Limb–girdle muscular dystrophy
Limb–girdle muscular dystrophy | |
---|---|
Other names | Erb's muscular dystrophy[1] |
Protein MYOT (also known as TTID one of the many genes whose mutations are responsible for this condition) | |
Specialty | Physical medicine and rehabilitation |
Symptoms | Pseudohypertrophy[2] |
Types | LGMD1 and LGMD2[3] |
Diagnostic method | Immunohistochemical dystrophin tests[4] |
Treatment | Occupational, speech and physical therapy[5] |
Limb–girdle muscular dystrophy or (LGMD) is a genetically and clinically heterogeneous group of rare muscular dystrophies.[6] It is characterised by progressive muscle wasting which affects predominantly hip and shoulder muscles. LGMD has an autosomal pattern of inheritance and currently has no known cure or treatment.[7][8]
Signs and symptoms
The symptoms of an individual with limb–girdle muscular dystrophy (LGMD) generally are great difficulty walking, going both up and down stairs, and rising from a chair. The inability to bend over or squat down is also present. Because of these difficulties, falling can occur frequently. Lifting certain objects, as well as difficulty extending the arms out or above the head, varies from difficult to impossible depending on the severity. Eventually, the abilities to walk and run deteriorate.[2][4]
Further presentations an individual with LGMD might have are:
- Pseudohypertrophy[2]
- Muscle hypertrophy[9]
- Respiratory muscle problems[9]
- Low back discomfort[2]
- Palpitation[2]
- Distal muscle problems[9]
- Facial muscle weakness[2]
- Weak shoulder muscle [2]
The disease inevitably gets worse over time, although progression is more rapid in some patients than others. Eventually the disease can affect other muscles such as the ones located in the face. The disease commonly leads to dependence on a wheelchair within years of symptom onset, but there is high inter-patient variability, with some patients maintaining mobility.[8][2]
The muscle weakness is generally symmetric, proximal, and slowly progressive. In most cases, pain is not present with LGMD, and mental function is not affected. LGMD can begin in childhood, adolescence, young adulthood or even later, the age of onset is usually between 10 and 30. Both genders are affected equally, when limb-girdle muscular dystrophy begins in childhood the progression appears to be faster and the disease more disabling. When the disorder begins in adolescence or adulthood the disease is generally not as severe and progresses more slowly. There is no sensory neuropathy or autonomic or visceral dysfunction at presentation.[medical citation needed]
Genetics
In terms of the genetics LGMD is an inherited disorder, though it may be inherited as a dominant or recessive genetic defect. The result of the defect is that the muscles cannot properly form certain proteins needed for normal muscle function. Several different proteins can be affected, and the specific protein that is absent or defective identifies the specific type of muscular dystrophy. Among the proteins affected in LGMD are α, β, γ and δ sarcoglycans. The sarcoglycanopathies could be possibly amenable to gene therapy.[3]
Diagnosis
The diagnosis of limb–girdle muscular dystrophy can be done via muscle biopsy, which will show the presence of muscular dystrophy, and genetic testing is used to determine which type of muscular dystrophy a patient has. Immunohistochemical dystrophin tests can indicate a decrease in dystrophin detected in sarcoglycanopathies. In terms of sarcoglycan deficiency there can be variance (if α-sarcoglycan and γ-sarcoglycan are not present then there's a mutation in LGMD2D).[4]
The 2014 Evidence-based guideline summary: Diagnosis and treatment of limb–girdle and distal dystrophies indicates that individuals suspected of having the inherited disorder should have genetic testing. Other tests/analysis are:[4][5]
- High CK levels(x10-150 times normal)
- MRI can indicate different types of LGMD.
- EMG can confirm the myopathic characteristic of the disease.
- Electrocardiography (cardiac arrhythmias in LGMD1B can occur)
Types
The "LGMD1" family is autosomal dominant, and the "LGMD2" family is autosomal recessive.[8] Limb–girdle muscular dystrophy is explained in terms of gene, locus, OMIM and type as follows:
Family | Inheritance | Type | OMIM | Gene | Locus | Notes |
---|---|---|---|---|---|---|
LGMD1 | autosomal dominant | LGMD1A | 159000 | TTID | ||
LGMD1B | 159001 | LMNA | ||||
LGMD1C | 607801 | CAV3 | ||||
LGMD1D | 603511 | DNAJB6 | ||||
LGMD1E | 601419 | DES | ||||
LGMD1F | 608423 | TNPO3 | 7q32.1–q32.2 | |||
LGMD1G | 609115 | HNRPDL | 4q21 | |||
LGMD1H | 613530 | 3p25.1–p23 | ||||
LGMD2 | autosomal recessive | LGMD2A | 253600 | CAPN3 | Often referred to as "calpainopathy."[10] | |
LGMD2B | 253601 | DYSF | LGMD with a mutation in this gene, along with Miyoshi Myopathy type 1 (MMD1 - 254130) are sometimes called dysferlinopathies.[11] | |||
LGMD2C | 253700 | SGCG | ||||
LGMD2D | 608099 | SGCA | ||||
LGMD2E | 604286 | SGCB | ||||
LGMD2F | 601287 | SGCD | ||||
LGMD2G | 601954 | TCAP | ||||
LGMD2H | 254110 | TRIM32 | ||||
LGMD2I | 607155 | FKRP | ||||
LGMD2J | 608807 | TTN | ||||
LGMD2K | 609308 | POMT1 | ||||
LGMD2L | 611307 | ANO5 | ||||
LGMD2M | 611588 | FKTN | ||||
LGMD2N | 607439 | POMT2 | ||||
LGMD2O | 606822 | POMGNT1 | ||||
LGMD2Q | 613723 | PLEC1 |
Treatment
There are few studies corroborating the effectiveness of exercise for limb–girdle muscular dystrophy. However studies have shown that exercise can, in fact, damage muscles permanently due to intense muscle contraction.[12] Physical therapy may be required to maintain as much muscle strength and joint flexibility as possible. Calipers may be used to maintain mobility and quality of life. Careful attention to lung and heart health is required, corticosteroids in LGMD 2C-F individuals, shows some improvement.[9] Additionally individuals can follow management that follows:[5]
- Occupational therapy
- Respiratory therapy
- Speech therapy
- Neutralizing antibody to myostatin should not be pursued
In terms of the prognosis of limb–girdle muscular dystrophy in its mildest form, affected individuals have near-normal muscle strength and function. LGMD isn't typically a fatal disease, though it may eventually weaken the heart and respiratory muscles, leading to illness or death due to secondary disorders. The frequency of limb–girdle muscular dystrophy ranges from 1 in 14,500 (in some instances 1 in 123,000).[6][8]
Research
There is a variety of research under way targeted at various forms of limb–girdle muscular dystrophy. Among the methods thought to hold promise for treatment include gene transfer therapy,[13] which works by inserting in cells of defective genes with a healthy gene.[14]
According to a review by Bengtsson et al. some success with AAV-mediated gene therapies (for different disorders) have increased interest in researchers, with CRISPR/Cas9 and exon-skipping helping these therapeutic goals along. Limb–girdle muscular dystrophies have many different types which are due to different gene mutations. LGMD2D is caused by a mutation in the α-sarcoglycan gene. Future treatment could be had by gene therapy through recombinant adeno-associated vectors.[15]
Conversely, according to a review by Straub, et al. there are several research issues that need to be targeted, the rareness of the disease, our poor understanding of the mechanism of LGMD2, and absence of patient cohorts, consequently biomarkers for individuals with LGMD2 are lacking. The review goes on to state that animal models for LGMD2 have been used to analyse therapeutic medications. Also adding that while prednisone has been used and has had positive effects on affected LGMD2 individuals there is still no evidence of its effectiveness in trials that are placebo-controlled.[16]
See also
References
- ^ Newfoundland, FRCP William Pryse-Phillips MD, FRCP(C) Faculty of Medicine Health Sciences Centre Memorial University of Newfoundland St John's (2009-05-06). Companion to Clinical Neurology. Oxford University Press, USA. p. 579. ISBN 9780199710041.
{{cite book}}
: CS1 maint: multiple names: authors list (link) - ^ a b c d e f g h MedlinePlus Encyclopedia: Limb-girdle muscular dystrophies
- ^ a b Reference, Genetics Home. "limb-girdle muscular dystrophy". Genetics Home Reference. Retrieved 2016-04-22.
- ^ a b c d "Limb-Girdle Muscular Dystrophy: Practice Essentials, Background, Pathophysiology". August 2018.
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: Cite journal requires|journal=
(help) - ^ a b c Narayanaswami, Pushpa; Weiss, Michael; Selcen, Duygu; David, William; Raynor, Elizabeth; Carter, Gregory; Wicklund, Matthew; Barohn, Richard J.; Ensrud, Erik (2014-10-14). "Evidence-based guideline summary: Diagnosis and treatment of limb-girdle and distal dystrophies". Neurology. 83 (16): 1453–1463. doi:10.1212/WNL.0000000000000892. ISSN 0028-3878. PMC 4206155. PMID 25313375.
- ^ a b "Limb-girdle muscular dystrophy".
- ^ "Limb-Girdle Muscular Dystrophy Treatment & Management: Medical Care, Surgical Care, Consultations". August 2018.
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(help) - ^ a b c d Pegoraro, Elena; Hoffman, Eric P. (1993-01-01). Pagon, Roberta A.; Adam, Margaret P.; Ardinger, Holly H.; Wallace, Stephanie E.; Amemiya, Anne; Bean, Lora JH; Bird, Thomas D.; Fong, Chin-To; Mefford, Heather C. (eds.). Limb-Girdle Muscular Dystrophy Overview. Seattle (WA): University of Washington, Seattle. PMID 20301582.update 2012
- ^ a b c d "Limb-girdle Muscular Dystrophy | Doctor".
- ^ Lasa-Elgarresta, J; Mosqueira-Martín, L; Naldaiz-Gastesi, N; Sáenz, A; López de Munain, A; Vallejo-Illarramendi, A (13 September 2019). "Calcium Mechanisms in Limb-Girdle Muscular Dystrophy with CAPN3 Mutations". International Journal of Molecular Sciences. 20 (18): 4548. doi:10.3390/ijms20184548. PMC 6770289. PMID 31540302.
{{cite journal}}
: CS1 maint: unflagged free DOI (link) - ^ Aoki, Masashi (March 5, 2015). "Dysferlinopathy". GeneReviews.
- ^ Siciliano G, Simoncini C, Giannotti S, Zampa V, Angelini C, Ricci G (2015). "Muscle exercise in limb girdle muscular dystrophies: pitfall and advantages". Acta Myologica. 34 (1): 3–8. PMC 4478773. PMID 26155063.
- ^ Liaison, Melanie Martinez, Office of Communications and Public. "Limb-Girdle Muscular Dystrophy". www.niams.nih.gov. Retrieved 2016-04-22.
{{cite web}}
: CS1 maint: multiple names: authors list (link) - ^ Reference, Genetics Home. "How does gene therapy work?". Genetics Home Reference. Retrieved 2016-04-23.
- ^ Bengtsson, Niclas E.; Seto, Jane T.; Hall, John K.; Chamberlain, Jeffrey S.; Odom, Guy L. (2016-04-15). "Progress and prospects of gene therapy clinical trials for the muscular dystrophies". Human Molecular Genetics. 25 (R1): R9 – R17. doi:10.1093/hmg/ddv420. ISSN 0964-6906. PMC 4802376. PMID 26450518.
- ^ Straub, Volker; Bertoli, Marta (2016-02-01). "Where do we stand in trial readiness for autosomal recessive limb girdle muscular dystrophies?". Neuromuscular Disorders. 26 (2): 111–125. doi:10.1016/j.nmd.2015.11.012. PMID 26810373. S2CID 23787096. – via ScienceDirect (Subscription may be required or content may be available in libraries.)
Further reading
- Cotta, Ana; Carvalho, Elmano; da-Cunha-Júnior, Antonio Lopes; Paim, Júlia Filardi; Navarro, Monica M.; Valicek, Jaquelin; Menezes, Miriam Melo; Nunes, Simone Vilela; Xavier Neto, Rafael (2014). "Common recessive limb girdle muscular dystrophies differential diagnosis: why and how?". Arquivos de Neuro-Psiquiatria. 72 (9): 721–734. doi:10.1590/0004-282X20140110. ISSN 0004-282X. PMID 25252238.
- Liu, Jian; Harper, Scott Q. (2012-08-01). "RNAi-based Gene Therapy for Dominant Limb Girdle Muscular Dystrophies". Current Gene Therapy. 12 (4): 307–314. doi:10.2174/156652312802083585. ISSN 1566-5232. PMC 4120526. PMID 22856606.
- ANGELINI, CORRADO; TASCA, ELISABETTA; NASCIMBENI, ANNA CHIARA; FANIN, MARINA (2014-12-01). "Muscle fatigue, nNOS and muscle fiber atrophy in limb girdle muscular dystrophy". Acta Myologica. 33 (3): 119–126. ISSN 1128-2460. PMC 4369848. PMID 25873780.