TREATMENT
Nonpharmacologic Approaches for All Migraineurs Migraine can often be managed to some degree by a variety of nonpharmacologic approaches. The measures that apply to a given individual should be used routinely since they provide a simple, cost-effective approach to migraine management. Patients with migraine do not encounter more stress than headache-free individuals; overresponsiveness to stress appears to be the issue. Since the stresses of everyday living cannot be eliminated, lessening one's response to stress by various techniques is helpful for many patients. These include yoga, transcendental meditation, hypnosis, and conditioning techniques such as biofeedback. For most patients, this approach is, at best, an adjunct to pharmacotherapy. Avoidance of migraine trigger factors may also provide significant prophylactic benefits . Unfortunately, these measures are unlikely to prevent all migraine attacks. When these measures fail to prevent an attack, then pharmacologic approaches are needed to abort an attack.
Pharmacologic Treatment of Acute Migraine The mainstay of pharmacologic therapy is the judicious use of one or more of the many drugs that are effective in migraine. The selection of the optimal regimen for a given patient depends on a number of factors, the most important of which is the severity of the attack. Mild migraine attacks can usually be managed by oral agents; the average efficacy rate is 50-70%. Severe migraine attacks may require parenteral therapy. Most drugs effective in the treatment of migraine are members of one of three major pharmacologic classes: anti-inflammatory agents, 5-HT1 agonists, and dopamine antagonists.
lists specific drugs effective in migraine. In general, an adequate dose of whichever agent is chosen should be used as soon as possible after the onset of an attack. If additional medication is required within 60 min because symptoms return or have not abated, the initial dose should be increased for subsequent attacks. Migraine therapy must be individualized for each patient; a standard approach for all patients is not possible. A therapeutic regimen may need to be constantly refined and personalized until one is identified that provides the patient with rapid, complete, and consistent relief with minimal side effects.
Nonsteroidal anti-inflammatory agents Both the severity and duration of a migraine attack can be reduced significantly by anti- inflammatory agents. Indeed, many undiagnosed migraineurs are self- treated with nonprescription anti-inflammatory agents. A general consensus is that NSAIDs are most effective when taken early in the migraine attack. However, the effectiveness of anti-inflammatory agents in migraine is usually less than optimal in moderate or severe migraine attacks. The combination of acetaminophen, aspirin, and caffeine (Excedrin Migraine) has been approved for use by the U.S. Food and Drug Administration (FDA) for the treatment of mild to moderate migraine. The combination of aspirin and metoclopramide has been show to be equivalent to a single dose of sumatriptan. Major side effects of NSAIDs include dyspepsia and gastrointestinal irritation.
5-HT1 agonists
ORAL Stimulation of 5-HT1 receptors can stop an acute migraine attack. Ergotamine and dihydroergotamine are nonselective receptor agonists, while the series of drugs known as triptans are selective 5-HT1 receptor agonists. A variety of triptans (e.g., naratriptan, rizatriptan, sumatriptan, zolmitriptan) are now available for the treatment of migraine .
Each of the triptan class of drugs has similar pharmacologic properties, but varies slightly in terms of clinical efficacy. Rizatriptan appears to be the fastest acting and most efficacious of the triptans currently available in the United States. Sumatriptan and zolmitriptan have similar rates of efficacy as well as time to onset, whereas naratriptan is the slowest acting and the least efficacious. Clinical efficacy appears to be related more to the tmax (time to peak plasma level) than to the potency, half-life, or bioavailability . This observation is in keeping with a significant body of data indicating that faster-acting analgesics are more efficacious than slower-acting agents.
Unfortunately, monotherapy with a selective oral 5-HT1 agonist does not result in rapid, consistent, and complete relief of migraine in all patients. Triptans are not effective in migraine with aura unless given after the aura is completed and the headache initiated. Side effects, although often mild and transient, occur in up to 89% of patients. Moreover, 5-HT1 agonists are contraindicated in individuals with a history of cardiovascular disease. Recurrence of headache is a major limitation of triptan use, and occurs at least occasionally in 40 to 78% of patients.
Ergotamine preparations offer a nonselective means of stimulating 5-HT receptors. A nonnauseating dose of ergotamine should be sought since a dose that provokes nausea is too high and may intensify head pain. Except for a sublingual formulation of ergotamine (Ergomar), oral formulations of ergotamine also contain 100 mg caffeine (theoretically to enhance ergotamine absorption and possibly to add additional vasoconstrictor activity). The average oral ergotamine dose for a migraine attack is 2 mg. Since the clinical studies demonstrating the efficacy of ergotamine in migraine predated the clinical trial methodologies used with the triptans, it is difficult to assess the clinical efficacy of ergotamine versus the triptans. In general, ergotamine appears to have a much higher incidence of nausea than triptans, but less headache recurrence.
NASAL The fastest acting nonparenteral antimigraine therapies that can be self-administered include nasal formulations of dihydroergotamine (Migranal) or sumatriptan (Imitrex Nasal). The nasal sprays result in substantial blood levels within 30 to 60 min. However, the nasal formulations suffer from inconsistent dosing, poor taste, and variable efficacy. Although in theory the nasal sprays might provide faster and more effective relief of a migraine attack than oral formulations, their reported efficacy is only approximately 50 to 60%.
PARENTERAL Parenteral administration of drugs such as dihydroergotamine (DHE-45 Injectable) and sumatriptan (
Dopamine Antagonists
ORAL Oral dopamine antagonists should be considered as adjunctive therapy in migraine. Drug absorption is impaired during migrainous attacks because of reduced gastrointestinal motility. Delayed absorption occurs in the absence of nausea and is related to the severity of the attack and not its duration. Therefore, when oral NSAIDs and/or triptan agents fail, the addition of a dopamine antagonist such as metoclopramide, 10 mg, should be considered to enhance gastric absorption. In addition, dopamine antagonists decrease nausea/vomiting and restore normal gastric motility.
PARENTERAL Parenteral dopamine antagonists (e.g., chlorpromazine, prochlorperazine, metoclopramide) can also provide significant acute relief of migraine; they can be used in combination with parenteral 5-HT1 agonists. A common intravenous protocol used for the treatment of severe migraine is the administration over 2 min of a mixture of 5 mg of prochlorperazine and 0.5 mg of dihydroergotamine.
Other Medications for Acute Migraine
ORAL The combination of acetaminophen, dichloralphenazone, and isometheptene (i.e., Midrin, Duradrin, generic), one to two capsules, has been classified by the FDA as "possibly" effective in the treatment of migraine. Since the clinical studies demonstrating the efficacy of this combination analgesic in migraine predated the clinical trial methodologies used with the triptans, it is difficult to assess the clinical efficacy of this sympathomimetic compound in comparison to other agents.
NASAL A nasal preparation of butorphanol is available for the treatment of acute pain. As with all narcotics, the use of nasal butorphanol should be limited to a select group of migraineurs, as described below.
PARENTERAL Narcotics are effective in the acute treatment of migraine. For example, intravenous meperidene (Demerol), 50 to 100 mg, is given frequently in the emergency room. This regimen "works" in the sense that the pain of migraine is eliminated. However, this regimen is clearly suboptimal in patients with recurrent headache for two major reasons. First, narcotics do not treat the underlying headache mechanism; rather, they act at the thalamic level to alter pain sensation. Second, the recurrent use of narcotics can lead to significant problems. In patients taking oral narcotics such as oxycodone (Percodan) or hydrocodone (Vicoden), narcotic addiction can greatly confuse the treatment of migraine. The headache that results from narcotic craving and/ or withdrawal can be difficult to distinguish from chronic migraine. Therefore, it is recommended that narcotic use in migraine be limited to patients with severe, but infrequent, headaches that are unresponsive to other pharmacologic approaches.
Prophylactic Treatment of Migraine A substantial number of drugs are now available that have the capacity to stabilize migraine. The decision of whether to use this approach depends on the frequency of attacks and on how well acute treatment is working. The occurrence of at least three attacks per month could be an indication for this approach. Drugs must be taken daily and there is usually a lag of at least 2 to 6 weeks before an effect is seen. The drugs that have been approved by the FDA for the prophylactic treatment of migraine include propranolol, timolol, sodium valproate, and methysergide. In addition, a number of other drugs appear to display prophylactic efficacy. This group of drugs includes amitriptyline, nortriptyline, verapamil, phenelzine, isocarbazid, and cyproheptadine. Phenelzine and methysergide are usually reserved for recalcitrant cases because of their serious potential side effects. Phenelzine is an MAOI; therefore, tyramine-containing foods, decongestants, and meperidine are contraindicated. Methysergide may cause retroperitoneal or cardiac valvular fibrosis when it is used for more than 8 months, thus monitoring is required for patients using this drug; the risk of the fibrotic complication is about 1:1500 and is likely to reverse after the drug is stopped.
The probability of success with any one of the antimigraine drugs is 50 to 75%; thus, if one drug is assessed each month, there is a good chance that effective stabilization will be achieved within a few months. Many patients are managed adequately with low-dose amitriptyline, propranolol, or valproate. If these agents fail or lead to unacceptable side effects, then methysergide or phenelzine can be used. Once effective stabilization is achieved, the drug is continued for 5 to 6 months and then slowly tapered to assess the continued need. Many patients are able to discontinue medication and experience fewer and milder attacks for long periods, suggesting that these drugs may alter the natural history of migraine.
CLUSTER HEADACHE
A variety of names have been used for this condition, including Raeder's syndrome, histamine cephalalgia, and sphenopalatine neuralgia. Cluster headache is a distinctive and treatable vascular headache syndrome. The episodic type is most common and is characterized by one to three short-lived attacks of periorbital pain per day over a 4- to 8-week period, followed by a pain- free interval that averages 1 year. The chronic form, which may begin de novo or several years after an episodic pattern has become established, is characterized by the absence of sustained periods of remission. Each type may transform into the other. Men are affected seven to eight times more often than women; hereditary factors are usually absent. Although the onset is generally between ages 20 and 50, it may occur as early as the first decade of life. Propranolol and amitriptyline are largely ineffective. Lithium is beneficial for cluster headache and ineffective in migraine. The cluster syndrome is thus clinically, genetically, and therapeutically different from migraine. Nevertheless, mixed features of the two disorders are occasionally present, suggesting some common elements to their pathogenesis.
Clinical Features Periorbital or, less commonly, temporal pain begins without warning and reaches a crescendo within 5 min. It is often excruciating in intensity and is deep, nonfluctuating, and explosive in quality; only rarely is it pulsatile. Pain is strictly unilateral and usually affects the same side in subsequent months. Attacks last from 30 min to 2 h; there are often associated symptoms of homolateral lacrimation, reddening of the eye, nasal stuffiness, lid ptosis, and nausea. Alcohol provokes attacks in about 70% of patients but ceases to be provocative when the bout remits; this on-off vulnerability to alcohol is pathognomonic of cluster headache. Only rarely do foods or emotional factors precipitate pain, in contrast to migraine.
There is a striking periodicity of attacks in at least 85% of patients. At least one of the daily attacks of pain recurs at about the same hour each day for the duration of a cluster bout. Onset is nocturnal in about 50% of the cases, and then the pain usually awakens the patient within 2 h of falling asleep.
Pathogenesis No consistent cerebral blood flow changes accompany attacks of pain. Perhaps the strongest evidence for a central mechanism is the periodicity of attacks; the existence of a central mechanism is also suggested by the observation that autonomic symptoms that accompany the pain are bilateral and are more severe on the painful side. The hypothalamus may be the site of activation in this disorder. The posterior hypothalamus contains cells that regulate autonomic functions, and the anterior hypothalamus contains cells (in the suprachiasmatic nuclei) that constitute the principal circadian pacemaker in mammals. Activation of both is necessary to explain the symptoms of cluster headache. The pacemaker is modulated via serotonergic dorsal raphe projections. It can be concluded tentatively that both migraine and cluster headache result from abnormal serotonergic neurotransmission, albeit at different loci.
TREATMENT
The most satisfactory treatment is the administration of drugs to prevent cluster attacks until the bout is over. Effective prophylactic drugs are prednisone, lithium, methysergide, ergotamine, sodium valproate, and verapamil. Lithium (600 to 900 mg daily) appears to be particularly useful for the chronic form of the disorder. A 10-day course of prednisone, beginning at 60 mg daily for 7 days followed by a rapid taper, may interrupt the pain bout for many patients. When ergotamine is used, it is most effective when given 1 to 2 h before an expected attack. Patients must be educated regarding the early symptoms of ergotism when ergotamine is used daily; a weekly limit of 14 mg should be adhered to.
For the attacks themselves, oxygen inhalation (9 L/min via a loose mask) is the most effective modality; 15 min of inhalation of 100% oxygen is often necessary. Sumatriptan, 6 mg subcutaneously, will usually shorten an attack to 10 to 15 min.
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