory to the motor arm of visceral reflex pathways is provided by direct or indirect connections between the nucleus of the solitary tract and visceral motoneurons.
Function
Sympathetic and parasympathetic divisions typically function in opposition to each other. But this opposition is better termed complementary in nature rather than antagonistic. For an analogy, one may think of the sympathetic division as the accelerator and the parasympathetic division as the brake. The sympathetic division typically functions in actions requiring quick responses. The parasympathetic division functions with actions that do not require immediate reaction. Consider sympathetic as "fight or flight" and parasympathetic as "rest and digest".
However, many instances of sympathetic and parasympathetic activity cannot be ascribed to "fight" or "rest" situations. For example, standing up from a reclining or sitting position would entail an unsustainable drop in blood pressure if not for a compensatory increase in the arterial sympathetic tonus. Another example is the constant, second to second modulation of heart rate by sympathetic and parasympathetic influences, as a function of the respiratory cycles. More generally, these two systems should be seen as permanently modulating vital functions, in usually antagonistic fashion, to achieve homeostasis. Some typical actions of the sympathetic and parasympathetic systems are listed below.
Sympathetic nervous system
Promotes a "fight or flight" response, corresponds with arousal and energy generation, and inhibits digestion.
- Diverts blood flow away from the gastro-intestinal (GI) tract and skin via vasoconstriction.
- Blood flow to skeletal muscles and the lungs is not only maintained, but enhanced (by as much as 1200% in the case of skeletal muscles).
- Dilates bronchioles of the lung, which allows for greater alveolar oxygen exchange.
- Increases heart rate and the contractility of cardiac cells (myocytes), thereby providing a mechanism for the enhanced blood flow to skeletal muscles.
- Dilates pupils and relaxes the ciliary muscle to the lens, allowing more light to enter the eye and far vision.
- Provides vasodilation for the coronary vessels of the heart.
- Constricts all the intestinal sphincters and the urinary sphincter.
- Inhibits peristalsis.
- Stimulates orgasm.
Parasympathetic nervous system
Promotes a "rest and digest" response, promotes calming of the nerves return to regular function, and enhances digestion.
- Dilates blood vessels leading to the GI tract, increasing blood flow. This is important following the consumption of food, due to the greater metabolic demands placed on the body by the gut.
- The parasympathetic nervous system can also constrict the bronchiolar diameter when the need for oxygen has diminished.
- Dedicated cardiac branches of the Vagus and thoracic Spinal Accessory nerves impart Parasympathetic control of the Heart or Myocardium.
- During accommodation, the parasympathetic nervous system causes constriction of the pupil and contraction of the ciliary muscle to the lens, allowing for closer vision.
- The parasympathetic nervous system stimulates salivary gland secretion, and accelerates peristalsis, so, in keeping with the rest and digest functions, appropriate PNS activity mediates digestion of food and indirectly, the absorption of nutrients.
- Is also involved in erection of genitals, via the pelvic splanchnic nerves 2–4.
- Stimulates sexual arousal.
Neurotransmitters and pharmacology
At the effector organs, sympathetic ganglionic neurons release noradrenaline (norepinephrine), along with other cotransmitters such as ATP, to act on adrenergic receptors, with the exception of the sweat glands and the adrenal medulla:
- Acetylcholine is the preganglionic neurotransmitter for both divisions of the ANS, as well as the postganglionic neurotransmitter of parasympathetic neurons. Nerves that release acetylcholine are said to be cholinergic. In the parasympathetic system, ganglionic neurons use acetylcholine as a neurotransmitter, to stimulate muscarinic receptors.
- At the adrenal cortex, there is no postsynaptic neuron. Instead the presynaptic neuron releases acetylcholine to act on nicotinic receptors.
- Stimulation of the adrenal medulla releases adrenaline (epinephrine) into the bloodstream which will act on adrenoceptors, producing a widespread increase in sympathetic activity.
The following table reviews the actions of these neurotransmitters as a function of their receptors.
Circulatory system
Heart
| Target | Sympathetic (adrenergic) | Parasympathetic (muscarinic) |
| cardiac output | β1, (β2): increases | M2: decreases |
| SA node: heart rate (chronotropic) | β1, (β2) [3]: increases | M2: decreases |
| Atrial cardiac muscle: contractility (inotropic) | β1, (β2)[3]: increases | M2: decreases |
| Ventricular cardiac muscle | β1, (β2): increases contractility (inotropic) increases cardiac muscle automaticity [3] |
--- |
| at AV node | β1: increases conduction increases cardiac muscle automaticity [3] |
M2: decreases conduction Atrioventricular block [3] |
Blood vessels
| Target | Sympathetic (adrenergic) | Parasympathetic (muscarinic) |
| vascular smooth muscle | α1: contracts; β2: relaxes | M3: relaxes [3] |
| renal artery | α1[4]: constricts | --- |
| larger coronary arteries | α1 and α2[5]: constricts [3] | --- |
| smaller coronary arteries | β2:dilates [6] | --- |
| arteries to viscera | α: constricts | --- |
| arteries to skin | α: constricts | --- |
| arteries to brain | α1[7]: constricts [3] | --- |
| arteries to erectile tissue | α1[8]: constricts | M3: dilates |
| arteries to salivary glands | α: constricts | M3: dilates |
| hepatic artery | β2: dilates | --- |
| arteries to skeletal muscle | β2: dilates | --- |
| Veins | α1 and α2 [9] : constricts β2: dilates |
--- |
Other
| Target | Sympathetic (adrenergic) | Parasympathetic (muscarinic) |
| platelets | α2: aggregates | --- |
| mast cells - histamine | β2: inhibits | --- |
Respiratory system
| Target | Sympathetic (adrenergic) | Parasympathetic (muscarinic) |
| smooth muscles of bronchioles | β2: relaxes (major contribution) α1: contracts (minor contribution) |
M3: contracts |
The bronchioles have no sympathetic innervation, but are instead affected by circulating adrenaline [3]
Nervous system
| Target | Sympathetic (adrenergic) | Parasympathetic (muscarinic) |
| Pupil dilator muscle | α1: contracts (causes mydriasis) |
M3: relaxes (causes miosis) |
| Ciliary muscle | β2: relaxes (causes long-range focus) |
M3: contracts (causes short-range focus) |
Digestive system
| Target | Sympathetic (adrenergic) | Parasympathetic (muscarinic) |
| salivary glands: secretions | β: stimulates viscous, amylase secretions α1: stimulates potassium cation |
M3: stimulates watery secretions |
| lacrimal glands (tears) | β: stimulates protein secretion [10] | --- |
| kidney (renin) | β1:[11] secretes | --- |
| parietal cells | --- | M1: Gastric acid secretion |
| liver | α1, β2: glycogenolysis, gluconeogenesis | --- |
| adipose cells | β1[11], β3: stimulates lipolysis | --- |
| GI tract (smooth muscle) motility | α1, α2[12], β2: decreases | M3, (M1) [3]: increases |
| sphincters of GI tract | α1 [11], α2 [3], β2: contracts | M3: relaxes |
| glands of GI tract | no effect [3] | M3: secretes |
Endocrine system
| Target | Sympathetic (adrenergic) | Parasympathetic (muscarinic) |
| pancreas (islets) | α2: decreases secretion from beta cells, increases secretion from alpha cells | M3[13] increases stimulation from alpha cells and beta cells |
| adrenal medulla | N (nicotinic ACh receptor): secretes epinephrine and norepinephrine | --- |
Urinary system
| Target | Sympathetic (adrenergic) | Parasympathetic (muscarinic) |
| Detrusor urinae muscle of bladder wall | β2: relaxes | M3:[11] contracts |
| urethral sphincter (internal) | α1: contracts | relaxes |
| sphincter | α1: contracts; β2 relaxes | M3:[11] relaxes |
Reproductive system
| Target | Sympathetic (adrenergic) | Parasympathetic (muscarinic) |
| uterus | α1: contracts (pregnant[3]) β2: relaxes (non-pregnant[3]) |
--- |
| genitalia | α1: contracts (ejaculation) | M3: erection |
Integumentary system
| Target | Sympathetic (muscarinic and adrenergic) | Parasympathetic (muscarinic) |
| sweat gland secretions | M: stimulates (major contribution); α1: stimulates (minor contribution) | --- |
| arrector pili | α1: stimulates | --- |
References
- ↑ 1.0 1.1 autonomic nervous system at Dorland's Medical Dictionary
- ↑ "eMedicine/Stedman Medical Dictionary Lookup!". http://www.emedicine.com/asp/dictionary.asp?keyword=autonomic+division+of+nervous+system. Retrieved 2008-11-30.
- ↑ 3.00 3.01 3.02 3.03 3.04 3.05 3.06 3.07 3.08 3.09 3.10 3.11 3.12 3.13 Rang, Dale, Ritter & Moore (2003). Pharmacology 5th ed.. Churchill Livingstone. p. 127. ISBN 0443071454.
- ↑ Renal alpha-1 and alpha-2 adrenergic receptors: biochemical and pharmacological correlations JM Schmitz, RM Graham, A Sagalowsky and WA Pettinger
- ↑ Coronary vasoconstriction mediated by alpha 1- and alpha 2-adrenoceptors in conscious dogs O. L. Woodman and S. F. Vatner
- ↑ Rang, H. P. (2003). Pharmacology. Edinburgh: Churchill Livingstone. ISBN 0-443-07145-4. Page 270
- ↑ Circulation & Lung Physiology I M.A.S.T.E.R. Learning Program, UC Davis School of Medicine
- ↑ 1A-Adrenoceptors mediate contractions to phenylephrine in rabbit penile arteries J S Morton1, C J Daly1, V M Jackson2 and J C McGrath1: "1A-ARs could be utilized to aid the erectile response in male erectile dysfunction sufferers by reducing vasoconstriction of the penile arteries"
- ↑ Elliott, J (1997). "Alpha-adrenoceptors in equine digital veins: Evidence for the presence of both alpha1 and alpha2-receptors mediating vasoconstriction". Journal of Veterinary Pharmacology & Therapeutics (Blackwell Publishings) 20 (4): 308–317. http://www.ingentaconnect.com/content/bsc/jvpt/1997/00000020/00000004/art00009;jsessionid=8lm5thggpj1x.alice?format=print.
- ↑ Protein secretion induced by isoproterenol or pentoxifylline in lacrimal gland P. Mauduit, G. Herman and B. Rossignol
- ↑ 11.0 11.1 11.2 11.3 11.4 Costanzo, Linda S. (2007). Physiology. Hagerstwon, MD: Lippincott Williams & Wilkins. ISBN 0-7817-7311-3.
- ↑ Sagrada, A; Fargeas, MJ; Bueno, L., A; Fargeas, MJ; Bueno, L (1987). "Involvement of alpha-1 and alpha-2 adrenoceptors in the postlaparotomy intestinal motor disturbances in the rat". Gutthen you cut in your @$$ 28 (8): 955–959. PMID 2889649. PMC 1433140. http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=1433140. PMID 1433140
- ↑ Verspohl EJ, Tacke R, Mutschler E, Lambrecht G (1990). "Muscarinic receptor subtypes in rat pancreatic islets: binding and functional studies". Eur. J. Pharmacol. 178 (3): 303–11. doi:10.1016/0014-2999(90)90109-J. PMID 2187704.
External links
- Receptors of the heart: Mnemonic
- Overview at arizona.edu
- ANS Medical Notes on rahulgladwin.com
- Explanations on the ANS by Dyansys, Inc.
- New technology for testing the wellness of the ANS
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