Formulary Drug Listing Decisions SKELETAL MUSCLE RELAXANTS Indications Recommendation Highlights
The management of discomfort ± acute muscle
n Skeletal muscle relaxants (SMRs) are a
spasm associated with painful musculoskeletal
(MSK) conditions (cylcobenzaprine, methocar-
treat muscle spasm, pain associated with
acute MSK conditions and spasticity associ-
The treatment of spasticity associated with
ated with spinal cord injuries and neuron
spinal cord injuries and neuron disorders
n Cyclobenzaprine, orphenadrine, and tizani-
dine have demonstrated significant short-
DAC Recommendation
term symptomatic relief and overall improve-ment of acute low back pain compared to
The DAC recommended that: (i) orphenadrine
placebo. Long-term data are unavailable.
and cyclobenzaprine be listed in the 25WS
Concerns exist in the medical literature
formulary ONLY; (ii) baclofen be listed in the
regarding their potential for central nervous
03WS formulary ONLY; and (iii) dantrolene,
system (CNS) adverse events and drug inter-
Drug Profile
methocarbamol, and tizanidine NOT BE LISTED
Products available in
n Tizanidine does not provide any therapeu-
tic benefit compared to cyclobenzaprine or
The WSIB Decision
orphenadrine in the treatment of acute back
pain; however, tizanidine is associated with
Based on the DAC’s recommendations, the
liver and cardiac side effects, an increased
WSIB has decided to: (i) LIST cyclobenzaprine
risk of abuse and a significantly higher cost.
and orphenadrine in the initial musculoskel-
etal (25WS) formulary; (ii) LIST baclofen in the
n Baclofen has fair to strong evidence of
CNS-Brain injury (03WS) formulary; and (iii)
efficacy in muscle spasm and spasticity as-
NOT LIST dantrolene, methocarbamol, or tizani-
sociated with upper motor neuron syndrome
(based mainly on trials in multiple sclerosis).
Rigorous evidence in other musculoskeletal
Formulary Status
n There is limited evidence for the use of meth-
Cyclobenzaprine and orphenadrine are listed
ocarbamol or dantrolene in the treatment
in the 25WS formulary ONLY. Baclofen is listed
of acute back pain or spasticity. Both drugs
in the 03WS formulary ONLY. New requests
are associated with CNS side effects and
for these drugs outside these formularies WILL NOT be approved. Dantrolene, methocarbamol, and tizanidine ARE NOT listed in any WSIB
n Overall, systematic reviews indicate that
most SMR trials have several methodologi-cal shortcomings including poor quality, poorly designed and described methods, short duration and heterogeneity of outcome measures.
n Relatively few comparative trials involving
SMRs are available, making it difficult to assess whether important differences exist between agents.
evaluated the cost-effectiveness of SMRs; those available have major methodological limitations.
n The DAC concluded that an independent review of the clinical efficacy, safety, and cost-effectiveness of SMRs in the treatment of acute muscle spasms and painful muscu- loskeletal conditions demonstrated variable evidence by drug class. Consequently, the DAC recommended that (i) cyclobenzaprine and orphenadrine be listed in the 25WS formulary as they present the best quality evidence; (ii) baclofen be listed in the 03WS formulary for the treatment of spasticity due to CNS-related injury/illness; and (iii) dan- trolene, methocarbamol, and tizanidine not be listed in any formularies as these agents do not provide any therapeutic advantage and pose additional risks. DETAILED DISCUSSION Background
(RCTs). Eight systematic reviews evaluating
The term skeletal muscle relaxants (SMRs)
acute low back pain (2), nonprogressive neu-
refers to a heterogeneous group of drugs used
rologic disease (2), spasticity and MSK condi-
to treat muscle spasm and pain associated with
tions (1), sciatica (1), mechanical neck disorders
acute musculoskeletal (MSK) conditions and
(1), and fibromyalgia (1) were included in the
spasticity associated with spinal cord injuries
report. The SMRs investigated were baclofen,
and neuron disorders (e.g., cerebral palsy,
cyclobenzaprine, dantrolene, methocarbamol,
multiple sclerosis, paraplegia, etc.). Although
SMRs are indicated for the short-term treatment
Baclofen is indicated in the treatment of spas-
of these symptoms/disorders, they are often
ticity from multiple sclerosis and spinal cord
prescribed for long-term use. Concerns have
injury/disease. There is fair to strong evidence
arisen in the medical literature surrounding the
that baclofen is effective in alleviating muscle
lack of evidence for their long-term use and
spasm (non-specific back pain) and spastic-
their potential for serious adverse events and
ity (mainly in multiple sclerosis). Although
balcofen has only been compared to placebo in lower back pain, head-to-head studies evaluat-
Summary of Committee
ing its use in relief of spasticity suggest that it
Considerations
is equivalent to tizanidine. Long-term efficacy and safety data are lacking. Baclofen’s efficacy
The DAC considered an external, independent
in other MSK conditions (e.g., non-progressive
review of the clinical efficacy, safety, and cost-
neurological diseases, spasticity following
effectiveness of SMRs in the treatment of acute
or chronic MSK conditions or traumatic nervous
disorders) remains unproven in rigorous trials
system diseases. The report included system-
of adequate duration. Baclofen is associated
atic reviews of randomized controlled trials
with an elevated risk of abuse, central nervous
system (CNS) adverse events, and exacerbation
evidence for the use of methocarbamol in
of psychiatric illnesses. Withdrawal reactions
muscle spasm or spasticity. Two placebo-con-
trolled trials produced inconsistent results and were rated as being of poor quality. Methocar-
Cyclobenzaprine is indicated for the short-
bamol’s efficacy in other MSK conditions has
term treatment of muscle spasm associated
not been investigated in rigorous RCTs. Drows-
with acute MSK conditions. Two systematic
iness, dizziness, and lightheadedness are the
reviews concluded that there is strong evidence
most frequently reported side effects. Blurred
for significant symptomatic relief and overall
vision, headache, fever, and nausea may also
improvement with short-term cyclobenzaprine
use in acute low back pain (ALBP). There is fair to good quality evidence that it is effective in
Orphenadrine is indicated in acute skeletal
treating acute neck pain compared to placebo.
muscle spasm. A systematic review concluded
Although fair quality evidence demonstrates
that orphenadrine is effective in the treatment
improved global functioning and sleep in fibro-
of ALBP. Fair evidence demonstrates that
myalgia patients, no improvement in fatigue or
orphenadrine is effective in general acute
tender points has been observed. Furthermore,
MSK conditions (e.g., neck pain). Its long-term
these studies are limited by their high drop-out
efficacy and safety have not been established.
rates and short duration. Cyclobenzaprine has
Orphenadrine’s efficacy in other MSK condi-
not been evaluated in the treatment of spastic-
tions has not been investigated in any rigorous
ity or spinal cord injuries/diseases. Multiple
adverse events have been reported, including
effects include dry mouth, urinary hesitancy or
cardiac arrhythmias, urinary retention, dry
retention, blurred vision, mydriasis, drowsiness,
mouth, sedation, and impairment of physical
headache, tachycardia, palpitations, and GI dis-
and mental abilities. Additive sedation can
turbances. Orphenadrine can impair an individ-
occur when taken with other sedating drugs.
ual’s ability to engage in potentially hazardous activities, such as operating machinery or
Dantrolene is indicated for controlling
symptoms of chronic spasticity from neurologi-cal conditions. Although there is moderate
Tizanidine is indicated for the management of
to good evidence that dantrolene reduces
spasticity. Similarly to cyclobenzaprine and
muscle spasm in ALBP compared to placebo,
orphenadrine, systematic reviews have dem-
the generalizability of these results is limited
onstrated strong evidence for significant relief
by the short duration of the trials (4-10 days).
and overall short-term improvement in ALBP
The evidence for the use of dantrolene in the
with tizanidine and fair evidence that it is more
treatment of spasticity associated with MSK
effective than placebo in MSK conditions, such
conditions is also limited and inconsistent,
as acute neck pain. Cyclobenzaprine has been
calling into question its role in the treatment
best studied and has produced the most consis-
of these conditions. Although there are no
tent evidence, however. Although there is fair
well-designed RCTs comparing dantrolene and
evidence for the use of tizanidine compared to
baclofen, dantrolene appears to be associated
placebo in the treatment of spasticity (primarily
with more severe adverse events. Side effects
in multiple sclerosis), it appears to be roughly
most commonly reported include drowsiness,
equivalent to baclofen. A single, low quality
weakness, malaise, fatigue, and diarrhea.
study failed to demonstrate any difference in
Fatal and nonfatal cases of hepatitis have also
overall improvement for tizanidine compared to
been reported. Dantrolene is contraindicated
placebo in the treatment of sciatica. The most
in individuals with a history of compromised
frequently reported side effects appear to be
pulmonary function. It should also be used
dose-related and include dry mouth, somno-
with caution in individuals with a history of
lence, asthenia, and dizziness. Tizanidine can
also produce hypotension and has been asso-ciated with reports of QT prolongation. Liver
Methocarbamol is indicated as an adjunct
injury has been reported (regular monitoring
in the relief of discomforts associated with
of aminotransferase levels is recommended).
acute, painful MSK conditions. There is limited
Rebound can occur upon sudden withdrawal.
Reports of abuse and dependence exist, espe-
evidence, the DAC concluded that there was no
cially with concurrent use of opioids, benzodiaz-
compelling evidence demonstrating efficacy
or safety for the long-term use of any SMRs. Evidence is available for the short-term use of
Overall, systematic reviews have concluded
cyclobenzaprine, orphenadrine, and tizanidine
that most SMR studies have numerous
in the treatment of acute MSK conditions and
methodological shortcomings, are of short
for the use of baclofen and dantrolene in spas-
duration, and provide limited evidence for their
ticity in neurological illness. However, multiple
efficacy. Where efficacy has been observed,
notable safety concerns exist with tizanidine
the magnitude of benefit has generally been
and dantrolene. Hence, the DAC recommend-
modest to moderate. Furthermore, all SMRs
ed that: (i) cyclobenzaprine and orphenadrine
are associated with frequent adverse events
be listed on the 25WS (initial Musculoskeletal)
that may limit their usefulness; many are as-
formulary only; (ii) baclofen be listed on the
sociated with rare but serious side effects.
03WS (CNS - Brain Injury) formulary only; and
(iii) dantrolene, methocarbamol, and tizanidine
Guidelines were reviewed to establish best
practices. In general, the short-term use of
SMRs (e.g., cyclobenzaprine) is recommended in the treatment of acute or subacute back pain, when first-and second-line agents (i.e., acet-aminophen and nonsteroidal anti-inflammatory drugs, respectively) have failed to produce sufficient relief. Long-term use is not recom-mended due to lack of evidence and concerns regarding possible CNS side effects and depen-dence.
The Ontario Drug Benefit Program does not list most SMRs. Diazepam is listed as a psychoac-tive agent. Dantrolene and baclofen are listed for the treatment of spasticity due to neuro-logical illness (e.g., cerebral palsy, spinal cord injury, etc.).
The WSIB will consider all relevant facts and circumstances, and shall make its decision based upon the merits and
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