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Title: Botulinum Toxin in the Treatment of Chronic Pain and Headaches Author: mauskops Last modified by: nn Created Date: 7/5/2000 10:04:18 PM Document presentation ... – PowerPoint PPT presentation

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Title: Advances in Migraine


1
Advances in Migraine
New York Headache Center
  • Alexander Mauskop, MD

2
Potential Conflict of Interest Disclosure
  • Allergan Pozen
  • AstraZeneca Procter Gamble
  • Bristol-Myers Squibb PR Osteo
  • Elan Royal Numico/GNC
  • GlaxoSmithKline UCB Pharma
  • Merck Weber Weber
  • Novartis Winston Laboratories
  • Ortho-McNeil Wyeth
  • Pfizer

3
News in Migraine
  • Pathophysiology
  • CGRP antagonists
  • PFO
  • Classification
  • Basilar migraine
  • Chronic migraine
  • Magnesium
  • Botulinum toxin

4
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7
Impact of Migraine onQuality of Life
Adapted from Solomon GD et al. Headache
199434(3)143-147
8
Migraine Is a NeurovascularDisorder
  • The genesis of migraine is neurologic
  • Likely that hyperexcitability of CNS confers
    susceptibility to migraine attacks
  • Migraine associated with regional reduction in
    cerebral blood flow and cortical spreading
    depression (CSD)
  • Trigeminovascular system involved in production
    of migraine pain

Aurora SK, Welch KMA. Curr Opin Neurol.
199811205-209 Aurora SK, Welch KMA. Curr Opin
Neurol. 200013273-276.
9
Cause of Migraines
  • A single gene is responsible for familial
    hemiplegic migraine
  • Common migraine is polygenetic, which accounts
    for its variable expression
  • Multiple triggers modify the frequency and the
    severity of attacks

10
Neuronal Hyperexcitabilityin Migraine
  • Neuronal hyperexcitability predisposes
    individuals to migraine
  • Migraine patients visualized phosphenes following
    transcranial magnetic stimulation
  • Increased neuronal hyperexcitability may be
    multifactorial
  • Abnormal calcium channels that influence
    presynaptic neurotransmitter release
  • Abnormal glutamate metabolism
  • Deficiency of systemic and brain magnesium
  • Migraine may be prevented by reducing neuronal
    hyperexcitability
  • Inhibition of excitatory neurotransmission (eg,
    Na channel)
  • Enhancement of inhibitory neurotransmission (eg,
    GABA)

Welch, et al. Neurol Clin. 19908817-828 Aurora
SK, Welch KMA. Curr Opin Neurol. 199811205-209
Cutrer, et al. Cephalalgia. 19971793-100.
11
Early Intervention May PreventCentral
Sensitization
  • Clinical experience suggest that migraineurs are
    most-responsive to medications within the initial
    30-60 minutes of an attack.
  • The development of central hypersensitivity
    points to the need for the early use of
    anti-migraine drugs.

12
Benefits of Early Treatment
  • Early pain-free response
  • Less recurrence
  • Prevents progression of attack
  • Less disability
  • Less need for multiple doses and rescue meds
  • Effective early treatment may prevent chronic
    migraine

13
Migraine Is Often Overlooked
  • Sinus headache is the most common misdiagnosis
  • Symptoms include
  • Dull ache located near the nose
  • Pressure in the sinus cavities
  • Thick, colored nasal discharge
  • OTCs can sometimes relieve the pain

Cady et al. Headache Free. 199336-38.
14
Migraine Is Often Overlooked
  • Sinus headache is the most common
    misdiagnosis
  • Symptoms include
  • Dull ache located near the nose
  • Pressure in the sinus cavities
  • Thick, colored nasal discharge
  • OTCs can sometimes relieve the pain

15
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16
Caffeine-containing Drugs
Rx
  • Cafergot
  • Wigraine
  • Esgic
  • Fiorinal
  • Fioricet
  • Norgesic
  • Synalgos DC

17
Caffeine-Containing Drugs
OTC
  • Anacin
  • Anacin Maximum Strength
  • Aspirin Free Excedrin
  • Excedrin Extra Strength
  • Excedrin Migraine
  • Maximum Strength Midol

18
Caffeine
The analgesic effects of caffeine in
headache (Ward et al., Pain 1990)
Caffeine (65 mg and 130 mg) equals to 650 mgof
acetaminophen
19
Caffeine
235 mg (2.5 cups) a day
  • 52 moderate or severe headache
  • 11 depression
  • 11 low vigor
  • 8 anxiety
  • 8 fatigue

Withdrawal syndrome after the double-blind
cessation of caffeine consumption.
(Silverman et al. NEJM 1992)
20

Magnesium and Migraine
Low brain magnesium in migraine N.M. Ramadan, H.
Halvorson, A. Vande-Linde et al. Headache
198929590-593.
21
Magnesium and Migraine
Oral magnesium load test in patients with
migraine
  • Trauninger et al. Headache 42114-1192002
  • Conclusions
  • Magnesium retention occurs in patients with
    migraine
  • after oral loading, suggesting a systemic
    magnesium
  • deficiency

22
Magnesium
Known effects of IMg2
  • glutamate
  • angiotensin II
  • potassium
  • serotonin
  • G proteins

acetylcholine nitric oxide norepinephrine calcium
enzyme complexes (325)
23
NMDA (N-Methyl-D-Aspartate)Receptor Complex
Ca2
Mg2
Zn GLY
Ca2
PCP MK801
NMDA
Mg2
TCA
24
Magnesium and Migraine
Potential causes of magnesium deficiency
  • Stress
  • Alcohol and caffeine
  • Genetics
  • Low dietary intake
  • Gastro-intestinal disorders
  • Chronic illness

25
IV MgSO4 for Acute Migraine
A. Mauskop et al, Clin Science 199589633-6
26
IV MgSO4 forCluster Headaches
x
0.76
x
0.60 0.58 0.56 0.54 0.52 0.50 0.48 0.46 0.44
o
x
x
o
x non-responders
o
xxx
o
xxx
o responders
ooo
xxx
IMg2 mmol/L
oooo
o
x
o
x
ooo
o
o
oo
Mauskop et al, Headache 199535597-600.
o
o
27

Magnesium and Migraine
Magnesium prophylaxis of menstrual
migraine Effects on intracellular magnesium.
F. Facchinetti, G. Sances, A.R. Genazzani, G.
Nappi. Cephalagia 1996 16257-263.
Magnesium pyrrolidone carboxylic acid 360 mg
Days with migraine reduced 4.7 to 2.4
(plt0.01) Significant reduction in MDQ scores
(plt0.05)
28

Magnesium and Migraine
Prophylaxis of migraine with oral magnesium
results from a prospective, multicenter,
placebo-controlled and double-blind randomized
study.
A. Peikert, C. Wilimzig, R. Kohne-Volland,
Cephalagia1996 16257-263.
Trimagnesium dicitrate 600 mg
Attack frequency reduced 41.6 vs
15.8 (plt0.05) Days with migraine reduced 52.3
vs 19.5 (plt0.05)
29

Magnesium and Migraine
Oral magnesium oxide prophylaxis of frequent
childhood migraine
Wang F, Van Den Eeden S, Ackerson L, et
al.Cephalagia 200020424 (abstract).
30

Magnesium and Migraine
Magnesium in the prophylaxis of migraine A
double-blind, placebo-controlled study.
Pfaffenrath V, Wessely P, Meyer C, et
al.Cephalagia 1996 16436-440.
31

Effectiveness of High-dose Riboflavin in Migraine
Prophylaxis
4
No. of Attacks per Month
3
Placebo Riboflavin P0.001
2


1
1
2
3
4
Month
J. Shoenen, J. Jacquy, M. Lenaerts. Neurology
1998 50466-440.
32
Botanical Remedies
Feverfew
Randomized double-blind placebo-controlled
trialof feverfew in migraine prevention.
Murphy JJ, Heptinsall S, Mitchell JRA. The
Lancet, 23 July 1988, pp 189-192.
33
Feverfew
Results
  • Reduction in mean number of attacks 3.6 vs 4.7
    (plt0.005)
  • Global assessment of improvement on VAS 74 vs
    60 (plt0.0001)
  • Reduced severity of nausea and vomiting (plt0.02)
  • Tendency toward milder intensity of pain
  • No effect on duration of attacks

34
Natural Remedies
The Case for Multi-Agent Therapies
  • Migraine is a multifactorial disease
  • Any single pharmacologic agent hasno more than
    60 efficacy
  • Single nutraceutical therapies may haveno more
    than 50 efficacy

35
Natural Remedies
Possible Combinations
  • Migra-Lieve

Riboflavin 400 mg Magnesium 300 mg Feverfew 100 mg
36
Petasites hybridus
Possible mechanisms of action
  • Inhibits constriction of smooth muscle
    preparation induced by acetylcholine, histamine
    and potassium chloride
  • Inhibits leukotriene synthesis

37
Botanical Remedies
  • Aromatherapy
  • Topical preparations
  • Oral preparations

38
Botanical remedies
Effect of Peppermint andEucalyptus Oil
  • Double-blind, placebo-controlled,
    randomizedcross-over design
  • 32 healthy subjects
  • Parameters tested
  • EMG activity
  • Exteroceptive suppression periods
  • Contingent negative variation
  • Sensitivity to experimental pain
  • Current mood states

39
Results

Combination of Peppermint Oiland Ethanol
  • Analgesic effect
  • Muscle relaxing effect
  • Mentally relaxing effect

40
Natural Remedies
What to recommend?
  • Aerobic exercise, neck exercise
  • Biofeedback / relaxation
  • Magnesium, riboflavin, feverfew
  • Acupuncture
  • Massage, shiatsu, reflexology
  • Dietary approaches

41
Candidates for Preventive Therapy
  • Disabling primary headaches
  • Chronic migraine
  • Frequent migraine
  • Chronic tension-type headache
  • Medication overuse (drug-induced headache)
  • Headaches refractory to routine treatment
  • Contraindication to acute therapy

42
Currently Used Preventive Therapies
  • Migraine Tension-type
  • Beta-blockers X
  • Antidepressants X X
  • Anticonvulsants X
  • Calcium channel blockers X
  • Methysergide X
  • NSAIDs X X
  • Muscle relaxants X

43
Potential Side Effects of Prophylactic Drugs
  • Beta-blockers fatigue, dizziness, depression
  • Antidepressants dry mouth, drowsiness, weight
    gain, constipation, sexual dysfunction
  • Anticonvulsants weight gain, cognitive
    dysfunction, drowsiness, fatigue, constipation
  • Calcium channel blockers constipation, edema
  • Methysergide fibrosis, water retention, leg
    cramps
  • NSAIDs dyspepsia, peptic ulcers, renal disease
  • Muscle relaxants sedation, dizziness

44
Prophylactic DrugsAdditional Drawbacks
  • Work in minority of patients
  • Compliance
  • Fear of adverse events
  • Drug-drug interactions

45
History of BTX-A Usein Migraine
  • Anecdotal reports of reduced migraines from
    patients receiving BTX-A treatment for other
    indications
  • A retrospective review of patient charts
    suggested migraine relief was associated with
    certain injection sites
  • This information was used in designing early
    clinical studies

46
The Neuromuscular Junction
47
Botulinum Toxin Type A Mechanism of Action
Current Hypothesis
48
Botulinum Toxin Type A Migraine Headache Study
  • Binder WJ, et al. Otolaryngol
  • Head Neck Surg 2000123669-676
  • Open-label study
  • Dx Migraine
  • N77
  • Variable dose
  • Outcome measure
  • Complete response
  • Partial response
  • No response

49
Botulinum Toxin Type A for Migraine Headache
  • Silberstein S, et al. Headache. 200040445-450.
  • Double-blind, vehicle-controlled study
  • Dx Migraine (N123)
  • Placebo (n41)
  • 25 U botulinum toxin type A (n42)
  • 75 U botulinum toxin type A (n40)
  • 3-month duration
  • Outcome measure
  • Reduction in migraine severity

50
BTX-A Injection Sites Fixed Sites, Fixed Dose
(Bilateral)
  • Frontalis Glabellar

Temporalis
51
Proof-of-Concept Studies
  • Two double-blind, vehicle-controlled studies
  • 1-month baseline period, treatment, 3-4 month
    follow-up
  • Study 1 (N123)
  • 2-8 moderate to severe migraines/month at
    baseline
  • Vehicle (n 41) 25 U BTX-A (BOTOX n 42) 75
    U BTX-A (n 40)
  • Study 2 (N418)
  • 4-8 moderate to severe migraines/month at
    baseline
  • Vehicle (n 106) 7.5 U BTX-A (n 105) 25 U
    BTX-A (n 101) 50 U BTX-A (n 106)

52
Botulinum Toxin Type Afor Migraine Silberstein
S, et al.
P lt.042 vs vehicle
53
Study 2
54
Safety Summary
  • BTX-A was well tolerated
  • All treatment-related adverse events were local
    and transient
  • Most common were
  • Blepharoptosis
  • Injection site weakness
  • Skin tightness
  • There were no serious treatment-related adverse
    events

55
Summary of Development Studies
  • Results of initial studies using frontal
    injections are not definitive
  • Improvement from baseline in migraine frequency
    and acute medication use in one study
  • Patients perceived significant global improvement
    in both studies
  • Safe and well tolerated in both studies
  • Future studies should employ alternative
    treatment approaches

56
Injection Sites Glabellar andFrontal Regions
X
X
X
X
X
X
X
X
X
57
Injection SiteTemporalis Muscle
X
X
X
X
58
Injection SiteSuboccipital Region
Trapezius muscle
Splenius capitismuscle
X
X
X
Adapted with permission from Netter FH. Atlas of
Human Anatomy. Icon Learning Systems Teterboro,
NJ. 1997.
59
Injection SiteOccipitalis Muscle
X
X
60
Botulinum Toxin Type A Cost in Migraines
  • M. Blumenfeld, Impact of Botulinum Toxin Type-A
    Treatemnt on Medication Costs and Usage in
    Difficult-to-Treat Chronic Headache Case
    Studies.
  • Headache Quarterly 200213(1)241-244.
  • BTX-A-induced decreases in the frequency and/pr
    severity of chronic headaches led to decreased
    headache medication costs. A reduction in ED and
    office visits may provide further savings.
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