Charcot-Marie-Tooth disease
Charcot-Marie-Tooth disease | |
The foot of a person with Charcot-Marie-Tooth. The lack of muscle, a high arch, and hammer toes are signs of the genetic disease. | |
ICD-10 | G60.0 |
ICD-9 | 356.1 |
DiseasesDB | 5815 Template:DiseasesDB2 |
MedlinePlus | 000727 |
MeSH | D002607 |
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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]
Synonyms and keywords: Hereditary motor and sensory neuropathy; peroneal Muscular Atrophy
Overview
Charcot-Marie-Tooth disease is a heterogeneous inherited disorder of nerves (neuropathy) that is characterized by loss of muscle tissue and touch sensation, predominantly in the feet and legs but also in the hands and arms in the advanced stages of disease. Though presently incurable, this disease is one of the most common inherited neurological disorders, with 36 in 100,000 affected.[1]
Description
The disorder is caused by the absence of molecules that are essential for normal function of the nerves due to errors in the genes coding these molecules. The absence of these chemical substances gives rise to dysfunction either in the axon or the myelin sheath of the nerve cell. Most of the mutations identified result in disrupted myelin production, however the most common mutations occur in gene MFN2, which doesn't seem to have anything to do with myelin. Instead MFN2 controls behaviour of mitochondria. Recent research showed that the mutated MFN2 causes mitochondria to form large clusters. In nerve cells these large clusters of mitochondria failed to travel down the axon towards the synapses. It is suggested these mitochondria clots make the synapses fail, resulting in CMT disease.[2]
The different classes of this disorder have been divided into the primary demyelinating neuropathies (CMT1, CMT3, and CMT4) and the primary axonal neuropathies (CMT2). Recent studies, however, show that the pathologies of these two classes are frequently intermingled, due to the dependence and close cellular interaction of Schwann cells and neurons. Schwann cells are responsible for myelin formation, enwrapping neural axons with their plasma membranes in a process called “myelination”.[3]
The molecular structure of the nerve depends upon the interactions between neurons, Schwann cells, and fibroblasts. Schwann cells and neurons, in particular, exchange signals that regulate survival and differentiation during development. These signals are important to CMT disease because a disturbed communication between Schwann cells and neurons, resulting from a genetic defect, is observed in this disorder.[3]
It is clear that interaction with demyelinating Schwann cells causes the expression of abnormal axonal structure and function, but we still do not know how these abnormalities result in CMT. One possibility is that the weakness and sensory loss experienced by patients with CMT is a result of axonal degradation. Another possibility is that axonal dysfunction occurs, not degeneration, and that this dysfunction is induced by demyelinating Schwann cells.[1]
Most patients experience demyelinating neuropathies, and this is characterized by a reduction in nerve conduction velocity (NCV), due to a partial or complete loss of the myelin sheath. Axonopathies, on the other hand, are characterized by a reduced compound muscle action potential (CMAP), while NCV is normal or only slightly reduced.[3]
The disease is named for those who classically described it: Jean-Martin Charcot (1825-1893) and his pupil Pierre Marie (1853-1940) ("Sur une forme particulière d'atrophie musculaire progressive, souvent familiale débutant par les pieds et les jambes et atteignant plus tard les mains", Revue médicale, Paris, 1886; 6: 97-138.), and Howard Henry Tooth (1856-1925) ("The peroneal type of progressive muscular atrophy", dissertation, London, 1886.)
Symptoms
Symptoms usually begin in late childhood or early adulthood. Usually, the initial symptom is foot drop due to involvement of the peroneal nerve, which is responsible for raising the feet, early in the course of the disease. This can also cause hammer toe, where the toes are always curled. Wasting of muscle tissue of the lower parts of the legs may give rise to "stork leg" or "inverted bottle" appearance. Weakness in the hands and forearms occurs in many people later in life as the disease progresses.
Symptoms and progression of the disease can vary. Breathing can be affected in some; so can hearing, vision, and the neck and shoulder muscles. Scoliosis is common. Hip sockets can be malformed. Gastrointestinal problems can be part of CMT, as can chewing, swallowing, and speaking (as vocal cords atrophy). A tremor can develop as muscles waste. Pregnancy has been known to exacerbate CMT, as well as extreme emotional stress. About the chemotherapy drug vincristine, the Charcot-Marie-Tooth Association classifies the drug as a Definite High Risk and states that vincristine has been proven hazardous and should be avoided by all CMT patients, including those with no symptoms.[4]
Diagnosis
The diagnosis is established by electromyography examination (which shows that the velocity of nerve impulse conduction is decreased and the time required to charge the nerve is increased) and nerve biopsy. Genetic markers have been identified for some, but not all forms of the disease.
Types of the disease
- CMT Type 1 (CMT1): Type 1 affects approximately 80% of CMT patients and is the most common type of CMT. The subtypes share clinical symptoms. Autosomal dominant. Causes demyelination, which can be detected by measuring nerve conduction velocities.
- CMT Type 2 (CMT2): Type 2 affects approximately 20-40% of CMT patients. Type 2 CMT is Autosomal dominant neuropathy with its main effect on the axon. The average nerve conduction velocity is slightly below normal, but generally above 38 m/s
- CMT Type 3 (CMT3): Type 3 affects a very few CMT patients.
- CMT Type 4 (CMT4): Type 4 affects a very few CMT patients.
- CMT X-Linked (CMTX): CMTX affects approximately 10-20% of CMT patients and is X-linked dominant. Approx 10% of X-linked CMT patients have some other form than CMTX.
More details on the types are provided in the table below:
Type | OMIM | Gene | Locus | Description |
CMT1A | 118220 | PMP22 | 17p11.2 | The most common form of the disease, 70-80% of Type 1 patients. Average NCV: 15-20 m/s when associated with essential tremor and ataxia, called Roussy-Levy Syndrome |
CMT1B | 118200 | MPZ | 1q22 | Caused by mutations in the gene producing protein zero (P0). 5-10% of Type 1 patients. Average NCV: <20 m/s |
CMT1C | LITAF | 16p13.1-p12.3 | Causes severe demyelination, which can be detected by measuring nerve conduction velocities. Autosomal dominant. Usually shows up in infancy. Average NCV: 26-42 m/s. Identical symptoms to CMT-1A. | |
CMD1D | EGR2 | 10q21.1-q22.1 | Average NCV: 15-20 m/s | |
CMT2A | 118210 | MFN2 or KIF1B | 1p36 | The cause is likely located on chromosome 1 for the mitofusion 2 protein. Some research has also linked this form of CMT to the protein kinesin 1B. Does not show up on nerve conduction velocity tests, because it is caused by axonopathy. |
CMT2B | 600882 | RAB7 (RAB7A, RAB7B) | 3q21. | |
CMT2B1 | LMNA | 1q22 | Autosomal recessive axonal CMT, (laminopathy) | |
CMT2C | 606071 | 12q23-q24 | May cause vocal cord, diaphragm, and distal weaknesses. | |
CMT2D | 601472 | GARS | 7p15 | Patients with mutations in the GARS gene tend to have more severe symptoms in the upper extremities (hands), which is atypical for CMT in general. |
CMT2E | NEFL | 8p21 | ||
CMT2F | 606595 | HSPB1 | 7q11-q21 | |
CMT2G | 608591 | 12q12-13 | ||
CMT2H | 607731 | GDAP1 | 8q13-q21.1 | |
CMT2J | 607736 | 1q22 | ||
CMT2K | 607831 | 8q13-q21.1 | ||
CMT2L | 608673 | 12q24 | ||
CMT3 | 145900 | varies | varies | Sometimes called Dejerine-Sottas disease. Rarely found. Autosomal recessive. Average NCV: Normal (50-60m/s) |
CMT4A | 214400 | GDAP1 | 8q13-q21.1 | Autosomal recessive. |
CMT4B1 | 601382 | MTMR2 | 11q22 | Autosomal recessive. |
CMT4B2 | CMT4B2 (SBF2) | 11p15 | May be called "SBF2/MTMR13". Autosomal recessive. | |
CMT4C | KIAA1985 (SH3TC2) | 5q32 | May lead to respiratory compromise. | |
CMT4D | 601455 | NDRG1 | 8q24.3 | Autosomal recessive, demyelinating, deafness |
CMT1E | 118300 | PMP22 | 17p11.2 | Autosomal dominant, demyelinating, deafness |
CMT4E | EGR2 | 10q21.1-10q22.1 | "CMT4E" is a tentative name | |
CMT4F | PRX | 19q13.1-19q13.2 | "CMT4F" is a tentative name | |
CMT4J | 611228 | KIAA0274 (FIG4) | 6q21 | Autosomal recessive |
CMTX1 | 302800 | GJB1 | Xq13.1 | Average NCV: 25-40 m/s |
CMTX2 | 302801 | Xq22.2 | ||
CMTX3 | 302802 | Xq26 | ||
CMT | 118301 | with Ptosis and Parkinsonism | ||
CMT | 302803 | type 1 aplasia cutis congenita |
Genetic testing
Genetic testing is available for many of the different types of Charcot-Marie-Tooth. For a listing of test availabilities, see GeneTests.org
External links
References
- ↑ 1.0 1.1 Krajewski, K.M., Lewis, R.A., Fuerst, D.R., Turansky, C., Hinderer, S.R., Gerbern, J., Kamholz, J. and M.E. Shy (2000) Brain 123:1516-1527 accessed 060220
- ↑ Baloh, R., Schmidt, R., Pestronk, A. and Milbrandt, J. (2007) The Journal of Neuroscience 27(2):422-430, http://www.jneurosci.org/cgi/content/abstract/27/2/422 accessed 070122
- ↑ 3.0 3.1 3.2 Berger, P., Young, P. and U. Suter (2002) Neurogenetics 4:1-15. http://www.springerlink.com/, accessed 060220
- ↑ CMT Association: Medical Alert
Template:Muscular Dystrophy Template:PNS diseases of the nervous system
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