Spinal Muscular Atrophy (SMA): Difference between revisions

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== Introduction ==
== Introduction ==
Spinal Muscular Atrophy (SMA) is a genetic condition under the scope of the [[Neurodegenerative Disease|neurodegenerative disorders]] and [[Motor Neurone Disease MND]]. It is characterised by degeneration of alpha motor neurons in the [[Spinal cord anatomy|spinal cord]] that affects the control of voluntary [[muscle]] movement. The disease is characterised as an autosomal recessive condition with a prevalence of approximately 1 in 6-10,000 births affected by SMA with a carrier frequency of 1 in 35-70<ref name=":0">Darras BT, Markowitz JA, Monani UR, De Vivo DC. Spinal muscular atrophies (2015) Neuromuscular Disorders of Infancy. Childhood, and Adolescence: A Clinician’s Approach.:117-45.</ref>. Classification of SMA type depends on the age of onset and the highest level of motor function achieved<ref name=":0" />           
Spinal Muscular Atrophy (SMA) is a genetic disorder also considered to be a [[Neurodegenerative Disease|neurodegenerative disorder,]] specifically a [[Motor Neurone Disease MND|motor neurone disease]]. SMA is characterised by the degeneration of alpha motor neurons in the [[Spinal cord anatomy|spinal cord]], affecting the control of voluntary [[muscle]] movement.<ref name=":0">Darras BT, Markowitz JA, Monani UR, De Vivo DC. Spinal muscular atrophies (2015) Neuromuscular Disorders of Infancy. Childhood, and Adolescence: A Clinician’s Approach.:117-45.</ref> It occurs in roughly one in 6,000–10,000 births.<ref name=":2" /> There are several classifications of SMA, which are assigned based on the age at which symptoms first occur along with the highest level of muscle activation attained or expected to be attained. <ref name=":0" /><ref name=":3" />           
{{#ev:youtube|https://www.youtube.com/watch?v=5mI_ZsWkkc4|width}}<ref>Genentech. Understanding Spinal Muscular Atrophy (SMA). Available from: https://www.youtube.com/watch?v=5mI_ZsWkkc4 (last accessed 7.6.2019)</ref>  
{{#ev:youtube|https://www.youtube.com/watch?v=5mI_ZsWkkc4|width}}<ref>Genentech. Understanding Spinal Muscular Atrophy (SMA). Available from: https://www.youtube.com/watch?v=5mI_ZsWkkc4 (last accessed 7.6.2019)</ref>
 
== Pathological Process ==
== Clinically Relevant Anatomy  ==
SMA is considered to be an [[Genetic Conditions and Inheritance|autosomal recessive]] condition resulting from the homozygous deletion of the gene SMN1 (survival of motor neuron 1).<ref name=":2" />  In some cases, it is possible for the neighboring SMN2 gene to compensate for a lack of the SMN1 geneTherefore, if there is one or more additional copies of the SMN2 gene, later-onset and less severe SMA symptoms can occur.<ref name=":3">Umphrend D, Lazaro R, Roller M, Burton G. Umphrend's Neurological Rehabilitation. Sixth Edition. St. Louis, MO, USA. Elsevier Mosby, 2013.</ref><br>
 
[[File:Autosomal recessive2.png|frameless|center|480x480px|Autosomal Recessive ]]
SMA is caused by deficiency of a motor neuron protein called SMN (Survival Motor Neuron). This protein is essential for normal motor function and the lack of it is caused by genetic flaws in chromosome 5 in the gene SMN1. The neighbouring SMN2 gene can compensate for some of the functions of SMN1 and this is where some of the pharmaceutical companies trying to develop a drug which can enhance the effect of SMN2<br>
 
== Pathological Process  ==
Spinal Muscular Atrophy is an autosomal recessive condition due in most cases to the homozygous deletion of the SMN1 gene<ref>Mercuri E, Bertini E, Iannaccone ST. [https://www.sciencedirect.com/science/article/pii/S1474442212700613 Childhood spinal muscular atrophy: controversies and challenges]. The Lancet Neurology. 2012 May 1;11(5):443-52.</ref>. This means that both parents of the affected individual are only carriers of the affected gene. Therefore, they are not going to present with any symptoms of the disease and this is what makes SMA difficult to foresee and apply preventable measures.  <br>
 
== Clinical Presentation and Classification  ==
== Clinical Presentation and Classification  ==


Spinal Muscular Atrophy (SMA) is the second most common neuromuscular disorder in childhood. People affected by the mildest types of SMA have proximal weakness and impaired ambulation. Furthermore, fatigue is a symptom present in almost every case of SMA which may also lead to impaired function and endurance. Current research in the area shows that there is a good correlation between upper and lower limb function in patients with the disease. There are several types of SMA, which start at different ages and may present with various phenotypes<ref>Spinal muscular atrophy. Available from https://www.nhs.uk/conditions/spinal-muscular-atrophy-sma/ Last accessed 14/08/2022</ref>.
SMA is classified based on the age at which symptoms first occur as well as the level of muscle activation attained or expected to be attained. <ref name=":0" /><ref name=":3" />SMA symptoms range in severity but often include hypotonia, muscle weakness (proximal muscles greater than distal muscles and lower extremity than upper extremity), bone or joint issues, difficulty swallowing, and/or difficulty breathing.<ref name=":3" /><ref>National Health Service. Spinal muscular atrophy. Available from https://www.nhs.uk/conditions/spinal-muscular-atrophy-sma/ Last accessed 4/24/2023.</ref>  


{{#ev:youtube|G5yIdH0yans|300}}<ref>Cure SMA. Learn to Spot the Warning Signs of SMA – Snapshot of Hallmark Symptoms (Video 9) Available from: https://www.youtube.com/watch?v=G5yIdH0yans&feature=emb_logo [last accessed 31/01/2021]</ref>
{{#ev:youtube|G5yIdH0yans}}<ref>Cure SMA. Learn to Spot the Warning Signs of SMA – Snapshot of Hallmark Symptoms (Video 9) Available from: https://www.youtube.com/watch?v=G5yIdH0yans&feature=emb_logo [last accessed 31/01/2021]</ref>


=== Types of SMA ===
=== Types of SMA ===
* SMA type I (Werdnig-Hoffmann disease) - affects babies less than six months old and is the most severe type of the disease. Sitting unsupported may never be achieved. Present with profound hypotonia, symmetrical flaccid paralysis, and no head control with poor spontaneous mobility and reduced antigravity movements of limbs.
{| class="wikitable"
* SMA type II - develops in babies between 7 and 18 months old. This type is less severe than type I and most children survive into adulthood and can live long, fulfilling lives. May achieve the ability to sit unsupported but may not be able to walk independently. Joint contractures and kyphoscoliosis are very common along with fine tremors of the upper extremities.
|+
* SMA type III (Kugelberg-Welander disease) - appears after 18 months of age and is the least severe type affecting children. SMA type III has been divided into two further sub-categories: SMA IIIa and SMA IIIb - according to the time when the first symptoms of the condition appear (if before or after 3 years of age).
!
* SMA type IV - this type of SMA patients are diagnosed in adulthood and they present with only mild problems.
!'''TYPE 1 (MOST SEVERE)(Werdnig-Hoffmann disease of acute infantile SMA)'''
!'''TYPE 2'''
!'''TYPE 3 (Kugelberg-Welander syndrome or juvenile SMA)'''
!'''TYPE 4'''
|-
|'''AGE OF ONSET'''
|First 6 months
|6-18 months
|18 months or older
|Adulthood (after 21 years)
|-
|'''SYMPTOMS'''
|
* Reduce muscle tone
* Contractures
* Reflexes absent
* Swallowing,feeding difficulty
|
* Can sit  
* Unable to stand/walk without support
* Respiratory difficulties
|
* Walk independently
* Difficulty in running, stair climbing
* Scoliosis
|Mild to moderate leg weakness.  
|-
|'''LIFE EXPENTANCY'''
|Die before 2 years  <ref name=":3" />
|Adolescence or young adulthood <ref name=":3" />
|Normal lifespan (with regular physical rehabilitations) <ref name=":3" />
|Normal lifespan(with little physical training) <ref name=":3" />
|}


== Diagnostic Procedures  ==
== Diagnostic Procedures  ==


Diagnoses could be made by prenatal screening or by gene panel investigation and/or muscle biopsy. In the early stages, the diagnosis may be suspected due to symptoms like floppiness and muscular weakness. Children with type I SMA can present with a lack of head control, minimal to absent anti-gravity movements and severe respiratory complications.
Diagnosis generally starts with genetic testing to determine whether or not the SMN1 gene is absent. Genetic testing has been found to have a 95% sensitivity (test shows the absence of SMN1 the  gene when it is truly absent) and an almost 100% specificity (test shows the  presence of SMN the gene when it is truly present). If genetic testing does return a result consistent with clinical signs and symptoms, additional testing in the form of electrocardiography, a muscle biopsy, a nerve conduction velocity study, or blood tests can be performed.<ref name=":3" /><ref>National Institute of Neurological Disorders and Stroke. Spinal Muscle Atrophy. Available from https://www.ninds.nih.gov/health-information/disorders/spinal-muscular-atrophy (accessed 4/26/2023).</ref>
 
The first step in diagnosing someone with SMA would be by taking a full clinical examination and family history.  A blood test might be required to look at the amount of creatine kinase (CK), an investigation to indicate if muscle damage has occurred. High levels of CK in the blood is not damaging itself, but it is an important indicator of a muscle disorder condition. Electrophysiological tests such as electromyography (EMG), and nerve conduction study should be performed, if EMG suggests a motor neuron disease, then, further testing should be done.  
 
Further investigation will probably include genetic testing as this is the most accurate way to diagnose if a patient has Spinal Muscular Atrophy.


== Differential Diagnosis ==
== Differential Diagnosis ==
Neuromuscular conditions:
[[File:DD of spinal Muscular Atrophy.png|center|DD of spinal Muscular Atrophy<ref>Prior TW, Leach ME, Finanger E. Table 5. [Disorders to Consider in the Differential Diagnosis of Spinal Muscular Atrophy (SMA)]. [Internet]. Nih.gov. University of Washington, Seattle; 2020 [cited 2024 Feb 6]. Available from: <nowiki>https://www.ncbi.nlm.nih.gov/books/NBK1352/table/sma.T.disorders_to_consider_in_the_diffe/</nowiki>
* [[Duchenne Muscular Dystrophy|Duchenne]] Muscular Dystrophy
* [[Charcot-Marie-Tooth Disease: A Case Study|Charcot-Marie-Tooth]]
* [[Amyotrophic Lateral Sclerosis]
Congenital Myopathies:
* congenital myotonic dystrophy,  
* congenital myasthenic syndromes,
* metabolic [[myopathies]]
Congenital disorders of the motor neuron and the peripheral nerve (congenital hypomyelinating neuropathy).


Non-Neuromuscular Conditions:
‌</ref>|thumb|1006x1006px]]
* [[Prader-Willi Syndrome|Prader-Willi syndrome]],
* acute hypoxic ischemic encephalopathy,
* neonatal [[sepsis]] and
* dyskinetic or metabolic conditions
The tools that can address these differential diagnostic possibilities beyond the clinical examination and careful family history are CK determination, EMG/nerve conduction studies, MRI of the brain, muscle biopsy, and specific genetic or metabolic testing.
 
<br>


== Outcome Measures  ==
== Outcome Measures  ==


There are several outcome measures which can be used to detect changes in the natural history of patients with SMA. These tools should be appropriately selected according to the age and severity of the disease.   
There are several outcome measures which can be used to detect changes in the course of treatment for patients with SMA. These tools should be appropriately selected according to the age and severity of the disease.   
* [[Six Minute Walk Test / 6 Minute Walk Test|Six-Minute Walking Test (6MWT)]] - The Six-Minute-Walking-Test can be safely performed in ambulant patients with SMA. It has been proven to detect fatigue-related changes in this population of patients and also correlates with other established outcome measures for patients with spinal muscular atrophy<ref>Montes J, McDermott MP, Martens WB, Dunaway S, Glanzman AM, Riley S, Quigley J, Montgomery MJ, Sproule D, Tawil R, Chung WK. [https://n.neurology.org/content/74/10/833.short Six-Minute Walk Test demonstrates motor fatigue in spinal muscular atrophy.] Neurology. 2010 Mar 9;74(10):833-8.</ref>.
* [[Six Minute Walk Test / 6 Minute Walk Test|'''Six-Minute Walking Test (6MWT)''']] - The Six-Minute-Walking-Test can be safely performed in ambulant patients with SMA. It has been proven to detect fatigue-related changes in this population of patients and also correlates with other established outcome measures for patients with spinal muscular atrophy<ref>Montes J, McDermott MP, Martens WB, Dunaway S, Glanzman AM, Riley S, Quigley J, Montgomery MJ, Sproule D, Tawil R, Chung WK. [https://n.neurology.org/content/74/10/833.short Six-Minute Walk Test demonstrates motor fatigue in spinal muscular atrophy.] Neurology. 2010 Mar 9;74(10):833-8.</ref>.


* [[Revised Hammersmith Scale (RHS) for Spinal Muscular Atrophy|Revised Hammersmith Scale for SMA (RHS)]] - The RHS is predominantly used in patients with SMA type 2 and 3. In a combination with the WHO motor milestones, the scale can be more sensitive toward the description of the SMA phenotype. The RHS has been designed to capture a wide range of abilities across a broad spectrum of SMA, from very young children to adolescents and adults<ref>Ramsey D, Scoto M, Mayhew A, Main M, Mazzone ES, Montes J, de Sanctis R, Dunaway Young S, Salazar R, Glanzman AM, Pasternak A. [https://journals.plos.org/plosone/article?id=10.1371/journal.pone.0172346 Revised Hammersmith Scale for spinal muscular atrophy: A SMA specific clinical outcome assessment tool]. PloS one. 2017 Feb 21;12(2):e0172346.</ref>.
* '''[[Revised Hammersmith Scale (RHS) for Spinal Muscular Atrophy|Revised Hammersmith Scale for SMA (RHS)]] -''' The RHS is predominantly used in patients with SMA types 2 and 3. In combination with the World Health Organisation (WHO) motor milestones, the scale can be more sensitive toward the description of the SMA phenotype. The RHS has been designed to capture a wide range of abilities across a broad spectrum of SMA, from very young children to adolescents and adults<ref name=":2">Ramsey D, Scoto M, Mayhew A, Main M, Mazzone ES, Montes J, de Sanctis R, Dunaway Young S, Salazar R, Glanzman AM, Pasternak A. [https://journals.plos.org/plosone/article?id=10.1371/journal.pone.0172346 Revised Hammersmith Scale for spinal muscular atrophy: A SMA specific clinical outcome assessment tool]. PloS one. 2017 Feb 21;12(2):e0172346.</ref>.


* [[WHO Developmental Milestones]] - The WHO scales aim to link the growth of the child and motor development in one single reference. The final version of the protocol includes six items: "Sitting without support", "Hands-and-knees crawling", "Standing with assistance", "Walking with assistance", "Standing alone", and "Walking alone". The WHO provides important information about a child's gross motor development in different cultural settings<ref>Wijnhoven TM, de Onis M, Onyango AW, Wang T, Bjoerneboe GE, Bhandari N, Lartey A, Rashidi BA. [https://journals.sagepub.com/doi/abs/10.1177/15648265040251S106 Assessment of gross motor development in the WHO Multicentre Growth Reference Study]. Food and nutrition bulletin. 2004;25(1_suppl_1):S37-45.</ref>.
* '''[[WHO Developmental Milestones]] -''' The WHO scales aim to link the growth of the child and motor development in one single reference. The final version of the protocol includes six items: "Sitting without support," "hands-and-knees crawling," "standing with assistance," "walking with assistance," "standing alone," and "walking alone.". The WHO provides important information about a child's gross motor development in different cultural settings<ref>Wijnhoven TM, de Onis M, Onyango AW, Wang T, Bjoerneboe GE, Bhandari N, Lartey A, Rashidi BA. [https://journals.sagepub.com/doi/abs/10.1177/15648265040251S106 Assessment of gross motor development in the WHO Multicentre Growth Reference Study]. Food and nutrition bulletin. 2004;25(1_suppl_1):S37-45.</ref>.


* Revised Upper Limb Module (RULM) for SMA - The RULM is a specifically designed outcome measure for upper limb function in patients with Spinal Muscular Atrophy. The scale has shown good reliability and validity, which makes it a good choice for assessing arm function in children and adults with SMA<ref>Mazzone ES, Mayhew A, Montes J, Ramsey D, Fanelli L, Young SD, Salazar R, De Sanctis R, Pasternak A, Glanzman A, Coratti G. [https://onlinelibrary.wiley.com/doi/abs/10.1002/mus.25430 Revised upper limb module for spinal muscular atrophy: development of a new module.] Muscle & nerve. 2017 Jun;55(6):869-74.</ref>.
* '''Revised Upper Limb Module (RULM) for SMA''' - The RULM is a specifically designed outcome measure for upper limb function in patients with Spinal muscular atrophy. The scale has shown good reliability and validity, which makes it a good choice for assessing arm function in children and adults with SMA<ref>Mazzone ES, Mayhew A, Montes J, Ramsey D, Fanelli L, Young SD, Salazar R, De Sanctis R, Pasternak A, Glanzman A, Coratti G. [https://onlinelibrary.wiley.com/doi/abs/10.1002/mus.25430 Revised upper limb module for spinal muscular atrophy: development of a new module.] Muscle & nerve. 2017 Jun;55(6):869-74.</ref>.


== Management / Interventions  ==
== Management / Interventions  ==
Spinal Muscular Atrophy (SMA) is a severe genetic condition which requires precise diagnosis and extensive physiotherapy treatment in order to protect the muscles from rapid deterioration and development of contractures. The management of SMA must be as a part of a broad multi-disciplinary team which should include rehabilitation, spinal management, orthopaedics, nutritional and gastrointestinal management.  
The management of SMA warrants a multi-disciplinary approach coordinated by the patient's primary clinician.<ref name=":4">Mercuri E, Finkel RS, Muntoni F, Wirth B, Montes J, Main M, Mazzone ES, Vitale M, Snyder B, Quijano-Roy S, Bertini E. [https://www.sciencedirect.com/science/article/pii/S0960896617312841 Diagnosis and management of spinal muscular atrophy: Part 1: Recommendations for diagnosis, rehabilitation, orthopedic and nutritional care]. Neuromuscular Disorders. 2018 Feb 1;28(2):103-15.</ref>


Recently, it has been stated that SMA might be a multi-organ disease and a more detailed examination should be performed. Further recommendations have been made on pulmonary management and acute care issues in the severe forms of spinal muscular atrophy<ref>Mercuri E, Finkel RS, Muntoni F, Wirth B, Montes J, Main M, Mazzone ES, Vitale M, Snyder B, Quijano-Roy S, Bertini E. [https://www.sciencedirect.com/science/article/pii/S0960896617312841 Diagnosis and management of spinal muscular atrophy: Part 1: Recommendations for diagnosis, rehabilitation, orthopedic and nutritional care]. Neuromuscular Disorders. 2018 Feb 1;28(2):103-15.</ref>.
==== Orthopedic Management ====
* '''Spinal deformities''' 
** Scoliosis 
*** Bracing
**** Limit scoliosis progression during growth years, not corrective
*** Surgical intervention (hardware implantation)
**** The goal is to ultimately promote better breathing mechanics and sitting alignment <ref name=":4" />
* '''Contractures'''
** Management through Physical Therapy
** Surgical intervention if significant impairment or pain is present
* '''Fractures'''
** Cast immobilization if non-ambulatory
** Surgical fixation, if ambulatory


<u>Medical Management</u><ref>Tiziano FD, Lomastro R, Pinto AM, Messina S, D'Amico A, Fiori S, Angelozzi C, Pane M, Mercuri E, Bertini E, Neri G. [https://jmg.bmj.com/content/47/12/856.short Salbutamol increases survival motor neuron (SMN) transcript levels in leucocytes of spinal muscular atrophy (SMA) patients: relevance for clinical trial design]. Journal of medical genetics. 2010 Dec 1;47(12):856-8.</ref>:
==== Nutrition Management ====
* Neuroprotective Drugs like riluzole,
* Maintenance of adequate nutritional intake
* Drugs to improve energy metabolism and
** Adequate calcium and vitamin D
* Drugs affecting the gene expression of SMN
* Maintenance of appropriate body mass index
<u>Gene Therapy:</u>
* Screening and monitoring for complications such as...
** Glucose abnormalities
** Hyperlipidemia
** Abnormal fatty acid metabolism
** Metabolic acidosis <ref name=":4" />


Along with advances in medical management, gene therapy approaches have been evaluated for SMA, using viral vectors to replace SMN1 gene<ref>Passini MA, Cheng SH. [https://www.sciencedirect.com/science/article/pii/S1471491411000037 Prospects for the gene therapy of spinal muscular atrophy]. Trends in molecular medicine. 2011 May 1;17(5):259-65.</ref>.
==== Speech and Language Pathology ====
* Screening and intervention for dysphagia


<u>Stem Cell Therapy:</u> cellular replacement strategy in the treatment of SMA<ref>Harper JM, Krishnan C, Darman JS, Deshpande DM, Peck S, Shats I, Backovic S, Rothstein JD, Kerr DA. [https://www.pnas.org/doi/abs/10.1073/pnas.0401103101 Axonal growth of embryonic stem cell-derived motoneurons in vitro and in motoneuron-injured adult rats]. Proceedings of the National Academy of Sciences. 2004 May 4;101(18):7123-8.</ref>. However, this therapy is still in the testing stages.
<u>Medical Management</u><ref>Tiziano FD, Lomastro R, Pinto AM, Messina S, D'Amico A, Fiori S, Angelozzi C, Pane M, Mercuri E, Bertini E, Neri G. [https://jmg.bmj.com/content/47/12/856.short Salbutamol increases survival motor neuron (SMN) transcript levels in leucocytes of spinal muscular atrophy (SMA) patients: relevance for clinical trial design]. Journal of medical genetics. 2010 Dec 1;47(12):856-8.</ref>:
 
* Neuroprotective drugs like riluzole
Cell replacement may be achieved by :
* Drugs to improve energy metabolism
* Transplantation of stem cell-derived cells which have undergone maturation in vitro
* Drugs affecting the gene expression of SMN. <ref name=":4" />
* Activation of endogenous stem cells in the CNS


<br>
==== Gene Therapy: ====
* Along with advances in medical management, gene therapy approaches have been evaluated for SMA, using viral vectors to replace the SMN1 gene.<ref>Passini MA, Cheng SH. [https://www.sciencedirect.com/science/article/pii/S1471491411000037 Prospects for the gene therapy of spinal muscular atrophy]. Trends in molecular medicine. 2011 May 1;17(5):259-65.</ref>


=== Physiotherapy ===
=== Physiotherapy ===
* Assessment of the patient with neuromuscular disease and particularly with SMA is of great importance. Looking at baseline function, joint range and power will assist the physiotherapist to follow on the progression of the condition.
* [https://reader.elsevier.com/reader/sd/pii/S0960896617312841?token=06107BB5462E8CF638ADE9FB80BEB5EDA90CAC62325B040CC5B20C283159DFFF3F04502759BE0581AC12817D96508543&originRegion=us-east-1&originCreation=20230507152629 Merconi et al.]<ref name=":4" /> provide a comprehensive outline of physiotherapy management for SMA broken down by functional level.
* Orthotics
{| class="wikitable"
* Splinting
|+Table derived from [https://reader.elsevier.com/reader/sd/pii/S0960896617312841?token=06107BB5462E8CF638ADE9FB80BEB5EDA90CAC62325B040CC5B20C283159DFFF3F04502759BE0581AC12817D96508543&originRegion=us-east-1&originCreation=20230507152629 Merconi et al.]<ref name=":4" />
* Taping
!'''Functional Level'''
* Management of contractures 
!'''Goals'''
* Exercise and activity
!'''Possible Deficits'''
!'''Possible Interventions/Adaptations'''
|-
|Patients not able to sit unsupported
|
* Facilitate optimal function
|
* Deficiencies in postural control
* Decreased sitting tolerance
* Contractures
* Muscular weakness
|
* Thoracic and cervical bracing to promote appropriate positioning and posture
* Orthoses, splints, serial casting, AAROM, PROM, stretching, and or standing frame use to facilitate contracture prevention and management
* Adaptive equipment
** Sitting brace or sitting system
** Postural support equipment
** Positioning equipment
** Hoist or lift system
** Recline/tilt wheelchair
* Eye tracking equipment for communication and computer use
|-
|Patients able to sit unsupported
|
* Contracture management/prevention
* Scoliosis management/prevention
* Facilitate independence with function and mobility
|
* Deficiencies in postural control
* Contractures
* Muscle weakness
|
* Thoracic and cervical bracing to promote appropriate posture
* Orthoses, splints, serial casting, AAROM, PROM, stretching, and or standing frame use to facilitate contracture prevention and management
* Adaptive equipment
** If needed, any equipment suggested for patients not able to sit unsupported
** Gait training devices
** UE support devices
** Power or lightweight wheelchair with appropriate postural support
|-
|Patients able to ambulate
|
* Facilitate highest level of function
* Improve or maintain joint ROM/contracture management and or prevention
* Improve of maintain endurance
* Improve or maintain balance
|
*Deficiencies in postural control
*Contractures
* Muscle weakness
* Decreased endurance
* Decreased balance
|
*Thoracic and cervical bracing to promote appropriate posture (while in sitting)
* Orthoses, splints, serial casting, AAROM, PROM, stretching, and or standing frame use to facilitate contracture prevention and management
* Adaptive equipment
** If needed, any equipment suggested for patients not able to sit unsupported
** Power wheelchair, lightweight wheelchair, or scooter for longer distances
* Gait training for improvement of endurance, efficiency, and safety
* Balance training
|}


=== Respiratory Care ===
=== Respiratory Care ===
Many children and adults with Spinal Muscular Atrophy will be dependent on pulmonary management due to loss of muscle function. When a patient with SMA has a respiratory failure they need to be transferred on non-invasive positive pressure ventilation (NIV). In order for this to be implemented in the best possible way, a respiratory physiotherapist should be involved in the assessment and the management of pulmonary complications<ref name=":1">Finkel RS, Mercuri E, Meyer OH, Simonds AK, Schroth MK, Graham RJ, Kirschner J, Iannaccone ST, Crawford TO, Woods S, Muntoni F. [https://www.sciencedirect.com/science/article/pii/S0960896617312907 Diagnosis and management of spinal muscular atrophy: Part 2: Pulmonary and acute care; medications, supplements and immunizations; other organ systems; and ethics.] Neuromuscular Disorders. 2018 Mar 1;28(3):197-207.</ref>.
Many children and adults with Spinal muscular atrophy will be dependent on pulmonary management due to a loss of muscle function. A respiratory therapist should be included in the multidisciplinary treatment team from an early stage to ensure proper respiratory management.<ref name=":1">Finkel RS, Mercuri E, Meyer OH, Simonds AK, Schroth MK, Graham RJ, Kirschner J, Iannaccone ST, Crawford TO, Woods S, Muntoni F. [https://www.sciencedirect.com/science/article/pii/S0960896617312907 Diagnosis and management of spinal muscular atrophy: Part 2: Pulmonary and acute care; medications, supplements and immunizations; other organ systems; and ethics.] Neuromuscular Disorders. 2018 Mar 1;28(3):197-207.</ref>
 
'''Airway clearance''' (chest physio) is best administered with the combination of Cough Assist and this should be the primary airway clearance therapy for all SMA patients with respiratory illness.
 
'''[[Suctioning]]''' is a critical part of the treatment and should be used in all patients with excessive secretions or in those with ineffective cough.
 
'''The high-frequency chest wall oscillation (Vest)''' is another option for managing secretions. However, there is no evidence that the Vest improves airway clearance and secretions.
 
[[Non Invasive Ventilation|'''Non-invasive positive pressure ventilation (NIV)''']] should be used for respiratory failure or to prevent chest wall distortion.


'''Continuous positive airway pressure (CPAP)''' should be used only when NIV is not tolerated or in the treatment of chronic respiratory failure<ref name=":1" />.<br>  
* '''Chest physiotherapy''' - assists with respiratory management and should be one of the primary airway clearance therapies.<ref name=":1" />
* '''Mechanical insufflation–exsufflation''' - devices such as Cough Assist or Vit  alCough can be used and this should be one of the primary airway clearance therapies.<ref name=":1" />
* '''[[Suctioning]]''' is a critical part of the treatment and should be used in all patients with excessive secretions or in those with an ineffective cough.
* '''The high-frequency chest wall oscillation (Vest)''' is another option for managing secretions. However, there is no evidence that the Vest improves airway clearance or secretions.<ref name=":1" />
* [[Non Invasive Ventilation|'''Non-invasive positive pressure ventilation (NIV)''']] should be used for respiratory failure or to prevent chest wall distortion.<ref name=":1" />
* '''Continuous positive airway pressure (CPAP)''' should be used only when NIV is not tolerated or in the treatment of chronic respiratory failure.<ref name=":1" /><br>  


== References  ==
== References  ==

Latest revision as of 06:55, 6 February 2024

Original Editor - Evelin Milev Top Contributors - Evelin Milev, Jeremy Bryan, Nikhil Benhur Abburi, Lucinda hampton, Kim Jackson, Rucha Gadgil, Momina Khalid, Aminat Abolade, Rachael Lowe and Meaghan Rieke

Introduction[edit | edit source]

Spinal Muscular Atrophy (SMA) is a genetic disorder also considered to be a neurodegenerative disorder, specifically a motor neurone disease. SMA is characterised by the degeneration of alpha motor neurons in the spinal cord, affecting the control of voluntary muscle movement.[1] It occurs in roughly one in 6,000–10,000 births.[2] There are several classifications of SMA, which are assigned based on the age at which symptoms first occur along with the highest level of muscle activation attained or expected to be attained. [1][3]

[4]

Pathological Process[edit | edit source]

SMA is considered to be an autosomal recessive condition resulting from the homozygous deletion of the gene SMN1 (survival of motor neuron 1).[2] In some cases, it is possible for the neighboring SMN2 gene to compensate for a lack of the SMN1 gene. Therefore, if there is one or more additional copies of the SMN2 gene, later-onset and less severe SMA symptoms can occur.[3]

Autosomal Recessive

Clinical Presentation and Classification[edit | edit source]

SMA is classified based on the age at which symptoms first occur as well as the level of muscle activation attained or expected to be attained. [1][3]SMA symptoms range in severity but often include hypotonia, muscle weakness (proximal muscles greater than distal muscles and lower extremity than upper extremity), bone or joint issues, difficulty swallowing, and/or difficulty breathing.[3][5]

[6]

Types of SMA[edit | edit source]

TYPE 1 (MOST SEVERE)(Werdnig-Hoffmann disease of acute infantile SMA) TYPE 2 TYPE 3 (Kugelberg-Welander syndrome or juvenile SMA) TYPE 4
AGE OF ONSET First 6 months 6-18 months 18 months or older Adulthood (after 21 years)
SYMPTOMS
  • Reduce muscle tone
  • Contractures
  • Reflexes absent
  • Swallowing,feeding difficulty
  • Can sit
  • Unable to stand/walk without support
  • Respiratory difficulties
  • Walk independently
  • Difficulty in running, stair climbing
  • Scoliosis
 Mild to moderate leg weakness.
LIFE EXPENTANCY Die before 2 years [3] Adolescence or young adulthood [3] Normal lifespan (with regular physical rehabilitations) [3] Normal lifespan(with little physical training) [3]

Diagnostic Procedures[edit | edit source]

Diagnosis generally starts with genetic testing to determine whether or not the SMN1 gene is absent. Genetic testing has been found to have a 95% sensitivity (test shows the absence of SMN1 the gene when it is truly absent) and an almost 100% specificity (test shows the presence of SMN the gene when it is truly present). If genetic testing does return a result consistent with clinical signs and symptoms, additional testing in the form of electrocardiography, a muscle biopsy, a nerve conduction velocity study, or blood tests can be performed.[3][7]

Differential Diagnosis[edit | edit source]

DD of spinal Muscular Atrophy[8]

Outcome Measures[edit | edit source]

There are several outcome measures which can be used to detect changes in the course of treatment for patients with SMA. These tools should be appropriately selected according to the age and severity of the disease.

  • Six-Minute Walking Test (6MWT) - The Six-Minute-Walking-Test can be safely performed in ambulant patients with SMA. It has been proven to detect fatigue-related changes in this population of patients and also correlates with other established outcome measures for patients with spinal muscular atrophy[9].
  • Revised Hammersmith Scale for SMA (RHS) - The RHS is predominantly used in patients with SMA types 2 and 3. In combination with the World Health Organisation (WHO) motor milestones, the scale can be more sensitive toward the description of the SMA phenotype. The RHS has been designed to capture a wide range of abilities across a broad spectrum of SMA, from very young children to adolescents and adults[2].
  • WHO Developmental Milestones - The WHO scales aim to link the growth of the child and motor development in one single reference. The final version of the protocol includes six items: "Sitting without support," "hands-and-knees crawling," "standing with assistance," "walking with assistance," "standing alone," and "walking alone.". The WHO provides important information about a child's gross motor development in different cultural settings[10].
  • Revised Upper Limb Module (RULM) for SMA - The RULM is a specifically designed outcome measure for upper limb function in patients with Spinal muscular atrophy. The scale has shown good reliability and validity, which makes it a good choice for assessing arm function in children and adults with SMA[11].

Management / Interventions[edit | edit source]

The management of SMA warrants a multi-disciplinary approach coordinated by the patient's primary clinician.[12]

Orthopedic Management[edit | edit source]

  • Spinal deformities
    • Scoliosis
      • Bracing
        • Limit scoliosis progression during growth years, not corrective
      • Surgical intervention (hardware implantation)
        • The goal is to ultimately promote better breathing mechanics and sitting alignment [12]
  • Contractures
    • Management through Physical Therapy
    • Surgical intervention if significant impairment or pain is present
  • Fractures
    • Cast immobilization if non-ambulatory
    • Surgical fixation, if ambulatory

Nutrition Management[edit | edit source]

  • Maintenance of adequate nutritional intake
    • Adequate calcium and vitamin D
  • Maintenance of appropriate body mass index
  • Screening and monitoring for complications such as...
    • Glucose abnormalities
    • Hyperlipidemia
    • Abnormal fatty acid metabolism
    • Metabolic acidosis [12]

Speech and Language Pathology[edit | edit source]

  • Screening and intervention for dysphagia

Medical Management[13]:

  • Neuroprotective drugs like riluzole
  • Drugs to improve energy metabolism
  • Drugs affecting the gene expression of SMN. [12]

Gene Therapy:[edit | edit source]

  • Along with advances in medical management, gene therapy approaches have been evaluated for SMA, using viral vectors to replace the SMN1 gene.[14]

Physiotherapy[edit | edit source]

  • Merconi et al.[12] provide a comprehensive outline of physiotherapy management for SMA broken down by functional level.
Table derived from Merconi et al.[12]
Functional Level Goals Possible Deficits Possible Interventions/Adaptations
Patients not able to sit unsupported
  • Facilitate optimal function
  • Deficiencies in postural control
  • Decreased sitting tolerance
  • Contractures
  • Muscular weakness
  • Thoracic and cervical bracing to promote appropriate positioning and posture
  • Orthoses, splints, serial casting, AAROM, PROM, stretching, and or standing frame use to facilitate contracture prevention and management
  • Adaptive equipment
    • Sitting brace or sitting system
    • Postural support equipment
    • Positioning equipment
    • Hoist or lift system
    • Recline/tilt wheelchair
  • Eye tracking equipment for communication and computer use
Patients able to sit unsupported
  • Contracture management/prevention
  • Scoliosis management/prevention
  • Facilitate independence with function and mobility
  • Deficiencies in postural control
  • Contractures
  • Muscle weakness
  • Thoracic and cervical bracing to promote appropriate posture
  • Orthoses, splints, serial casting, AAROM, PROM, stretching, and or standing frame use to facilitate contracture prevention and management
  • Adaptive equipment
    • If needed, any equipment suggested for patients not able to sit unsupported
    • Gait training devices
    • UE support devices
    • Power or lightweight wheelchair with appropriate postural support
Patients able to ambulate
  • Facilitate highest level of function
  • Improve or maintain joint ROM/contracture management and or prevention
  • Improve of maintain endurance
  • Improve or maintain balance
  • Deficiencies in postural control
  • Contractures
  • Muscle weakness
  • Decreased endurance
  • Decreased balance
  • Thoracic and cervical bracing to promote appropriate posture (while in sitting)
  • Orthoses, splints, serial casting, AAROM, PROM, stretching, and or standing frame use to facilitate contracture prevention and management
  • Adaptive equipment
    • If needed, any equipment suggested for patients not able to sit unsupported
    • Power wheelchair, lightweight wheelchair, or scooter for longer distances
  • Gait training for improvement of endurance, efficiency, and safety
  • Balance training

Respiratory Care[edit | edit source]

Many children and adults with Spinal muscular atrophy will be dependent on pulmonary management due to a loss of muscle function. A respiratory therapist should be included in the multidisciplinary treatment team from an early stage to ensure proper respiratory management.[15]

  • Chest physiotherapy - assists with respiratory management and should be one of the primary airway clearance therapies.[15]
  • Mechanical insufflation–exsufflation - devices such as Cough Assist or Vit alCough can be used and this should be one of the primary airway clearance therapies.[15]
  • Suctioning is a critical part of the treatment and should be used in all patients with excessive secretions or in those with an ineffective cough.
  • The high-frequency chest wall oscillation (Vest) is another option for managing secretions. However, there is no evidence that the Vest improves airway clearance or secretions.[15]
  • Non-invasive positive pressure ventilation (NIV) should be used for respiratory failure or to prevent chest wall distortion.[15]
  • Continuous positive airway pressure (CPAP) should be used only when NIV is not tolerated or in the treatment of chronic respiratory failure.[15]

References[edit | edit source]

  1. 1.0 1.1 1.2 Darras BT, Markowitz JA, Monani UR, De Vivo DC. Spinal muscular atrophies (2015) Neuromuscular Disorders of Infancy. Childhood, and Adolescence: A Clinician’s Approach.:117-45.
  2. 2.0 2.1 2.2 Ramsey D, Scoto M, Mayhew A, Main M, Mazzone ES, Montes J, de Sanctis R, Dunaway Young S, Salazar R, Glanzman AM, Pasternak A. Revised Hammersmith Scale for spinal muscular atrophy: A SMA specific clinical outcome assessment tool. PloS one. 2017 Feb 21;12(2):e0172346.
  3. 3.0 3.1 3.2 3.3 3.4 3.5 3.6 3.7 3.8 Umphrend D, Lazaro R, Roller M, Burton G. Umphrend's Neurological Rehabilitation. Sixth Edition. St. Louis, MO, USA. Elsevier Mosby, 2013.
  4. Genentech. Understanding Spinal Muscular Atrophy (SMA). Available from: https://www.youtube.com/watch?v=5mI_ZsWkkc4 (last accessed 7.6.2019)
  5. National Health Service. Spinal muscular atrophy. Available from https://www.nhs.uk/conditions/spinal-muscular-atrophy-sma/ Last accessed 4/24/2023.
  6. Cure SMA. Learn to Spot the Warning Signs of SMA – Snapshot of Hallmark Symptoms (Video 9) Available from: https://www.youtube.com/watch?v=G5yIdH0yans&feature=emb_logo [last accessed 31/01/2021]
  7. National Institute of Neurological Disorders and Stroke. Spinal Muscle Atrophy. Available from https://www.ninds.nih.gov/health-information/disorders/spinal-muscular-atrophy (accessed 4/26/2023).
  8. Prior TW, Leach ME, Finanger E. Table 5. [Disorders to Consider in the Differential Diagnosis of Spinal Muscular Atrophy (SMA)]. [Internet]. Nih.gov. University of Washington, Seattle; 2020 [cited 2024 Feb 6]. Available from: https://www.ncbi.nlm.nih.gov/books/NBK1352/table/sma.T.disorders_to_consider_in_the_diffe/ ‌
  9. Montes J, McDermott MP, Martens WB, Dunaway S, Glanzman AM, Riley S, Quigley J, Montgomery MJ, Sproule D, Tawil R, Chung WK. Six-Minute Walk Test demonstrates motor fatigue in spinal muscular atrophy. Neurology. 2010 Mar 9;74(10):833-8.
  10. Wijnhoven TM, de Onis M, Onyango AW, Wang T, Bjoerneboe GE, Bhandari N, Lartey A, Rashidi BA. Assessment of gross motor development in the WHO Multicentre Growth Reference Study. Food and nutrition bulletin. 2004;25(1_suppl_1):S37-45.
  11. Mazzone ES, Mayhew A, Montes J, Ramsey D, Fanelli L, Young SD, Salazar R, De Sanctis R, Pasternak A, Glanzman A, Coratti G. Revised upper limb module for spinal muscular atrophy: development of a new module. Muscle & nerve. 2017 Jun;55(6):869-74.
  12. 12.0 12.1 12.2 12.3 12.4 12.5 Mercuri E, Finkel RS, Muntoni F, Wirth B, Montes J, Main M, Mazzone ES, Vitale M, Snyder B, Quijano-Roy S, Bertini E. Diagnosis and management of spinal muscular atrophy: Part 1: Recommendations for diagnosis, rehabilitation, orthopedic and nutritional care. Neuromuscular Disorders. 2018 Feb 1;28(2):103-15.
  13. Tiziano FD, Lomastro R, Pinto AM, Messina S, D'Amico A, Fiori S, Angelozzi C, Pane M, Mercuri E, Bertini E, Neri G. Salbutamol increases survival motor neuron (SMN) transcript levels in leucocytes of spinal muscular atrophy (SMA) patients: relevance for clinical trial design. Journal of medical genetics. 2010 Dec 1;47(12):856-8.
  14. Passini MA, Cheng SH. Prospects for the gene therapy of spinal muscular atrophy. Trends in molecular medicine. 2011 May 1;17(5):259-65.
  15. 15.0 15.1 15.2 15.3 15.4 15.5 Finkel RS, Mercuri E, Meyer OH, Simonds AK, Schroth MK, Graham RJ, Kirschner J, Iannaccone ST, Crawford TO, Woods S, Muntoni F. Diagnosis and management of spinal muscular atrophy: Part 2: Pulmonary and acute care; medications, supplements and immunizations; other organ systems; and ethics. Neuromuscular Disorders. 2018 Mar 1;28(3):197-207.
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