Refractory Migraine

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Refractory Migraine

Refractory migraine refers to migraine that fails to respond adequately to multiple standard preventive and acute treatments. There is no universally accepted definition, but the AHS/EHF propose criteria requiring failure of at least 3 preventive classes and 3 acute medication classes. These patients represent 3-5% of the migraine population and require systematic evaluation, multi-modal therapy, and often combination treatments. Before labeling migraine as refractory, it is essential to address modifiable factors including medication overuse, comorbid conditions, and treatment adequacy.

Bottom Line

Definition: Failure of ≥3 preventive medication classes at adequate dose/duration AND inadequate response to ≥3 acute treatments (including triptans)
Before calling it refractory: Rule out medication overuse headache, confirm diagnosis, address comorbidities (anxiety, depression, sleep disorders), and ensure prior treatments were given adequate trials
Combination therapy: The cornerstone of refractory management — combining treatments from different mechanism classes (e.g., Botox + CGRP mAb + nerve blocks)
CGRP mAbs after Botox failure: 30-40% of Botox non-responders respond to CGRP mAbs (different mechanism)
Procedural options: Serial nerve blocks, trigger point injections, IV infusion protocols, and neuromodulation devices
Multidisciplinary approach: Behavioral therapy, physical therapy, and biofeedback should always be part of the plan

Defining Refractory Migraine

Criterion	Requirement
Diagnosis	ICHD-3 migraine (episodic or chronic)
Preventive failures	Failure of ≥3 classes at adequate dose for ≥8 weeks each: • Beta-blocker (propranolol ≥120 mg or equivalent) • Antiepileptic (topiramate ≥100 mg or valproate ≥500 mg) • TCA or SNRI (amitriptyline ≥50 mg or venlafaxine ≥150 mg) • OnabotulinumtoxinA (≥2 cycles of 155 U) • CGRP mAb (≥3 months)
Acute treatment failures	Inadequate response to ≥3 acute medications including: • At least 2 triptans (different routes) • NSAID or combination analgesic • Gepant or ditan
Modifiable factors addressed	Medication overuse eliminated, comorbidities treated, lifestyle modifications implemented

Systematic Evaluation

Before Labeling Migraine as Refractory

Confirm the diagnosis: Review ICHD-3 criteria. Consider secondary headache mimics (especially in progressive or atypical presentations). CSF pressure disorders, cervicogenic headache, and occipital neuralgia may masquerade as refractory migraine.
Medication overuse: Present in up to 50% of patients referred for refractory migraine. Must be addressed first — no preventive works optimally in the setting of MOH.
Adequate trials? Many "failures" were at subtherapeutic doses or inadequate duration. Topiramate at 25 mg for 3 weeks is not a fair trial. Review each prior treatment systematically.
Comorbidities: Depression, anxiety, PTSD, insomnia, and sleep apnea all worsen migraine and must be treated concurrently. Untreated comorbidities are the most common reason for apparent treatment resistance.
Expectations: Patients may expect complete headache elimination. A realistic goal is ≥50% reduction in headache days and improved function — not necessarily headache freedom.

Combination Preventive Therapy

The key principle in refractory migraine is combining treatments from different mechanistic classes for additive or synergistic benefit.

Combination	Evidence	Rationale
OnabotulinumtoxinA + CGRP mAb	Growing real-world evidence. Blumenfeld (2021): erenumab add-on reduced migraine days by 4.4 additional days. Ailani (2022): 54% of Botox partial responders achieved ≥50% response after adding fremanezumab.	Complementary mechanisms: Botox blocks CGRP release; mAbs block CGRP in extracellular space
CGRP mAb + oral preventive	Permitted in pivotal trials. No pharmacokinetic interactions. Subgroup analyses show additive benefit.	mAb targets CGRP pathway; oral agent targets different pathway (beta-blocker, TCA, antiepileptic)
Botox + oral preventive	Common practice. No interaction data concerns.	Different targets; oral agents fill gaps between Botox cycles
Triple therapy (Botox + CGRP mAb + oral)	Case series only. Used in tertiary headache centers.	Maximum mechanism coverage for most refractory patients
Any preventive + nerve blocks	Widely used as adjunct. GON blocks every 2-4 weeks.	Addresses peripheral trigeminal sensitization; immediate relief while preventives take effect
Any preventive + neuromodulation	Device therapy (Cefaly, sTMS, Nerivio) can be added to any regimen without interaction.	Non-pharmacologic layer with no drug interactions

Switching Within CGRP Class

Failure of one CGRP mAb does not predict failure of others. Antibody targets differ: erenumab targets the CGRP receptor; galcanezumab, fremanezumab, and eptinezumab target the CGRP ligand.
Switch evidence: 30-40% of patients who fail one CGRP mAb respond to a different one (retrospective series)
mAb to gepant: Patients failing CGRP mAbs may respond to oral gepants (different pharmacology — small molecule competitive antagonist vs large molecule binding)
Eptinezumab (IV): Consider for patients failing SC mAbs. 100% bioavailability with IV dosing; quarterly infusion.

Procedural Interventions

Procedure	Frequency	Role in Refractory Migraine
GON block (+ LON, supraorbital)	Every 2-4 weeks	Bridge therapy; ongoing adjunct. Can use combined block (GON + frontal nerves bilaterally) for broader coverage.
SPG block (intranasal)	Twice weekly for 6 weeks (Cady protocol), then as needed	Targets parasympathetic pathway; may reduce attack frequency in chronic migraine
Trigger point injections	Every 4-6 weeks	Addresses pericranial muscle tenderness and peripheral sensitization. Trapezius, temporalis, SCM.
IV infusion protocol	As needed for prolonged attacks	Magnesium 2g + ketorolac 30mg + metoclopramide 10mg + dexamethasone 8mg +/- valproate 500-1000mg IV. Series of 3-5 infusions over 5-10 days for intractable migraine.
Ketamine infusion	Specialized centers only	Sub-anesthetic IV ketamine (0.1-0.5 mg/kg/hour) over 3-7 days. NMDA antagonism may reset central sensitization. Limited evidence; used in tertiary centers for most refractory cases.

Multidisciplinary Management

The Complete Refractory Migraine Program

Behavioral therapy (CBT): Level A evidence. Addresses pain catastrophizing, avoidance behavior, and maladaptive coping. Essential, not optional, in refractory patients.
Biofeedback: Thermal or EMG biofeedback. Level A evidence. Particularly useful for patients who want active participation in their treatment.
Physical therapy: Targets cervicogenic contributions, postural dysfunction, and pericranial myofascial pain. Cervical spine manual therapy reduces headache frequency in patients with neck involvement.
Psychology/psychiatry: Treat comorbid depression, anxiety, and PTSD. Address sleep disorders (CBT-I for insomnia). Consider that untreated psychiatric comorbidity is the number one barrier to migraine treatment success.
Lifestyle optimization: Consistent sleep-wake schedule, regular exercise (150 min/week), hydration, stress management, and trigger avoidance. These fundamentals must be reinforced even in highly treated patients.
Pain rehabilitation programs: Intensive outpatient or inpatient multidisciplinary headache programs (e.g., MIDAS, Mayo, Jefferson, Diamond) for the most refractory patients. Combine medication optimization, medication withdrawal, behavioral therapy, physical therapy, and infusion therapy over 2-3 weeks.

Investigational and Emerging Approaches

Psilocybin: Phase 2 trials ongoing for migraine prevention. Preliminary data suggest a single dose may reduce migraine frequency for weeks. Mechanism likely involves 5-HT2A-mediated neuroplasticity.
Invasive neuromodulation: Occipital nerve stimulation (ONS) has mixed RCT data; reserved for most refractory cases. SPG stimulation via implanted device (Pulsante) showed efficacy in cluster headache; migraine data pending.
Monoclonal antibodies targeting PACAP: PACAP (pituitary adenylate cyclase-activating polypeptide) is a second neuropeptide pathway implicated in migraine. Anti-PACAP antibodies are in early clinical development.
Novel oral targets: Orexin receptor antagonists, glutamate modulators, and neurosteroids are in preclinical or early clinical development for migraine.

Management Algorithm

Stepwise Approach to Refractory Migraine

Re-evaluate: Confirm diagnosis, eliminate MOH, treat comorbidities, verify adequate prior treatment trials
Optimize current regimen: Maximize dose of current preventive, add behavioral therapy and lifestyle interventions
Combine mechanisms: Add a treatment from a different class (e.g., if on Botox, add CGRP mAb; if on oral preventive, add nerve blocks)
Switch within CGRP class: Try a different mAb or switch mAb → gepant
Procedural layer: Add serial nerve blocks, SPG blocks, or neuromodulation devices
Infusion therapy: Outpatient IV infusion series for acute exacerbations or prolonged attacks
Intensive rehabilitation: Refer to multidisciplinary headache center for comprehensive inpatient/outpatient program
Investigational: Clinical trial enrollment for novel targets (PACAP, psilocybin, neuromodulation)

References

Schulman EA, et al. Defining refractory migraine and refractory chronic migraine: proposed criteria from the Refractory Headache Special Interest Section of the American Headache Society. Headache. 2008;48(6):778-782.
Blumenfeld AM, et al. Real-world evidence for the addition of CGRP monoclonal antibodies to onabotulinumtoxinA treatment for migraine. Headache. 2021;61(8):1246-1256.
Ailani J, et al. Fremanezumab in patients with chronic migraine and comorbid depression or anxiety: post hoc analysis of a randomized trial. Headache. 2022;62(1):34-46.
Sacco S, et al. European Headache Federation guideline on the use of monoclonal antibodies acting on the calcitonin gene related peptide or its receptor for migraine prevention. J Headache Pain. 2019;20(1):6.
Schwedt TJ, et al. Comprehensive systematic review and evidence-based guidelines for the management of refractory migraine. Headache. 2022;62(9):1169-1186.