Disease characteristics

Excerpted from the GeneReview: Dysferlinopathy

Dysferlinopathy includes a spectrum of muscle disease characterized by two major phenotypes: Miyoshi muscular dystrophy (MMD) and limb-girdle muscular dystrophy type 2B (LGMD2B); and two minor phenotypes: asymptomatic hyperCKemia and distal myopathy with anterior tibial onset (DMAT). MMD (median age of onset 19 years) is characterized by muscle weakness and atrophy, most marked in the distal parts of the legs, especially the gastrocnemius and soleus muscles. Over a period of years, the weakness and atrophy spread to the thighs and gluteal muscles. The forearms may become mildly atrophic with decrease in grip strength; the small muscles of the hands are spared. LGMD2B is characterized by early weakness and atrophy of the pelvic and shoulder girdle muscles in adolescence or young adulthood, with slow progression. Other phenotypes in this spectrum are scapuloperoneal syndrome and congenital muscular dystrophy. Asymptomatic hyperCKemia is characterized by marked elevation of serum CK concentration only. DMAT is characterized by early and predominant distal muscle weakness, particularly of the muscles of the anterior compartment of the legs. [from GeneReviews]

Authors:
Masashi Aoki | Toshiaki Takahashi view full author information

Additional descriptions

From OMIM
Miyoshi muscular dystrophy (MMD) is an autosomal recessive skeletal muscle disorder characterized by onset in young adulthood of distal muscle weakness affecting the upper and lower limbs but sparing the intrinsic hand muscles. Muscle weakness and atrophy particularly affects the gastrocnemius and soleus muscles, and can later spread to involve the thigh and gluteal muscles. Patients showed impaired tiptoe standing, difficulty in climbing stairs, and difficulty walking, but usually remain ambulatory. Serum creatine kinase is increased and muscle biopsies show myopathic and dystrophic changes with necrosis (summary by Miyoshi et al., 1986). Genetic Heterogeneity of Miyoshi Muscular Dystrophy Miyoshi muscular dystrophy is a genetically heterogeneous disorder: MMD2 (613318) has been mapped to chromosome 10p, and MMD3 (613319) is caused by mutation in the ANO5 gene (608662) on chromosome 11p14. See also Welander myopathy (604454), an autosomal dominant form of late-onset distal myopathy. http://www.omim.org/entry/254130

From MedlinePlus Genetics
Rarely, abnormal heart rhythms (arrhythmias) have developed in people with Miyoshi myopathy. Individuals with Miyoshi myopathy have highly elevated levels of an enzyme called creatine kinase (CK) in their blood, which often indicates muscle disease.

As Miyoshi myopathy slowly worsens, the muscle weakness and atrophy spread up the leg to the muscles in the thigh and buttock and can also involve the upper arm and shoulder muscles. Eventually, affected individuals may have difficulty climbing stairs or walking for an extended period of time. Some people with Miyoshi myopathy may eventually need wheelchair assistance.

Miyoshi myopathy is a muscle disorder that begins with weakness in the muscles that are located away from the center of the body (distal muscles), such as those in the legs. During early to mid-adulthood, affected individuals typically begin to experience muscle weakness and wasting (atrophy) in one or both calves. If only one leg is affected, the calves appear different in size (asymmetrical). Calf weakness can make it difficult to stand on tiptoe. https://medlineplus.gov/genetics/condition/miyoshi-myopathy

Clinical features

From HPO

Lower limb muscle weakness

MedGen UID:: 324478
•Concept ID:: C1836296
•: Finding

Weakness of the muscles of the legs.

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Decreased Achilles reflex

MedGen UID:: 324765
•Concept ID:: C1837323
•: Finding

Decreased intensity of the Achilles reflex (also known as the ankle jerk reflex), which can be elicited by tapping the tendon is tapped while the foot is dorsiflexed.

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Decreased/absent ankle reflexes

MedGen UID:: 340635
•Concept ID:: C1850816
•: Finding

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Muscle fibrillation

MedGen UID:: 65418
•Concept ID:: C0231531
•: Finding

Fine, rapid twitching of individual muscle fibers with little or no movement of the muscle as a whole as ascertained by electromyography (EMG). If a motor neuron or its axon is destroyed, the muscle fibers it innervates undergo denervation atrophy. This leads to hypersensitivity of individual muscle fibers to acetyl choline so that they may contract spontaneously. Isolated activity of individual muscle fibers is generally so fine it cannot be seen through the intact skin, although it can be recorded as a short-duration spike in the EMG.

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Tip-toe gait

MedGen UID:: 98104
•Concept ID:: C0427144
•: Finding

An abnormal gait pattern characterized by the failure of the heel to contact the floor at the onset of stance during gait.

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Muscular dystrophy

MedGen UID:: 44527
•Concept ID:: C0026850
•: Disease or Syndrome

The term dystrophy means abnormal growth. However, muscular dystrophy is used to describe primary myopathies with a genetic basis and a progressive course characterized by progressive skeletal muscle weakness and wasting, defects in muscle proteins, and histological features of muscle fiber degeneration (necrosis) and regeneration. If possible, it is preferred to use other HPO terms to describe the precise phenotypic abnormalities.

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Difficulty climbing stairs

MedGen UID:: 68676
•Concept ID:: C0239067
•: Finding

Reduced ability to climb stairs.

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Distal muscle weakness

MedGen UID:: 140883
•Concept ID:: C0427065
•: Finding

Reduced strength of the musculature of the distal extremities.

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Distal amyotrophy

MedGen UID:: 338530
•Concept ID:: C1848736
•: Disease or Syndrome

Muscular atrophy affecting muscles in the distal portions of the extremities.

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Deposits immunoreactive to beta-amyloid protein

MedGen UID:: 343012
•Concept ID:: C1853934
•: Finding

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Elevated circulating creatine kinase concentration

MedGen UID:: 69128
•Concept ID:: C0241005
•: Finding

An elevation of the level of the enzyme creatine kinase (also known as creatine phosphokinase (CK; EC 2.7.3.2) in the blood. CK levels can be elevated in a number of clinical disorders such as myocardial infarction, rhabdomyolysis, and muscular dystrophy.

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Abnormality of limbs
Abnormality of metabolism/homeostasis
- Elevated circulating creatine kinase concentration
Abnormality of the musculoskeletal system
Abnormality of the nervous system
- Muscle fibrillation
- Tip-toe gait

Term Hierarchy

GTR
MeSH

CClinical test, RResearch test, OOMIM, GGeneReviews, VClinVar

CROGVLimb-girdle muscular dystrophy
- CROGVAutosomal recessive limb-girdle muscular dystrophy
- CROGVMuscular dystrophy, limb-girdle, autosomal dominant

Phenotypic abnormality
- Abnormality of the musculoskeletal system
  - Abnormality of the musculature
    - Abnormal skeletal muscle morphology
      - Muscular dystrophy
        Miyoshi muscular dystrophy 1

Professional guidelines

PubMed

Genotype-phenotype correlation and natural history study of dysferlinopathy: a single-centre experience from India.

Nashi S, Polavarapu K, Bardhan M, Anjanappa RM, Preethish-Kumar V, Vengalil S, Padmanabha H, Geetha TS, Prathyusha PV, Ramprasad V, Joshi A, Chawla T, Unnikrishnan G, Sharma P, Huddar A, Uppilli B, Thomas A, Baskar D, Mathew S, Menon D, Arunachal G, Faruq M, Thangaraj K, Nalini A
Neurogenetics 2023 Jan;24(1):43-53. Epub 2022 Dec 29 doi: 10.1007/s10048-022-00707-3. PMID: 36580222

Left ventricular function in adults with muscular dystrophies: genotype-phenotype correlations.

Martins E, Silva-Cardoso J, Silveira F, Nadais G, Gonçalves FR
Rev Port Cardiol 2005 Jan;24(1):23-35. PMID: 15773664

See all (2)

Recent clinical studies

Etiology

Annexins and Membrane Repair Dysfunctions in Muscular Dystrophies.

Croissant C, Carmeille R, Brévart C, Bouter A
Int J Mol Sci 2021 May 17;22(10) doi: 10.3390/ijms22105276. PMID: 34067866 Free PMC Article

See all (1)

Synonym:	MMD1

Gene (location): Gene(s) directly associated with this condition or phenotype.	DYSF (2p13.2)

Monarch Initiative:	MONDO:0024545
OMIM®:	254130

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Miyoshi muscular dystrophy 1(MMD1)

Disease characteristics

Additional descriptions

Clinical features

Term Hierarchy

Professional guidelines

PubMed

Recent clinical studies

Etiology

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