Information about Neuropathy

Neuropathy
Classification & external resources
ICD-10G56. - G63.,
G90.0, G99.0
ICD-9337.0-337.1,
356-357, 377
eMedicinetopic list
Neuropathy is usually short for peripheral neuropathy, meaning a disease of the peripheral nerve or nerves.

Types

The four major forms of nerve damage are polyneuropathy, autonomic neuropathy, mononeuropathy, and mononeuritis multiplex. The most common form is peripheral polyneuropathy, which mainly affects the feet and legs.

Often the form of neuropathy is further broken down as to cause (see below), or other type, such as small fiber peripheral neuropathy, which is idiopathic.

There are other less common forms of neuropathy, for example Enteric Neuropathy

Peripheral neuropathy is not a disease in itself, but a symptom or a complication of other underlying conditions. Peripheral nerves, either singly or in groups, are damaged through lack of circulation, chemical imbalance, trauma, or other factors.

- Ruth Werner, LMP, NCTMB A Massage Therapist's Guide to Pathology; Third Edition Copyright 2005

Causes

Aside from diabetes (see Diabetic neuropathy), the common causes of neuropathy are herpes zoster infection, HIV-AIDS, toxins, alcoholism, chronic trauma (such as repetitive motion disorders) or acute trauma (including surgery), various neurotoxins and autoimmune conditions such as celiac disease, which can account for approximately 16% of small fiber neuropathy cases.[1] Neuropathic pain is common in cancer as a direct result of the cancer on peripheral nerves (e.g., compression by a tumor), as a side effect of many chemotherapy drugs, and as a result of electrical injury. In many cases the neuropathy is "idiopathic," meaning no cause is found. A form of spinal nerve entrapment called Posterior Rami Syndrome can lead to neuropathic pain.

Symptoms

Neuropathy often results in numbness, abnormal sensations called dysesthesias and allodynias that occur either spontaneously or in reaction to external stimuli, and a characteristic form of pain, called neuropathic pain or neuralgia, that is qualitatively different from the ordinary nociceptive pain one might experience from stubbing a toe or hitting a finger with a hammer.

Neuropathic pain is usually perceived as a steady burning and/or "pins and needles" and/or "electric shock" sensations and/or tickling. The difference is due to the fact that "ordinary" pain stimulates only pain nerves, while a neuropathy often results in the firing of both pain and non-pain (touch, warm, cool) sensory nerves in the same area, producing signals that the spinal cord and brain do not normally expect to receive.

Treatment of neuropathic pain

Neuropathic pain can be very difficult to treat. Sometimes strong opioid analgesics may provide only partial relief. Opioid analgesics are to be considered only as a tertiary treatment.

A systematic review of randomized controlled trials found that the best treatments are tricyclic antidepressants, older anticonvulsants, and capsaicin.[2] Tricyclic antidepressants include amitriptyline (Elavil®). Older anticonvulsants, valproate or carbamazepine (Tegretol®), were more effective than the newer anticonvulsants pregabalin (Lyrica®) and gabapentin (Neurontin®). In general, the antidepressants seem to be most effective on continuous burning pain, while the anticonvulsants seem to work best on sudden, lancinating, "shock-like" pains that appear to involve large numbers of peripheral nerves improperly firing together.

In animal models of neuropathic pain it has been found that compounds which only block serotonin reuptake do not improve neuropathic pain.[3][4][5][6][7][8][9][10] Similarly, compounds that only block norepinephrine reuptake also do not improve neuropathic pain. Compounds such as duloxetine, venlafaxine, and milnacipran that block both serotonin reuptake and norepinephrine reuptake do improve neuropathic pain.

Many of the pharmacologic treatments for chronic neuropathic pain decrease the sensitivity of nociceptive receptors, or desensitize C fibers such that they transmit fewer signals. The newer anticonvulsants gabapentin and pregabalin appear to work by blocking calcium channels in damaged peripheral neurons. Tricyclic antidepressants may also work on sodium channels in peripheral nerves. The anticonvulsants carbamazepine (Tegretol®) and oxcarbazepine (Trileptal®), especially effective on trigeminal neuralgia, are thought to work principally on sodium channels.

Topical agents

In some forms of neuropathy, especially post-herpes neuralgia, the topical application of local anesthetics such as lidocaine can provide relief. A transdermal patch containing 5% lidocaine is available. Ketamine in a transdermal gel is also frequently effective when the neuropathy is localized. Neurontin 100mg/g PLO gel is also effective for treating peripheral neuropathy, including Carpal Tunnel Syndrome. Capsaicin cream can be beneficial in several neurogenic pain disorders, which causes release of the pain neurotransmitter Substance P, and eventually reduces the availability of Substance P.

Antidepressants

Main article: antidepressants
Antidepressants usually reduce neuropathic pain more quickly and with smaller doses than they relieve depression. Antidepressants therefore seem to work differently on neuropathic pain than on depression, perhaps by activating descending norepinephrinergic and serotonergic pathways in the spinal cord that block pain signals from ascending to the brain.

Anticonvulsants

Main article: anticonvulsants

Reducing the sympathetic nerve activity

In some neuropathic pain syndromes, "crosstalk" occurs between descending sympathetic nerves and ascending sensory nerves. Increases in sympathetic nervous system activity result in an increase of pain; this is known as sympathetically-mediated pain. Reducing the sympathetic nerve activity in the painful region with local nerve blocks or systemic medications such as the alpha-blocker clonidine may provide relief. Other drugs, known for their ability to desensitize cardiac tissue, include beta-blockers such as propanolol and calcium channel blockers such as verapamil.

NMDA antagonism

The N-methyl-D-aspartate receptor (NMDA) seems to play a major role in neuropathic pain and in the development of opioid tolerance.

Several opioids, particularly methadone and dextromethorphan, have NMDA antagonist activity in addition to their μ-opioid agonist properties that seems to make them effective against neuropathic pain, although this is still the subject of intensive research and clinical study. Methadone has this property because it is a racemic mixture; one stereo-isomer is a μ-opioid agonist; the other is a NMDA antagonist.

Experiments in both animals and humans have established that NMDA antagonists such as ketamine and dextromethorphan[11] can alleviate neuropathic pain and reverse opioid tolerance. Unfortunately, only a few NMDA antagonists are clinically available and their use is usually associated with unacceptable side effects.

Transcutaneous electrical nerve stimulation

Transcutaneous electrical nerve stimulation (TENS) is worth a trial in chronic neurogenic pain. Some pain management specialists will try acupuncture, with variable results. TENS, with certain electrical waveforms, appears to have an acupuncture-like function.

Marijuana

A recent study showed smoking marijuana is beneficial in treating HIV-associated peripheral neuropathy.[12]

Photo therapy

In more recent years, infrared photo therapy has been used to treat neuropathic symptoms. Photo therapy devices emit near infrared light typically at a wavelength of 890nm. This wavelength is believed to stimulate the release of nitric oxide, an endothelium-derived relaxing factor into the bloodstream, thus vasodilating the capilaries and venuoles in the microcirculatory system. This increase in circulation has been shown effective in various clinical studies, to decrease pain and improve sensation in diabetic and non-diabetic patients. Note that the U.S. FDA has not approved any infrared photo therapy devices to treat neuropathy.[13]

Other modalities

In addition to pharmacological treatment there are several other modalities that help some cases. While lacking double blind trials, these have shown to reduce pain and improve patient quality of life particularly for chronic neuropathic pain: Interferential Stimulation; Acupuncture; Meditation; Cognitive Therapy; and prescribed exercise.

Alternative medicine treatments

There are 2 dietary supplements that have clinical evidence showing them to be effective treatments of diabetic neuropathy; alpha lipoic acid and benfotiamine. In several studies using a variety of dosages and routes of administration, alpha lipoic acid was found to reduce the various symptoms of peripheral diabetic neuropathy. A recent review of the published data determined “ALA should be considered as a treatment option for patients with peripheral diabetic neuropathy.” Also a recent study using orally administered alpha lipoic acid found that 600 mg once a day caused a marked reduction in the symptoms of diabetic neuropathy including stabbing pain, burning pain, paresthesia, and asleep numbness of the feet. Benfotiamine is a lipid soluble form of thiamine that has several placebo controlled double blind trials proving efficacy in treating neuropathy and various other diabetic comorbidities. 400 mg a day was the most commonly studied dose.

See also

Footnotes

1. ^ Up to 16% of Patients with Small Fiber Neuropathy May Have Celiac Disease. Celiac.com. Retrieved on 2007-26-06.
2. ^ Wong MC, Chung JW, Wong TK (2007). "Effects of treatments for symptoms of painful diabetic neuropathy: systematic review". BMJ 335 (7610): 87. DOI:10.1136/bmj.39213.565972.AE. PMID 17562735. 
3. ^ Bennett G, Xie Y (1988). "A peripheral mononeuropathy in rat that produces disorders of pain sensation like those seen in man". Pain 33 (1): 87-107. PMID 2837713. 
4. ^ Seltzer Z, Dubner R, Shir Y (1990). "A novel behavioral model of neuropathic pain disorders produced in rats by partial sciatic nerve injury". Pain 43 (2): 205-18. PMID 1982347. 
5. ^ Kim S, Chung J (1992). "An experimental model for peripheral neuropathy produced by segmental spinal nerve ligation in the rat". Pain 50 (3): 355-63. PMID 1333581. 
6. ^ Malmberg A, Basbaum A (1998). "Partial sciatic nerve injury in the mouse as a model of neuropathic pain: behavioral and neuroanatomical correlates". Pain 76 (1-2): 215-22. PMID 9696476. 
7. ^ Sung B, Na H, Kim Y, Yoon Y, Han H, Nahm S, Hong S (1998). "Supraspinal involvement in the production of mechanical allodynia by spinal nerve injury in rats". Neurosci. Lett. 246 (2): 117-9. PMID 9627194. 
8. ^ Lee B, Won R, Baik E, Lee S, Moon C (2000). "An animal model of neuropathic pain employing injury to the sciatic nerve branches". Neuroreport 11 (4): 657-61. PMID 10757496. 
9. ^ Decosterd I, Woolf C (2000). "Spared nerve injury: an animal model of persistent peripheral neuropathic pain". Pain 87 (2): 149-58. PMID 10924808. 
10. ^ Vadakkan K, Jia Y, Zhuo M (2005). "A behavioral model of neuropathic pain induced by ligation of the common peroneal nerve in mice". The journal of pain : official journal of the American Pain Society 6 (11): 747-56. PMID 16275599. 
11. ^ w23 Nelson KA, Park KM, Robinovitz E, Tsigos C, Max MB. High-dose oral dextromethorphan versus placebo in painful diabetic neuropathy and postherpetic neuralgia. Neurology 1997;48:1212-8. PMID 9153445
12. ^ Abrams D, Jay C, Shade S, Vizoso H, Reda H, Press S, Kelly M, Rowbotham M, Petersen K (2007). "Cannabis in painful HIV-associated sensory neuropathy: a randomized placebo-controlled trial". Neurology 68 (7): 515-21. PMID 17296917. 
13. ^ [1]

Neuropathy related organizations

External links



The International Statistical Classification of Diseases and Related Health Problems (most commonly known by the abbreviation ICD
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List of ICD-10 codes. The version for 2007 is available online at [1]

Chapter Blocks Title
I Certain infectious and parasitic diseases
II Neoplasms
III Diseases of the blood and blood-forming organs and certain disorders involving the immune mechanism
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The International Statistical Classification of Diseases and Related Health Problems (most commonly known by the abbreviation ICD
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The following is a list of codes for International Statistical Classification of Diseases and Related Health Problems. These codes are in the public domain.

See also


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eMedicine is an online clinical medical knowledge base that was founded in 1996 by Scott Plantz and Richard Lavely, two medical doctors. It was sold to WebMD in January 2006.
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MeSH D010523 Peripheral neuropathy is the term for damage to nerves of the peripheral nervous system, which may be caused either by diseases of the nerve or from the side-effects of systemic illness.
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A nerve is an enclosed, cable-like bundle of axons (the long, slender projection of a neuron). Neurons are sometimes called nerve cells, though this term is technically imprecise since many neurons do not form nerves, and nerves also include the glial cells that
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MeSH D011115 Polyneuropathy is a neurological disorder that occurs when many peripheral nerves throughout the body malfunction simultaneously. It may be acute and appear without warning, or chronic and develop gradually over a longer period of time.
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Autonomic neuropathy (also called visceral neuropathy) is a disease of the non-voluntary, non-sensory nervous system (i.e. the Autonomic Nervous System) affecting mostly the internal organs such as the bladder muscles, the cardiovascular system, the digestive tract, and the
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MeSH D020422 Mononeuropathy (or "mononeuritis") is a type of neuropathy that only affects a single peripheral or cranial nerve. It is diagnostically useful to distinguish them from peripheral neuropathy and autonomic neuropathy because the limitation in scope makes it more
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MeSH D020422

Mononeuritis multiplex is the clinical picture that arises from problems with multiple individual nerves serially or almost simultaneously.

Synonyms

Mononeuropathy multiplex

Clinical findings


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The foot is a biological structure found in many animals that is used for locomotion. In many animals with feet, the foot is a separate organ at the terminal part of the leg made up of one or more segments or bones, generally including claws or nails.
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In common usage, a human leg is the lower limb of the body, extending from the hip to the ankle, and including the thigh, the knee, and the cnemis.[1] The largest bone in the human body, the femur, is in the leg.
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Small fiber peripheral neuropathy is a type of neuropathy. It is also called small fiber neuropathy, small fiber sensory neuropathy (SFSN), and C fiber neuropathy. Small nerve fibers are the nerve fibers near the skin's surface, which is why the symptoms deal with sensation.
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Idiopathic is an adjective used primarily in medicine meaning arising spontaneously or from an obscure or unknown cause. From Greek ἴδιος, idios (one's own) + παθος, pathos (suffering), it means approximately "a
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Enteric Neuropathy is a degenerative neuromuscular condition of the digestive system. In simple terms the gut stops functioning, due to degradation of the nerves and muscles. The condition affects all parts of the digestive tract.
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Diabetic neuropathy
Classification & external resources

ICD-10 E10.4, E11.4, E12.4, E13.4, E14.4
ICD-9 250.6

Diabetic neuropathies are neuropathic disorders that are associated with diabetes mellitus.
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Herpes zoster
Classification & external resources

Herpes zoster blisters on the neck and shoulder
ICD-10 B 02.
ICD-9 053

DiseasesDB 29119
MedlinePlus 000858
eMedicine med/1007   derm/180 emerg/823 oph/257 ped/996

Herpes zoster
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MeSH D001327 Autoimmunity is the failure of an organism to recognize its own constituent parts (down to the sub-molecular levels) as "self", which results in an immune response against its own cells and tissues.
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Coeliac disease
Classification & external resources

Biopsy of small bowel showing coeliac disease manifested by blunting of villi, crypt hyperplasia, and lymphocyte infiltration of crypts.
ICD-10 K 90.0
ICD-9 579.
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Chemotherapy is the use of chemical substances to treat disease. In its modern-day use, it refers to cytotoxic drugs used to treat cancer or the combination of these drugs into a standardized treatment regimen.
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An electric shock can occur upon contact of a human's body with any source of voltage high enough to cause sufficient current flow through the muscles or hair. The minimum current a human can feel is thought to be about 1 milliampere (mA).
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Posterior Ramus Syndrome, also referred to as Thoracolumbar Junction Syndrome, Maigne Syndrome and Dorsal Ramus Sundrome is caused by the unexplained activation of the primary division of a posterior ramus of a spinal nerve (Dorsal ramus of spinal nerve).
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Dysesthesia (dysaesthesia in British English) is a tactile hallucination. It signals that damage is being done to tissue when none is occurring. However, recent advances in neuroinflammation indicate that the patient is not actually hallucinating.
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Allodynia, meaning "other pain", is an exaggerated response to otherwise non-noxious stimuli and can be either static or mechanical. Allodynia is not referred pain, but can occur in other areas than the one stimulated; it is also dysesthetic.
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Pain is a sensation transmitted from sensory nerves through the spinal cord and to the sensory area of the cerebrum, where the sensation is perceived. It is defined by the International Association for the Study of Pain (IASP) as “an unpleasant sensory and emotional
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An opioid is a chemical substance that has a morphine-like action in the body. The main use is for pain relief. These agents work by binding to opioid receptors, which are found principally in the central nervous system and the gastrointestinal tract.
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Tertiary geological time interval covers roughly the time span between the demise of the non-avian dinosaurs and beginning of the most recent Ice Age, approximately 65 million to 1.8 million years ago.
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A systematic review is a literature review focused on a single question which tries to identify, appraise, select and synthesize all high quality research evidence relevant to that question.
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