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Charcot–Marie–Tooth disease classifications
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    Charcot–Marie–Tooth disease classifications

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    Classifications of Charcot–Marie–Tooth disease refers to the types and subtypes of Charcot–Marie–Tooth disease (CMT), a genetically and clinically heterogeneous group of inherited disorders of the peripheral nervous system characterized by progressive loss of muscle tissue and touch sensation across various parts of the body. CMT is a result of genetic mutations in a number of genes.

    Clinical categories

    Type Name Incidence Notes
    CMT1 Demyelinating type Affects approximately 30% of CMT patients Causes severe demyelination, thereby impairing nerve conduction velocity.
    CMT2 Axonal type Affects approximately 20–40% of CMT patients Mainly affects axons. Tends to affect lower extremities more than upper extremities. Clinical symptoms are often less severe than in CMT1. As it is an axonopathy, average nerve conduction velocity is usually not affected (sometimes slightly below normal but mostly above 38 m/s).
    CMT3 Dejerine–Sottas disease Very rare Severely impaired nerve conduction velocity.
    CMT4 Spinal type
    CMT5 Pyramidal type
    CMT6 With optic atrophy
    CMTDI Dominant intermediate type
    CMTRI Recessive intermediate type
    CMTX X-linked type Affects approximately 10–20% of CMT patients This type encompasses all CMT forms that are inherited in an X-linked manner. Average NCV: 25–40 m/s.

    Genetic subtypes

    Type Subtype OMIM Gene Locus Inheritance Notes
    CMT1 CMT1A 118220 PMP22 17p11.2 Autosomal dominant The most common form of the disease, 70–80% of Type 1 patients. Average NCV: 20–25 m/s. Allelic with subtype CMT1E. When associated with subtype CMT1B (causing essential tremor and ataxia), it is called Roussy–Lévy syndrome.
    CMT1B 118200 MPZ 1q23.3 Autosomal dominant Responsible for 5–10% of Type 1 patients. Average NCV: < 15 m/s
    CMT1C 601098 LITAF 16p13.13 Autosomal dominant Usually shows up in infancy. Average NCV: 26–42 m/s. Symptoms are identical to CMT1A.
    CMT1D 607678 EGR2 10q21.3 Autosomal dominant Average NCV: 15–20 m/s
    CMT1E 118300 PMP22 17p11.2 Autosomal dominant Characterised by demyelination and loss of hearing; allelic with subtype CMT1A
    CMT1F 607734 NEFL 8p21.2 Autosomal dominant
    CMT1G 618279 PMP2 8q21.13 Autosomal dominant
    CMT2 CMT2A1 118210 KIF1B 1p36.22 Autosomal dominant
    CMT2A2A 609260 MFN2 1p36.22 Autosomal dominant
    CMT2A2B 617087 MFN2 1p36.22 Autosomal recessive
    CMT2B 600882 RAB7A
    RAB7B
    3q21.3 Autosomal dominant
    CMT2B1 605588 LMNA 1q22 Autosomal recessive A laminopathy
    CMT2B2 605589 MED25 19q13.33 Autosomal dominant
    CMT2C 606071 TRPV4 12q24.11 Autosomal dominant May cause vocal cord, diaphragm, and distal weakness
    CMT2D 601472 GARS 7p14.3 Autosomal dominant Symptoms are more severe in the upper extremities (hands), which is atypical for CMT
    CMT2E 607684 NEFL 8p21.2 Autosomal dominant
    CMT2F 606595 HSPB1 7q11.23 Autosomal dominant
    CMT2H 607731 GDAP1 8q21.11 Autosomal dominant Allelic with subtype CMT2K
    CMT2I 607677 MPZ 1q23.3 Autosomal dominant Allelic with subtype CMT2J and forms of CMT3
    CMT2J 607736 MPZ 1q23.3 Autosomal dominant Allelic with subtype CMT2I and forms of CMT3
    CMT2K 607831 GDAP1 8q21.11 Autosomal dominant Allelic with subtype CMT2H
    CMT2L 608673 HSPB8 12q24.23 Autosomal dominant Allelic with Autosomal dominant distal spinal muscular atrophy
    CMT2M 606482 DNM2 19p13.2 Autosomal dominant Full name: CMT2M, included; more commonly classified as subtype CMTDIB
    CMT2N 613287 AARS 16q22.1 Autosomal dominant
    CMT2O 614228 DYNC1H1 14q32.31 Autosomal dominant Allelic with spinal muscular atrophy with lower extremity predominance 1
    CMT2P 614436 LRSAM1 9q33.3 Autosomal dominant
    Autosomal recessive
    Juvenile or adult onset, slowly progressive
    CMT2Q 615025 DHTKD1 10p14 Autosomal dominant
    CMT2R 615490 TRIM2 4q31.3 Autosomal recessive
    CMT2S 616155 IGHMBP2 11q13.3 Autosomal recessive
    CMT2T 617017 MME 3q25 Autosomal recessive
    CMT2U 616280 MARS 12q13.3 Autosomal dominant
    CMT2V 616491 NAGLU 17q21.2 Autosomal dominant
    CMT2W 616625 HARS1 5q31.3 Autosomal dominant
    CMT2X 616668 SPG11 15q21.1 Autosomal recessive
    CMT2Y 616687 VCP 9p13.3 Autosomal dominant
    CMT2Z 616688 MORC2 22q12.2 Autosomal dominant
    CMT2CC 616924 NEFH 22q12.2 Autosomal dominant
    CMT2DD 618036 ATP1A1 1p13.1 Autosomal dominant
    CMT2EE 618400 MPV17 2p23.3 Autosomal recessive
    CMT3 CMT3 145900 MPZ
    EGR2
    PMP22
    PRX
    1q23.3
    10q21.3
    17p12
    19q13.2
    Autosomal dominant
    Autosomal recessive
    More commonly known as Dejerine–Sottas disease; subtype CMT4F sometimes included here
    CMT4 CMT4A 214400 GDAP1 8q21.11 Autosomal recessive Allelic with subtype CMTRIA
    CMT4B1 601382 MTMR2 11q21 Autosomal recessive
    CMT4B2 604563 SBF2 11p15.4 Autosomal recessive
    CMT4B3 615284 SBF1 22q13.33 Autosomal recessive
    CMT4C 601596 SH3TC2 5q32 Autosomal recessive May lead to respiratory compromise
    CMT4D 601455 NDRG1 8q24.3 Autosomal recessive Characterised by demyelination and loss of hearing
    CMT4E 605253 MPZ
    EGR2
    1q23.3
    10q21.3
    Autosomal recessive Also known as congenital hypomyelinating neuropathy; phenotype largely overlapping with subtype CMT4F
    CMT4F 145900 PRX 19q13.2 Autosomal recessive Phenotype largely overlapping with subtype CMT4E; may be the same as CMT3
    CMT4G 605285 HK1 10q22.1 Autosomal recessive Also known as Russe-type hereditary motor and sensory neuropathy (HMSNR); second most common cause of CMT in the Spanish Roma population
    CMT4H 609311 FGD4 12p11.21 Autosomal recessive
    CMT4J 611228 FIG4 6q21 Autosomal recessive Allelic to amyotrophic lateral sclerosis type 11
    CMT5 CMT5 600361 ? 4q34.3–q35.2 Autosomal dominant Also known as CMT with pyramidal features; onset in 2nd decade of life with distal muscle wasting, particularly in legs
    CMT6 CMT6 601152 MFN2 1p36.22 Autosomal dominant Characterised by optic atrophy, hence known also as CMT with optic atrophy. Also known as hereditary motor and sensory neuropathy type VI.
    CMTDI CMTDIA 606483 ? 10q24.1–q25.1 Autosomal dominant
    CMTDIB 606482 DNM2 19p13.2 Autosomal dominant Also classified as subtype CMT2M
    CMTDIC 608323 YARS 1p35.1 Autosomal dominant
    CMTDID 607791 MPZ 1q23.3 Autosomal dominant
    CMTDIE 614455 INF2 14q32.33 Autosomal dominant
    CMTDIF 615185 GNB4 3q26.33 Autosomal dominant
    CMTRI CMTRIA 608340 GDAP1 8q21.11 Autosomal recessive Allelic with subtype CMT4A
    CMTRIB 613641 KARS 16q23.1 Autosomal recessive
    CMTX CMTX1 302800 GJB1 Xq13.1 X-linked dominant Responsible for approximately 90% of CMTX patients; some studies put this number significantly higher. Note that different mutations of GJB1 may produce markedly different forms of Charcot–Marie–Tooth disease.
    CMTX2 302801 CMTX2 Xq22.2 X-linked recessive
    CMTX3 302802 CMTX3 Xq26 X-linked recessive
    CMTX4 310490 NAMSD Xq24–q26.1 X-linked recessive Also known as Cowchock syndrome
    CMTX5 311070 PRPS1 Xq22.3 X-linked recessive Also known as Rosenberg–Chutorian syndrome; signs include optic atrophy, polyneuropathy and deafness
    CMTX6 300905 PDK3 Xp22.11 X-linked dominant
    Type Subtype OMIM Gene Locus Inheritance Notes

    It has to be kept in mind that sometimes a particular patient diagnosed with CMT can exhibit a combination of any of the above gene mutations; thus, in these cases precise classification can be arbitrary.


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