Papers

Prophylactic treatment of migraine with angiotensin converting enzyme inhibitor (lisinopril): randomised, placebo controlled, crossover study

Harald Schrader, professor of neurology, Lars Jacob Stovner, professor of neurology, Grethe Helde, research assistant, Trond Sand, professor of clinical neurophysiology, Gunnar Bovim, professor of neurology. 

Norwegian University of Science and Technology, Department of Neurology, 7006 Trondheim, Norway

Correspondence to: H Schrader harald.schrader{at}medisin.ntnu.no

	Abstract

Top Abstract Introduction Participants and methods Results Discussion References

Objective: To determine the efficacy of an angiotensin converting enzyme inhibitor in the prophylaxis of migraine.
Design: Double blind, placebo controlled, crossover study.
Setting: Neurological outpatient clinic.
Participants: Sixty patients aged 19-59 years with migraine with two to six episodes a month.
Interventions: Treatment period of 12 weeks with one 10 mg lisinopril tablet once daily for one week then two 10 mg lisinopril tablets once daily for 11 weeks, followed by a two week wash out period. Second treatment period of one placebo tablet once daily for one week and then two placebo tablets for 11 weeks. Thirty participants followed this schedule, and 30 received placebo followed by lisinopril.
Main outcome measures: Primary end points: number of hours with headache, number of days with headache, number of days with migraine. Secondary end points: headache severity index, use of drugs for symptomatic relief, quality of life and number of days taken as sick leave, acceptability of treatment.
Results: In the 47 participants with complete data, hours with headache, days with headache, days with migraine, and headache severity index were significantly reduced by 20% (95% confidence interval 5% to 36%), 17% (5% to 30%), 21% (9% to 34%), and 20% (3% to 37%), respectively, with lisinopril compared with placebo. Days with migraine were fewer by at least 50% in 14 participants for active treatment versus placebo. Intention to treat analysis of data from 55 patients supported the differences in favour of lisinopril for the primary end points.
Conclusion: The angiotensin converting enzyme inhibitor, lisinopril, has a clinically important prophylactic effect in migraine.

	Introduction

Top Abstract Introduction Participants and methods Results Discussion References

Despite treatment of symptomatic migraine with triptans many patients experience only partial relief of symptoms. Furthermore, about 30-40% do not respond, and in some, triptans induce headache. For these patients and for those who do not respond to non-specific treatments, prophylactic drugs are indicated for people who experience two or more attacks a month. Some  blockers, the anti-epileptic drug sodium valproate, the 5-hydroxytryptamine receptor antagonists pizotifen and methysergide, flunarizine, and several non-steroidal anti-inflammatory drugs have shown some prophylactic effect. Most of the recommended drugs, however, cause adverse events that preclude long term treatment. Thus, there is a need for new prophylactic drugs that have greater efficacy and are better tolerated.

We had observed an impressive improvement in migraine in a patient treated with lisinopril for hypertension. This effect has already been described in a case series.¹ Furthermore, we had obtained anecdotal evidence for the efficacy of lisinopril in 10 women who had migraine, eight of whom reported fewer attacks during treatment. We carried out a randomised, double blind, placebo controlled, crossover study to investigate the prophylactic effect of the angiotensin converting enzyme inhibitor lisinopril.

	Participants and methods

Top Abstract Introduction Participants and methods Results Discussion References

The study followed the guidelines recommended by the International Headache Society's committee on clinical trials in migraine² and was carried out between April 1998 and December 1999. Of the 60 randomised patients, 35 were recruited from an outpatient clinic and 25 responded to advertisements in a local newspaper.

Inclusion criteria were diagnosis of migraine with and without aura according to the criteria of the International Headache Society,³ men and women aged between 18 and 60 years, presence of migraine for more than a year, onset of migraine before the age of 50 years, and attacks of migraine occurring two to six times a month. Exclusion criteria were interval headache that the patient was unable to differentiate from migraine, use of prophylactic drugs for migraine in the four weeks before randomisation, pregnancy or inability to use contraceptives, decreased renal or hepatic function, hypersensitivity to angiotensin converting enzyme inhibitors, history of angioneurotic oedema, and psychiatric disorder. The study was performed in accordance with the Declaration of Helsinki. The study protocol was approved by the regional ethics committee for medical research, and all patients gave written, informed consent before enrolment.

Study design
The design is reported in the longer version of this paper on the BMJ 's website. After a four week placebo run-in period to verify the frequency of attacks, patients were randomly allocated to take one tablet daily containing either 10 mg lisinopril (active) or placebo (inactive).

View larger version (32K): [in this window] [in a new window]   Trial profile in study of prophylactic treatment of migraine with lisinopril

Statistical analysis
We used the Wilcoxon signed rank test to compare end point variables. For comparison of adverse events and acceptability we used a McNemar's matched pairs test. A two-sided P<0.05 was considered significant. A paired study including 55 subjects will have about 80% power to detect a group mean difference of 0.5 SD (with Student's t test).⁵

	Results

Top Abstract Introduction Participants and methods Results Discussion References

Participants
Of the 60 patients who were randomised, three withdrew from the study because of adverse events (fatigue, dizziness and fatigue, exanthema, and monarthritis), one declined to continue, and one had an inadequate response on placebo (see figure). Eight patients did not comply with treatment but kept a diary for the whole study period. The 47 remaining participants (38 women, mean (SD) age 41 (9) years; nine men, 43 (5) years) provided complete data for final evaluation of efficacy. Table 1 shows the adverse events in the 60 randomised patients.

Outcomes
There was a significant difference in favour of lisinopril for hours with headache, number of days with headache, number of days with migraine, and headache severity index (table 2). There was a reduction of at least 50% in symptoms in 14 (30%) participants for days with migraine and 15 (32%) for headache severity index during lisinopril compared with placebo treatment. In the intention to treat analysis in 55 patients, significant differences were retained for the primary efficacy end points (table 3).

	Discussion

Top Abstract Introduction Participants and methods Results Discussion References

Our results show that lisinopril has a clinically relevant prophylactic effect in migraine. Compared with the placebo period, there was a reduction of about 20% in primary efficacy parameters during lisinopril treatment. A comparison of the effect of lisinopril with those reported for other prophylactic drugs for migraine is difficult because of differences in study designs and ways of reporting results.⁶ A meta-analysis of the effect of propranolol 160 mg indicated an improvement of 33% with regard to the headache index on active medication compared with placebo, but this analysis included both open and controlled studies.⁷ For this parameter we saw an improvement of 20%, and we consider this to be a promising result in a study performed with an up to date and robust methodological design. To assess the relative efficacy, safety, and tolerability of different drugs reliably, however, only direct comparisons in a single study are valid.

Study strengths
The main strength of our study is that it was performed according to the guidelines for controlled trials of drugs in migraine.² We chose the crossover design for this single centre study because fewer patients were needed than for a parallel group design. There are known disadvantages of the crossover design,⁸ but we found no period effect and no carry over effect. The drop out rate was low (8%), despite the relatively long duration of the study (31 weeks).

Why it might work
Lisinopril has various pharmacological effects that may be relevant in migraine. In addition to blocking the conversion of angiotensin I to angiotensin II, it also alters sympathetic activity, inhibits free radical activity, increases prostacyclin synthesis,⁹ and blocks the degradation of bradykinin, encephalin, and substance P.¹⁰ Of great relevance may be the recent finding that migraine without aura seems to be more common in people with the angiotensin converting enzyme DD gene, and migraineurs with this gene also have higher angiotensin converting enzyme activity and a higher frequency of attacks than other migraine sufferers.¹¹

Safety and tolerability
Lisinopril was well tolerated, as can be seen from the acceptability and the quality of life scores, and the adverse events observed in this study were those known to be associated with angiotensin converting enzyme inhibitors.¹² Symptoms associated with hypotension (dizziness and tendency to faint) may be minimised by reducing the intake of lisinopril to its lowest effective dose. Cough, a side effect not related to dose, was severe enough to prohibit further use in three patients.

	Acknowledgments

   Contributors: HS had the original idea for the study and is the guarantor. HS and LJS were the principal investigators and designed the protocol, assessed the patients, and wrote the manuscript. GH assisted in the design of the study, recruitment of the patients, and data collection and analysis. TS helped to draw up the protocol and participated in the statistical analysis. TS and GH contributed to the revision of the manuscript. GB participated in planning the study, assessment of patients, and revision of the manuscript. He also advised on the study design and the statistical analysis. The database was managed by the investigators who performed the statistical analyses of the data.

	Footnotes

Funding: AstraZeneca provided the computer generated randomisation scheme, study medication, and financial support.

Competing interests: HS and GB have been reimbursed by AstraZeneca, one of the manufacturers of lisinopril, for attending conferences. These conferences were unrelated to the present study.

The full version of this paper appears on the BMJ's website

	References

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(Accepted 9 October 2000)