This is the current release of the guideline.

• Trigeminal neuralgia (TN)
• Classic TN (CTN)
• Symptomatic TN (STN)

Diagnosis
Evaluation
Screening
Treatment

Family Practice
Internal Medicine
Neurological Surgery
Neurology
Pharmacology

Physicians

• To perform an evidence-based review of the diagnosis and treatment of trigeminal neuralgia (TN) and make evidence-based recommendations
• To address the following TN diagnostic questions:
  • How often does routine neuroimaging (computed tomography [CT], magnetic resonance imaging [MRI]) identify a structural cause of TN (excluding vascular contact with compression of the fifth cranial nerve)?
  • Which clinical or laboratory features accurately identify patients with symptomatic TN (STN)?
  • For patients with classic TN (CTN), does high-resolution MRI accurately identify patients with neurovascular compression?
• To address the following TN pharmacologic questions:
  • Which drugs effectively treat CTN?
  • Which drugs effectively treat STN?
  • Is there evidence of efficacy of intravenous drugs in acute exacerbations of TN?
• To address the following TN surgical questions:
  • When should surgery be offered?
  • Which surgical technique gives the longest pain-free period with the fewest complications and good quality of life?
  • Which surgical techniques should be used in patients with multiple sclerosis?

Patients with trigeminal neuralgia

Diagnosis/Evaluation

1. Routine neuroimaging (computed tomography [CT], magnetic resonance imaging [MRI])
2. Identification of patients with symptomatic trigeminal neuralgia (STN) through clinical examination
3. Electrophysiology studies (measurement of trigeminal reflexes)
4. Use of high-resolution MRI to identify neurovascular compression (considered but not recommended)

Treatment

1. Carbamazepine
2. Oxcarbazepine
3. Baclofen
4. Lamotrigine
5. Pimozide
6. Percutaneous procedures on the Gasserian ganglion
7. Gamma knife surgery
8. Microvascular decompression
9. Topical ophthalmic anesthesia (specifically not recommended)

• Diagnostic yields of imaging studies
• Diagnostic accuracy of assessing clinical features for predicting risk of symptomatic trigeminal neuralgia (STN)
• Diagnostic accuracy of measuring trigeminal reflexes and trigeminal evoked potentials for identifying patients with STN
• Sensitivity and specificity of high-resolution magnetic resonance imaging (MRI) to identify neurovascular compression
• Effectiveness of drug treatment for reducing pain
• Effectiveness of surgery for reducing pain and improving quality of life
• Adverse and side effects of pharmacological therapies
• Complications of surgery
• Quality of life
• Mortality

Hand-searches of Published Literature (Primary Sources)
Hand-searches of Published Literature (Secondary Sources)
Searches of Electronic Databases

The American Academy of Neurology (AAN) and European Federation of Neurological Societies (EFNS) assembled a panel of experts who searched MEDLINE, EMBASE, and the Cochrane library. Searches extended from the time of database inception to December 2007. All searches used the following synonyms for TN: trigeminal neuralgia, tic douloureux, facial pain, or trigeminal neuropathy. The primary search was supplemented by a secondary search using the bibliography of retrieved articles and knowledge from the panel. Only full-length original communications were accepted. Inclusion criteria were as follows: relevant to the clinical questions, limited to human subjects, randomized controlled trials, case control, cohort studies, case series >6, or meta-analysis. Abstracts, reviews, and studies with undocumented or unstated mention of improvement were excluded.

47

Weighting According to a Rating Scheme (Scheme Given)

Classification of Evidence for Rating of a Screening Article

Class I: A statistical, population-based sample of patients studied at a uniform point in time (usually early) during the course of the condition. All patients undergo the intervention of interest. The outcome, if not objective, is determined in an evaluation that is masked to the patients' clinical presentations.

Class II: A statistical, non-referral-clinic-based sample of patients studied at a uniform point in time (usually early) during the course of the condition. Most patients undergo the intervention of interest. The outcome, if not objective, is determined in an evaluation that is masked to the patients' clinical presentations.

Class III: A sample of patients studied during the course of the condition. Some patients undergo the intervention of interest. The outcome, if not objective, is determined in an evaluation by someone other than the treating physician.

Class IV: Expert opinion, case reports or any study not meeting criteria for Class I to III.

Classification of Evidence for Rating of a Diagnostic Article

Class I: Evidence provided by a prospective study in a broad spectrum of persons with the suspected condition, using a reference (gold) standard for case definition, where test is applied in a blinded evaluation, and enabling the assessment of appropriate tests of diagnostic accuracy. All patients undergoing the diagnostic test have the presence or absence of the disease determined.

Class II: Evidence provided by a prospective study of a narrow spectrum of persons with the suspected condition, or a well designed retrospective study of a broad spectrum of persons with an established condition (by "gold standard") compared to a broad spectrum of controls, where test is applied in a blinded evaluation, and enabling the assessment of appropriate tests of diagnostic accuracy.

Class III: Evidence provided by a retrospective study where either persons with the established condition or controls are of a narrow spectrum, and where the reference standard, if not objective, is applied by someone other than the person that performed the test.

Class IV: Any design where test is not applied in an independent evaluation OR evidence provided by expert opinion alone or in descriptive case series (without controls).

Classification of Evidence for Rating of a Therapeutic Article

Class I: Prospective, randomized, controlled clinical trial with masked outcome assessment, in a representative population. The following are required:

1. Concealed allocation
2. Primary outcome(s) clearly defined
3. Exclusion/inclusion criteria clearly defined
4. Adequate accounting for drop-outs and cross-overs with numbers sufficiently low to have minimal potential for bias
5. Relevant baseline characteristics are presented and substantially equivalent among treatment groups or there is appropriate statistical adjustment for differences.

Class II: Prospective matched group cohort study in a representative population with masked outcome assessment that meets a-e above OR a randomized controlled trial in a representative population that lacks one criteria a-d.

Class III: All other controlled trials (including well-defined natural history controls or patients serving as own controls) in a representative population, where outcome is independently assessed, or independently derived by objective outcome measurement.*

Class IV: Evidence from uncontrolled studies, case series, case reports, or expert opinion.

*Objective outcome measurement: an outcome measure that is unlikely to be affected by an observer's (patient, treating physician, investigator) expectation or bias (e.g., blood tests, administrative outcome data).

Systematic Review with Evidence Tables

Panel members reviewed abstracts and titles for relevance. Two panel members reviewed papers meeting inclusion criteria. An additional panel member arbitrated disagreements. The risk of bias was determined using the classification of evidence for each study (Classes I–IV; see "Rating Scheme for the Strength of the Evidence).

Other

Not stated

Classification of Recommendations

Level A = Established as effective, ineffective, or harmful (or established as useful/predictive or not useful/predictive) for the given condition in the specified population. (Level A rating requires at least two consistent Class I studies.)**

Level B = Probably effective, ineffective, or harmful (or probably useful/predictive or not useful/predictive) for the given condition in the specified population. (Level B rating requires at least one Class I study or at least two consistent Class II studies.)

Level C = Possibly effective, ineffective, or harmful (or possibly useful/predictive or not useful/predictive) for the given condition in the specified population. (Level C rating requires at least one Class II study or two consistent Class III studies.)

Level U = Data inadequate or conflicting; given current knowledge, treatment (test, predictor) is unproven. (Studies not meeting criteria for Class I–Class III.)

**In exceptional cases, one convincing Class I study may suffice for an "A" recommendation if 1) all criteria are met, 2) the magnitude of effect is large (relative rate improved outcome >5 and the lower limit of the confidence interval is <2).

A formal cost analysis was not performed and published cost analyses were not reviewed.

External Peer Review
Internal Peer Review

This guideline was approved by the Quality Standards Subcommittee on February 8, 2008; by the Practice Committee on March 20, 2008; and by the American Academy of Neurology Board of Directors on June 30, 2008.

Definitions of the classification of screening evidence (Classes I–IV), classification of therapeutic evidence (Classes I–IV), and strength of recommendations (A, B, C, U) are provided at the end of the "Major Recommendations" field.

For patients with trigeminal neuralgia (TN), routine imaging may be considered to identify symptomatic TN (STN) (Level C).

The presence of trigeminal sensory deficits or bilateral involvement of the trigeminal nerves should be considered useful to identify patients with STN. However, because of poor specificity, the absence of these features is not useful for excluding STN (Level B).

Measuring trigeminal reflexes in a qualified electrophysiologic laboratory should be considered useful for distinguishing STN from classic TN (CTN) (Level B).

Younger age at onset, involvement of the first division of the trigeminal nerve, unresponsiveness to treatment, and abnormal trigeminal evoked potentials should be disregarded as useful for accurately identifying patients with STN (Level B).

To control pain in patients with TN: carbamazepine should be offered (Level A), oxcarbazepine should be considered (Level B), baclofen, lamotrigine, and pimozide may be considered (Level C), and topical ophthalmic anesthesia should not be considered (Level B).

For patients with TN refractory to medical therapy: early surgical therapy may be considered (Level C), and percutaneous procedures on the Gasserian ganglion, gamma knife, and microvascular decompression may be considered (Level C).

Definitions:

Classification of Evidence for Rating of a Screening Article

Class I: A statistical, population-based sample of patients studied at a uniform point in time (usually early) during the course of the condition. All patients undergo the intervention of interest. The outcome, if not objective, is determined in an evaluation that is masked to the patients' clinical presentations.

Class II: A statistical, non-referral-clinic-based sample of patients studied at a uniform point in time (usually early) during the course of the condition. Most patients undergo the intervention of interest. The outcome, if not objective, is determined in an evaluation that is masked to the patients' clinical presentations.

Class III: A sample of patients studied during the course of the condition. Some patients undergo the intervention of interest. The outcome, if not objective, is determined in an evaluation by someone other than the treating physician.

Class IV: Expert opinion, case reports or any study not meeting criteria for Class I to III.

Classification of Evidence for Rating of a Diagnostic Article

Class I: Evidence provided by a prospective study in a broad spectrum of persons with the suspected condition, using a reference (gold) standard for case definition, where test is applied in a blinded evaluation, and enabling the assessment of appropriate tests of diagnostic accuracy. All patients undergoing the diagnostic test have the presence or absence of the disease determined.

Class II: Evidence provided by a prospective study of a narrow spectrum of persons with the suspected condition, or a well designed retrospective study of a broad spectrum of persons with an established condition (by "gold standard") compared to a broad spectrum of controls, where test is applied in a blinded evaluation, and enabling the assessment of appropriate tests of diagnostic accuracy.

Class III: Evidence provided by a retrospective study where either persons with the established condition or controls are of a narrow spectrum, and where the reference standard, if not objective, is applied by someone other than the person that performed the test.

Class IV: Any design where test is not applied in an independent evaluation OR evidence provided by expert opinion alone or in descriptive case series (without controls).

Classification of Evidence for Rating of a Therapeutic Article

Class I: Prospective, randomized, controlled clinical trial with masked outcome assessment, in a representative population. The following are required:

1. Concealed allocation
2. Primary outcome(s) clearly defined
3. Exclusion/inclusion criteria clearly defined
4. Adequate accounting for drop-outs and cross-overs with numbers sufficiently low to have minimal potential for bias
5. Relevant baseline characteristics are presented and substantially equivalent among treatment groups or there is appropriate statistical adjustment for differences.

Class II: Prospective matched group cohort study in a representative population with masked outcome assessment that meets a-e above OR a randomized controlled trial in a representative population that lacks one criteria a-d.

Class III: All other controlled trials (including well-defined natural history controls or patients serving as own controls) in a representative population, where outcome is independently assessed, or independently derived by objective outcome measurement.*

Class IV: Evidence from uncontrolled studies, case series, case reports, or expert opinion.

*Objective outcome measurement: an outcome measure that is unlikely to be affected by an observer's (patient, treating physician, investigator) expectation or bias (e.g., blood tests, administrative outcome data).

Classification of Recommendations

Level A = Established as effective, ineffective, or harmful (or established as useful/predictive or not useful/predictive) for the given condition in the specified population. (Level A rating requires at least two consistent Class I studies.)**

Level B = Probably effective, ineffective, or harmful (or probably useful/predictive or not useful/predictive) for the given condition in the specified population. (Level B rating requires at least one Class I study or at least two consistent Class II studies.)

Level C = Possibly effective, ineffective, or harmful (or possibly useful/predictive or not useful/predictive) for the given condition in the specified population. (Level C rating requires at least one Class II study or two consistent Class III studies.)

Level U = Data inadequate or conflicting; given current knowledge, treatment (test, predictor) is unproven. (Studies not meeting criteria for Class I–Class III.)

**In exceptional cases, one convincing Class I study may suffice for an "A" recommendation if 1) all criteria are met, 2) the magnitude of effect is large (relative rate improved outcome >5 and the lower limit of the confidence interval is <2).

None provided

The type of supporting evidence is identified and graded for each recommendation (see "Major Recommendations").

Appropriate diagnostic evaluation and treatment of trigeminal neuralgia

• Carbamazepine is sometimes poorly tolerated and severe adverse events have been reported.
• Sensory loss after percutaneous procedures is present in almost half of patients. Less than 6% develop troublesome dysesthesias. The incidence of anesthesia dolorosa is around 4%. Postoperatively, 12% of patients report a discomfort described as burning, heavy, aching, or tiring. Corneal numbness, with the risk of keratitis, occurs in 4% of patients. Problems with other cranial nerves are uncommon, and the major perioperative complication is meningitis, mainly aseptic (0.2%). Up to 50% of patients undergoing balloon compression suffer temporary and rarely chronic masticatory problems. Mortality is extremely low.
• After gamma knife surgery, studies report sensory complications in some patients; complications include facial numbness, troublesome sensory loss, and paresthesias. There have been no reports of complications unrelated to the trigeminal nerve.
• The average mortality associated with microvascular decompression is 0.2%. Up to 4% of patients incur major problems such as cerebrospinal fluid leaks, infarcts, or hematomas. Aseptic meningitis is the most common complication (occurring in 11% of patients). Diplopia is often transient and facial weakness is rare. Sensory loss occurs in 7% of patients. The major long-term complication is hearing loss which can occur in as many as 10% of patients.

This statement is provided as an educational service of the American Academy of Neurology. It is based on an assessment of current scientific and clinical information. It is not intended to include all possible proper methods of care for a particular neurologic problem or all legitimate criteria for choosing to use a specific procedure. Neither is it intended to exclude any reasonable alternative methodologies. The AAN recognizes that specific patient care decisions are the prerogative of the patient and the physician caring for the patient, based on all of the circumstances involved. The clinical context section is made available in order to place the evidence-based guideline into perspective with current practice habits and challenges. No formal practice recommendations should be inferred.

An implementation strategy was not provided.

Living with Illness

Effectiveness
Patient-centeredness

Not applicable: The guideline was not adapted from another source.

2008 Oct 7

American Academy of Neurology - Medical Specialty Society
European Federation of Neurological Societies - Medical Specialty Society

American Academy of Neurology (AAN)

Quality Standards Subcommittee

Primary Authors: G. Gronseth, MD, FAAN; G. Cruccu, MD; J. Alksne, MD; C. Argoff, MD; M. Brainin, MD, FESO; K. Burchiel, MD; T. Nurmikko, MD, PhD; J.M. Zakrzewska, MD, FDSRCS, FFDRCSI

Quality Standards Subcommittee Members: Jacqueline French, MD, FAAN (Chair); Charles E. Argoff, MD; Eric Ashman, MD; Stephen Ashwal, MD, FAAN (Ex-officio); Christopher Bever, Jr., MD, MBA, FAAN; John D. England, MD, FAAN; Gary Franklin, MD, MPH, FAAN (Ex-officio); Deborah Hirtz, MD, FAAN (Ex-officio); Robert G. Holloway, MD, MPH, FAAN; Donald J. Iverson, MD, FAAN; Steven R. Messé, MD; Leslie A. Morrison, MD; James C. Stevens, MD, FAAN (Ex-officio); David J. Thurman, MD, MPH (Ex-officio); Dean M. Wingerchuk, MD, MSc, FRCP(C); Theresa A. Zesiewicz, MD, FAAN

This is the current release of the guideline.

This summary was completed by ECRI Institute on September 23, 2008. This summary was completed by ECRI Institute on November 10, 2008. The information was verified by the guideline developer on December 11, 2008. This summary was updated by ECRI Institute on May 1, 2009 following the U.S. Food and Drug Administration advisory on antiepileptic drugs.

This NGC summary is based on the original guideline, which is copyrighted by the American Academy of Neurology.