Duchenne Muscular Dystrophy:Neuromuscular Management
Introduction
• Muscles weaken due to lack of dystrophin• Regular checkups with specialists are required• Steroids are the only drugs which alter the
natural history of DMD– Should only be prescribed by doctors with
appropriate expertise– Proactive side-effect management is crucial– No current evidence that other supplements work
Regular Checkups
• Neuromuscular specialist every 6 months– Monitor disease progression– Make decisions about new treatments at
appropriate times– Anticipate and prevent any problems including
side effect prevention and management
• Specialist physiotherapist and/or occupational therapist every 4 months
What to measure?• Specific tests vary between clinics– Consistency, experience and regular review important
• Areas of assessment include– Strength (force generated at joints)– Range of joint motion (monitor contractures)– Timed tests (e.g. 6MWT, rise from floor, steps)– Motor function scales (e.g. North Star) – different scales
may be needed at different times– Activities of daily living (assess whether additional help
required to assist independence)• Further information in TREAT-NMD Registry of
Outcome Measures www.treat-nmd.eu/rom
Assessments: Strength Testing• Method
– Manual muscle testing (MRC scale)– Quantitative myometry (if MRC scale 3-5)
• Aims– Serial assessment to identify outliers from expected clinical course– Monitor disease progression, predict functional losses– Assess response to treatment– Monitor muscle imbalance
• Ambulatory– Test lower extremity strength by manual muscle testing every 6
months• Non-Ambulatory
– Early stages: test upper and lower extremity strength every 6 months– Later stages: value of testing is less certain
Assessments: Range of motion• Method
– Goniometry• Aims
– Baseline: identify emerging muscle hypoextensibility and joint contractures that might contribute/lead to functional deterioration or musculoskeletal or integumentary problems
– To identify need for additional/altered therapeutic/surgical intervetion (i.e. orthoses, splinting, use of standers, iliotibial band lengthening)
• Ambulatory– Lower extremities: hip, knee, ankle joints, iliotibial band, hamstrings,
gastrocnemius• Non-Ambulatory
– Lower extremities: hip, knee, ankle joints, iliotibial band, hamstrings, gastrocnemius
– Upper extremities: elbow, wrist, long finger flexors
Assessments: Timed Testing• Method
– Standardised use of timed function tests• Aims
– Easy and relevant measure of daily functional status and responsiveness to change
• Ambulatory– Timed 10m walk– Timed Gowers’ manouvre– Time to climb 4 stairs– Time to rise from chair– Time to put on a shirt may be relevant in late ambulatory stage
• Non-Ambulatory– Time to put on a shirt may be relevant in early non-ambulatory stage– Timed testing not applicable in late non-ambulatory stage
Assessments: Motor function scales
• Method– Assessment of motor function in specific domains to give a composite
score• Aims
– Allows monitoring of progression and response to therapy• Ambulatory
– Vignos lower extremity scale– North Star Ambulatory Assessment– Motor function measure
• Non-Ambulatory– Brooke upper extremity scale– Egen Klassifikation functional assessment– Hammersmith motor scales– Motor function measure
Assessments: Activities of daily living
• Method– Assessment of impairment in daily activities in the home, school and
community settings• Aims
– Highly relevant to targeted input with aids, adaptation, and access to environmental controls
• Ambulatory– Frequency of falls, step activity monitoring– Self-care skills– Writing, computer use– Functioning in school and community settings
• Non-Ambulatory– Self-care skills– Writing, computer use– Control of manual and electric wheelchair– Functioning in school and community settings
Drug Treatments
• Steroids are only evidence-based drug treatment for musculoskeletal DMD symptoms
• Effective and safe use is based on regular assessment of function and side-effects
• As new evidence is available, these guidelines will be revised
Steroid Treatment: Introduction
• Significant experience in steroid use for many conditions
• Benefits should be balanced with proactive management of possible side-effects
• Use of steroids very important: should be discussed with all families early
Steroids: The Basics
• Steroids are the only drugs known to slow decline in muscle strength and motor function in DMD
• Goals– Help child walk independently for longer– Minimise later breathing, heart and orthopaedic
problems– Can also reduce risk of scoliosis
• Prevention/management of side-effects should be proactive and anticipatory.
• Early intervention to prevent problems.
Steroids: Starting treatment
• Optimal time for starting treatment is when motor skills have reached a plateau (4-6yrs)
• Not recommended to start steroids in children who are still gaining motor skills (esp <2 yrs)
• Recommended national vaccination schedule should be completed prior to beginning steroid treatment
• Varicella (chicken pox) immunity should be established
Steroids: Starting treatment (2)• Decision to initiate treatment should be based on
a serial assessment and parental report: care is required if initiating steroid treatment at an initial visit, or as a second-opinion consultation
• Starting treatment in non-ambulant boys is an individual decision, which should take into consideration individual risk factors
• Many experts recommend continuation of steroid treatment after the loss of ambulation, to preserve upper limb strength, slow scoliosis, and delay decline in respiratory and cardiac function
Steroid Regimes 1
• Two steroids recommended for DMD– Prednisone (also known as prednisolone)– Deflazacort
• Believed to work similarly: neither known to be better• Planned trials will provide more knowledge• Choice of steroid depends on– Availability– Cost to family– The way the drug is taken– Perceived side effects
Steroids: Prednisone
• Inexpensive, both tablet/liquid fomulations• Recommended starting dose: 0.75mg/kg/day• In ambulatory individuals dosage commonly
increased as child grows, to ~40kg in weight• Max dose capped at ~30mg/kg/day• Non-ambulatory teenagers above 40kg: – Dosage often allowed to drift down to 0.3-0.6mg/kg/day
range: below cap, but still shows substantial benefits
Steroids: Deflazacort• May have slightly lower risk of weight gain• More expensive than prednisone, available in
fewer tablet sizes, and liquid formulation not widely available.
• Recommended starting dose: 0.9mg/kg/day• In ambulatory individuals dosage commonly
increased as child grows, to ~40kg in weight• Max dose capped at ~36mg/kg/day• Non-ambulatory teenagers above 40kg:
– Dosage often allowed to drift down to 0.5-0.7mg/kg/day range: below cap, but still shows substantial benefits
Steroid Regimes 2• Daily dose of steroids better understood than alternate
regimes (trial data may modify this)• Maintenance steroid dose
– Balance between growth, individual response, and burden of side-effects
– Should be reviewed at every clinic visit, based on test results and tolerability/manageability of side effects
• For boys on relatively low dosage (less than starting dose per kg of body weight) who begin to show functional decline, it may be necessary to consider a “functional rescue” adjustment. – The dosage is increased to target, and the individual re-
evaluated for any benefit in 2-3 months.
Initiation of steroids in non-ambulatory individuals
• No consensus on optimal steroid dosage if initiated in a non-ambulatory individual
• Not known how effective this treatment is in preventing scoliosis or stabilising cardiac/respiratory function
• This area warrants further study
Steroid management and side effects
• Some patients may experience short-lived side-effects (hyperactivity, mood swings) for a few hours after medication is given. Administration in the afternoon may alleviate these difficulties
• Before starting/stopping medication, the doctor should be consulted
• Doctors should always be informed that a patient is on steroids – especially if considering surgery, or during infection/injury, as steroids can suppress the immune system.
• Patients should never stop taking steroids suddenly
Management of steroid medication
• Dose reduction suggested if intolerable/non-manageable side-effects occur, with reassessment by phone/clinical visit one month later to assess control of side effects
• If daily dosing schedule leads to unmanageable and/or intolerable side effects that do not improve when the dose is reduced, it is appropriate to change to an alternative regime
Management of steroid medication (2)
• Steroid therapy should not be abandoned until at least one dosage reduction and change to an alternative regime have been pursued, for both ambulatory and non-ambulatory patients
• Should adjustments prove ineffective in making any significant side-effects sufficiently manageable/tolerable, it is necessary to discontinue steroid therapy. – Decision should be made in partnership with the
patient and family– Steroids should never be stopped suddenly
Other drugs and supplements• Oxandrolone, an anabolic steroid, is not recommended • Safety in the use of botulinum toxin A (Botox) has not been studied in
treatment/prevention of contractures for DMD and is not recommended
• No support for systemic use of creatine; if a patient is taking creatine and has evidence of kidney problems it is necessary to discontinue this supplement
• Due to a paucity of evidence in published literature, no recommendations can be made about other drugs/supplements, including: – Co-enzyme Q10– Carnitine– Amino acids (glutamine, arginine)– Anti-inflammatories/antioxidants (fish oil, vitamin E, green tea extract,
pentoxifylline)– Herbal/botanical extracts
• Additional research is needed in this area
Steroid side effects: recommended monitoring and intervention
• Different people will have very different responses to steroids. Some of the more common side-effects are listed below.
• Key to successful management is an awareness of potential side-effects, preventing/reducing them where possible.
Side effects: general & cosmetic Steroid side effect Recommended monitoring Intervention
Weight gain, obesity and Cushingoid features
Particular vigilance needed if patient, parents, or siblings are obese
Dietary advice to be reinforced before starting steroids; warn about increased appetite
Implement proactive dietary management for the entire family, not just the patient
Consider change from prednisone to deflazacort
Select an alternative regimen
Hirsutism Forewarn parents Does not usually occur to an extent that warrants a change in medication
Acne, tinea, warts More noticeable in teenagers Use ancillary treatment measures (topical prescription) and do not rush to change the GC regimen unless the boy is emotionally distressed
Side effects: general & cosmetic (2), behavioural
Steroid side effect Recommended monitoring Intervention
Growth retardation Monitor height at least every 6 months as part of general care (stature often small in DMD even without steroids)
Consider endocrine evaluation if growth plateaus
Delayed puberty Monitor Tanner stage
Identify any family history of delayed sexual maturation
Consider endocrine assessment if notably delayed or patient is upset by the delay
Adverse behavioural changes
Identify any baseline mood, temperament, ADHD issues, and advise parents that these often transiently worsen in the initial 6 weeks on GC therapy
Decide whether baseline issues should be treated before starting GC therapy (e.g. ADHD counselling or prescription)
Consider changing timing of GC medication to later in the day
Consider behavioural health referral
Side effects: immune/adrenal suppression
Steroid side effect Recommended monitoring Intervention
Immune/adrenal suppression
Advise parents of risk of serious infection and need to promptly address minor infection
Advise parents to inform all medical personnel that their child is on steroids and carry steroid alert card
Ensure that the GC is not stopped abruptly
Obtain varicella immunisation before starting GC therapy; confirm with protective serum titre
Engage in tuberculosis surveillance
Obtain infectious diseases consultation if serious infection occurs
Substitute prednisone equivalent if deflazacort is temporarily unavailable
Implement intravenous stress-dose hydrocortisone or methylprednisolone coverage for surgery or major illness (no accepted treatment strategy; anaesthesia or endocrine consultation recommended)
Give intravenous coverage if nothing by mouth
Side effects: hypertension, glucose intolerance, gastric complications (1)
Steroid side effect Recommended monitoring Intervention
Hypertension Monitor blood pressure as percentile for height and sex at each clinic visit
If blood pressure >99%, reduce salt intake, weight reduction
If ineffective, refer for possible ACE inhibitor or β blocker medication
Glucose intolerance Urine dipstick for glucose at clinic visits
Enquire about polyuria, polydipsia
If urine is glucose-positive, then try fasting or post-prandial blood glucose, and if abnormal, then seek an endocrine consultation
Gastritis / Gastroesophagal Reflux Disease (GERD)
Enquire about GERD symptoms (heartburn)
Advise parents to report symptoms
Avoid NSAIDs
Prescribe ranitidine or proton-pump inhibitor and antacid if symptomatic
Side effects: gastric complications (2), cataracts
Steroid side effect Recommended monitoring Intervention
Peptic ulcer disease Advise parents of risk and to report symptoms
History of gastritis, GERD, abdominal pain, or faecal blood
Test stool for blood if anaemic or suggestive history
Avoid NSAIDs
Prescribe ranitidine or proton-pump inhibitor and antacid if symptomatic
Seek gastrointestinal consultation
Cataracts Annual ophthalmological examination
Consider switching from deflazacort to prednisone if cataracts evolve that affect vision
Seek ophthalmology consultation
Side effects: bone demineralisationSteroid side effect Recommended monitoring Intervention
Bone demineralisation and increased fracture risk
Take careful fracture history
Annual DEXA to monitor bone density
Annual monitoring of 25-hydroxy vitamin D blood
concentration (ideally late winter in seasonal climates) and supplement with vitamin D3 if level is <32 nmol/L
Dietitian should assess calcium and vitamin D intake
For 25-hydroxy vitamin D concentration 20–31 nmol/L, give 1000 IU orally twice daily, for <20 nmol/L, give 2000 IU orally twice daily
Recheck serum 25-hydroxy vitamin D concentration again after 3 months on therapy
Encourage weight-bearing activities
Take multivitamin supplements with vitamin D3
Consider bisphosphonates, such as pamidronate
Side effects: myoglobinuriaSteroid side effect Recommended monitoring Intervention
Myoglobinuria Enquire about abnormal coloration of urine after exercise, urine testing
Advise avoidance of excessive eccentric (eg, descending stairs, squatting down, trampolining) and
resistive exercise
Commence renal investigations if persistent
Schema for initiation of GC medication
Prednisone Deflazacort
0.75mg/kg/day
First line unless pre-existing weight and/or behavioural issues favour deflazacort
0.9mg/kg/day
Consider as first line when pre-existing weight and/or behavioural issues
Age <2 years Age 2-5 years Age ≥ 6 years
Improving (typical): GC initiation not recommended
Plateau (uncommon): monitor closely
Decline (atypical): consider alternative diagnoses/concomitant pathology
Improving: GC initiation not recommended
Plateau: GC initiation recommended
Decline: GC initiation highly recommended
Improving (uncommon): consider BMD
Plateau: GC initiation highly recommended
Decline: GC initiation highly recommended
Non-ambulatory: refer to text
Schema for management of GC medication
If any side effects are manageable and tolerable
Incremental increase in dose for growth to maximum weight of 40kg (prednisone 30mg/day or deflazacort 36mg/day)
If in functional decline and on subtarget dose, increase to target dose
Continue even when non-ambulatory for retarding of scoliosis, decline in pulmonary function tests, and possible heart failure.
If side-effects unmanageable/intolerable : change in GC regimen necessary
Reduce daily dosage by 25-33% and reassess in 1 month
If side-effects are still unmanageable and intolerable
Consider lowering additional 25% on daily schedule; minimum effective daily dose of prednisone is approximately 0.3mg/kg/day
If weight gain/behaviour are main issues, consider change to deflazacort or high-dose weekend
If patient/parents about to abandon treatment entirely, consider 10/10 or 10/20 intermittent dose
Alternative GC dosing strategiesPrednisone dose
Deflazacort dose
Comments In case of side-effects
Alternate day
0.75-1.25mg/kg every other day
2mg/kg every other day
Less effective but consider when daily schedule has side-effects that are not effectively managed or tolerated
Must reduce dose if side-effects are not manageable or tolerable
High-dose weekend
5mg/kg given each Friday and Saturday
Not yet tested Less data on effectiveness as compared to a daily schedule, especially if weight gain/behavioural issues are problematic
Must reduce dose if side-effects are not manageable or tolerable
Intermittent 0.75mg/kg for 10 days alternating with 10-20 days off medication
0.6mg/kg on days 1-20 and none for the remainder of the month
Less effective, but has fewer side effects. Considered the least effective, but possibly best tolerated regimen before abandoning steroid treatment altogether
Must reduce dose if side-effects are not manageable or tolerable
References & Resources
• The Diagnosis and Management of Duchenne Muscular Dystrophy, Bushby K et al, Lancet Neurology 2010 9 (1) 77-93 & Lancet Neurology 2010 9 (2) 177-189– Particularly references, p186-188
• The Diagnosis and Management of Duchenne Muscular Dystrophy: A Guide for Families
• TREAT-NMD website: www.treat-nmd.eu • CARE-NMD website: www.care-nmd.eu