Cyclobenzaprine Explained

Cyclobenzaprine, sold under several brand names including, historically, Flexeril, is a muscle relaxer used for muscle spasms from musculoskeletal conditions of sudden onset. It is not useful in cerebral palsy. It is taken by mouth.^[5]

Common side effects include headache, feeling tired, dizziness, and dry mouth.^[5] Serious side effects may include an irregular heartbeat.^[5] There is no evidence of harm in pregnancy, but it has not been well studied in this population.^[5] It should not be used together with MAOIs.^[5] How it works is unclear.^[5]

Cyclobenzaprine was approved for medical use in the United States in 1977.^[5] It is available by prescription as a generic medication.^[5] In 2021, it was the 45th most commonly prescribed medication in the United States, with more than 15million prescriptions.^{[6] [7]} It was not available in the United Kingdom as of 2012.^[8]

Medical use

Cyclobenzaprine is used, in conjunction with physical therapy, to treat muscle spasms that occur because of acute musculoskeletal conditions.^[9] After sustaining an injury, muscle spasms occur to stabilize the affected body part, which may increase pain to prevent further damage. Cyclobenzaprine is used to treat such muscle spasms associated with acute, painful musculoskeletal conditions.^[10] It decreases pain in the first two weeks,^{[11] [12]} peaking in the first few days, but has no proven benefit after two weeks.^[13] Since no benefit is proven beyond that, therapy should not be continued long-term. It is the best-studied muscle relaxer. It is not useful for spasticity due to neurologic conditions such as cerebral palsy.^[14]

A 2004 review found benefit for fibromyalgia symptoms, with a reported number needed to treat of 4.8 (meaning that 1 person out of every 4.8 benefits from treatment) for pain reduction, but no change in fatigue or tender points.^[15] A 2009 Cochrane review found insufficient evidence to justify its use in myofascial pain syndrome.^[16] It may also be used along with other treatments for tetanus.^[17]

Side effects

Cyclobenzaprine results in increased rates of drowsiness (38%), dry mouth (24%), and dizziness (10%). Drowsiness and dry mouth appear to intensify with increasing dose.^[18] The sedative effects of cyclobenzaprine are likely due to its antagonistic effect on histamine, serotonin, and muscarinic receptors.

Agitation is a common side effect observed, especially in the elderly. Some experts believe that cyclobenzaprine should be avoided in elderly patients because it can cause confusion, delirium, and cognitive impairment.^{[19] [20]} In general, the National Committee for Quality Assurance recommends avoiding the use of cyclobenzaprine in the elderly because of the potential for more severe side effects.^[21]

Dysphagia, a life-threatening side-effect, may rarely occur.^[22] Treatment protocols and support should follow the same as for any structurally related tricyclic, such as tricyclic antidepressants.^[23]

Overdose

The most common effects of overdose are drowsiness and tachycardia. Rare but potentially critical complications are cardiac arrest, abnormal heart rhythms, severe low blood pressure, seizures, and neuroleptic malignant syndrome. Life-threatening overdose is rare, however, as the median lethal dose is about 338 milligrams/kilogram in mice and 425 mg/kg in rats. The potential harm is increased when central nervous system depressants and antidepressants are also used; deliberate overdose often includes other drugs.

Interactions

Cyclobenzaprine has major contraindications with monoamine oxidase inhibitors (MAOIs). At least one study also found increased risk of serotonin syndrome when cyclobenzaprine was taken with the serotonergic drugs duloxetine or phenelzine.^[24]

These substances may interact with cyclobenzaprine:

• Central nervous system depressants (e.g. alcohol, opioids, benzodiazepines, nonbenzodiazepines, phenothiazines, carbamates, barbiturates, major tranquilizers)
• Monoamine oxidase inhibitors taken within two weeks of cyclobenzaprine may result in serious, life-threatening side effects.

Cyclobenzaprine may affect the medications used in surgical sedation and some surgeons request that patients temporarily discontinue its use prior to surgery.^[25]

Pharmacology

Cyclobenzaprine is a centrally acting muscle relaxant.^[26] Cyclobenzaprine is a 5-HT₂ receptor antagonist; it relieves muscle spasm through action on the central nervous system at the brain stem, rather than targeting the peripheral nervous system or muscles themselves.^[27]

Pharmacodynamics

Cyclobenzaprine (and metabolite)^[28] !Site!CBP!NCBP!Action

5-HT1A	5300	3200	Agonist
5-HT2A	5.2	13	Antagonist
5-HT2B	100	???	Antagonist
5-HT2C	5.2	43	Antagonist
α1A	5.6	34	ND
α2A	4.3	6.4	Antagonist
α2B	21	150	ND
α2C	21	48	ND
H1	1.3	5.6	ND
M1	7.9	30	ND
Values are Ki (nM), unless otherwise noted. The smaller the value, the more strongly the drug binds to the site.

Pharmacokinetics

Cyclobenzaprine has an oral bioavailability of about 55% and approximately 93% is bound to proteins in plasma. The half-life of the drug is 18 hours and it has a plasma clearance of 0.7 litres per minute.^{[26] [29] [30]}

Comparison to other medications

Cyclobenzaprine has been found to be not inferior to tizanidine, orphenadrine, and carisoprodol in the treatment of acute lower back pain, although none have been proven to be effective for long-term use (beyond two weeks of treatment). No differences in pain or spasm scores were noted among these agents, nor when compared to benzodiazepines.^[31] However, nonbenzodiazepine (including cyclobenzaprine) treatment was found to have a lower risk of medication abuse and continuation of use against medical advice. Side effects such as sedation and ataxia are also less pronounced with nonbenzodiazepine antispasmodics.

In a study on the treatment of musculoskeletal pain treatment with cyclobenzaprine alone or in combination with ibuprofen, no significant differences in pain scores were noted among the three treatment groups. Peak benefit was found to occur on day seven of the treatment for all groups.^[32]

Formulations

By mouth, cyclobenzaprine is marketed as Apo-Cyclobenzaprin, Fexmid, Flexeril and Novo-Cycloprine. It is available in generic form. A once-a-day, extended-release formulation, Amrix, is available.^[33] Cyclobenzaprine is also used by compounding pharmacies in topical creams.

Notes and References

1. Micromedex® 2010 – DRUGDEX Evaluations (Cyclobenzaprine Hydrochloride)
2. Web site: Cyclobenzaprine Hydrochloride Tablets USP Revised: April 2005 Rx only . nih.gov . 1 October 2016 .
3. Web site: AMR40470 (Amrix) Prescribing Information. May 2016. Teva Pharmaceuticals USA, Inc.
4. Web site: NDA 17-821/S-045 Flexeril (Cyclobenzaprine HCl) Tablets. U.S. Food and Drug Administration.
5. Web site: Cyclobenzaprine Monograph for Professionals . Drugs.com . AHFS . 22 December 2018 .
6. Web site: The Top 300 of 2021 . ClinCalc . 14 January 2024 . 15 January 2024 . https://web.archive.org/web/20240115223848/https://clincalc.com/DrugStats/Top300Drugs.aspx . live .
7. Web site: Cyclobenzaprine - Drug Usage Statistics . ClinCalc . 14 January 2024.
8. Fibromyalgia, psychiatric comorbidity, and the somatosensory cortex . British Journal of Medical Practitioners . 2012 . 5 . 2 . a522 .
9. Yang YW, Macdonald JB, Nelson SA, Sekulic A . Treatment of vismodegib-associated muscle cramps with cyclobenzaprine: A retrospective review . Journal of the American Academy of Dermatology . 77 . 6 . 1170–1172 . December 2017 . 29132849 . 10.1016/j.jaad.2016.12.017 . 8265576 .
10. Web site: Cyclobenzaprine- cyclobenzaprine hydrochloride tablet, film coated . DailyMed . 30 December 2019 . 26 September 2020.
11. Chou R, Peterson K, Helfand M . Comparative efficacy and safety of skeletal muscle relaxants for spasticity and musculoskeletal conditions: a systematic review . Journal of Pain and Symptom Management . 28 . 2 . 140–75 . August 2004 . 15276195 . 10.1016/j.jpainsymman.2004.05.002 . free .
12. van Tulder MW, Touray T, Furlan AD, Solway S, Bouter LM . Muscle relaxants for non-specific low back pain . The Cochrane Database of Systematic Reviews . 2 . 2 . CD004252 . 2003 . 12804507 . 6464310 . 10.1002/14651858.CD004252 . Van Tulder . Maurits W .
13. Browning R, Jackson JL, O'Malley PG . Cyclobenzaprine and back pain: a meta-analysis . Archives of Internal Medicine . 161 . 13 . 1613–20 . July 2001 . 11434793 . 10.1001/archinte.161.13.1613 . free .
14. Ashby P, Burke D, Rao S, Jones RF . Assessment of cyclobenzaprine in the treatment of spasticity . Journal of Neurology, Neurosurgery, and Psychiatry . 35 . 5 . 599–605 . October 1972 . 4563483 . 494138 . 10.1136/jnnp.35.5.599 .
15. Tofferi JK, Jackson JL, O'Malley PG . Treatment of fibromyalgia with cyclobenzaprine: A meta-analysis . Arthritis and Rheumatism . 51 . 1 . 9–13 . February 2004 . 14872449 . 10.1002/art.20076 . free .
16. Leite FM, Atallah AN, El Dib R, Grossmann E, Januzzi E, Andriolo RB, da Silva EM . Cyclobenzaprine for the treatment of myofascial pain in adults . The Cochrane Database of Systematic Reviews . 3 . CD006830 . July 2009 . 2009 . 19588406 . 6481902 . 10.1002/14651858.CD006830.pub3 .
17. Book: Smith . Blaine T. . Pharmacology for Nurses . 2014 . Jones & Bartlett Publishers . 9781449689407 . 122 .
18. Web site: Flexeril: Side effects . 22 February 2010 . RxList.com . dead . https://web.archive.org/web/20080912150824/http://www.rxlist.com/cgi/generic/cyclobnz_ad.htm . 12 September 2008 . dmy-all .
19. Book: Ottawa, Ontario . Canadian Agency for Drugs and Technologies in Health . 23 February 2015 . Long-term Use of Cyclobenzaprine for Pain: A Review of the Clinical Effectiveness . CADTH Rapid Response Reports . 25763449 .
20. Potentially inappropriate medications for the elderly according to the revised Beers criteria. 2012. Duke Clinical Research Institute website. https://wayback.archive-it.org/all/20130507004226/http://www.americangeriatrics.org/files/documents/beers/2012AGSBeersCriteriaCitations.pdf
21. Web site: High risk medications. dead. https://web.archive.org/web/20100201113909/http://www.ncqa.org/Portals/0/Newsroom/SOHC/Drugs_Avoided_Elderly.pdf. 1 February 2010. 22 February 2010. National Committee for Quality Assurance.
22. Web site: MEDICATIONS AND DYSPHAGIA/ SWALLOWING RISKS.
23. Chabria SB. July 2006. Rhabdomyolysis: a manifestation of cyclobenzaprine toxicity. Journal of Occupational Medicine and Toxicology. 1. 1. 16. 10.1186/1745-6673-1-16. 1540431. 16846511 . free .
24. Keegan MT, Brown DR, Rabinstein AA . Serotonin syndrome from the interaction of cyclobenzaprine with other serotoninergic drugs . Anesthesia and Analgesia . 103 . 6 . 1466–8 . December 2006 . 17122225 . 10.1213/01.ane.0000247699.81580.eb . free .
25. Web site: Medications to Avoid, Continue, or Stop - Before & After Surgery. Medical Practice of William H. Gorman, M.D.. 18 February 2014. 2 February 2017. 1 December 2017. https://web.archive.org/web/20171201233049/https://www.whgormanmd.com/blog/2014/1/3/medications-to-avoid-continue-or-stop-before-surgery. dead.
26. Web site: Cyclobenzaprine . www.drugbank.ca.
27. Kobayashi H, Hasegawa Y, Ono H . Cyclobenzaprine, a centrally acting muscle relaxant, acts on descending serotonergic systems . European Journal of Pharmacology . 311 . 1 . 29–35 . September 1996 . 8884233 . 10.1016/0014-2999(96)00402-5 .
28. Web site: Cyclobenzaprine (CBP) and Its Major Metabolite Norcyclobenzaprine (nCBP) Are Potent Antagonists of Human Serotonin Receptor 2a (5HT2a), Histamine Receptor H-1 and α-Adrenergic Receptors: Mechanistic and Safety Implications for Treating Fibromyalgia Syndrome by Improving Sleep Quality. 27 January 2022. ACR Meeting Abstracts. en-US.
29. Web site: Cyclobenzaprine . pubchem.ncbi.nlm.nih.gov . en.
30. Winchell GA, King JD, Chavez-Eng CM, Constanzer ML, Korn SH . Cyclobenzaprine pharmacokinetics, including the effects of age, gender, and hepatic insufficiency . Journal of Clinical Pharmacology . 42 . 1 . 61–9 . January 2002 . 11808825 . 10.1177/0091270002042001007 . 7749001 .
31. Web site: Medscape: Medscape Access . medscape.com . 1 October 2016 .
32. Childers MK, Petri M, Laudadio C, Harrison D, Silber S, Bowen D . Comparison of cyclobenzaprine alone versus cyclobenzaprine plus ibuprofen in patients with acute musculoskeletal spasm and pain . 10.1016/j.annemergmed.2004.07.286 . Annals of Emergency Medicine . 44 . 4 . S87–S88 . 2004 .
33. Web site: Patient Web site for Amrix (Cyclobenzaprine Hydrochloride Extended-Release Capsules) . amrix.com . 1 October 2016 .