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The Use of Cannabinoids in Pain

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Title: The Use of Cannabinoids in Pain

1
The Use of Cannabinoids in Pain

Allan Gordon MD
Neurologist and Director
Wasser Pain Management Centre
Mount Sinai Hospital

2
Pot eases peripheral neuropathy pain, U.S. study
shows

SAN FRANCISCO Smoking marijuana eased
HIV-related pain in some patients in a small
study that nevertheless represented one of the
few rigorous attempts to find out if the drug has
medicinal benefits.
The Office of National Drug Control Policy, part
of the administration of President George W.
Bush, quickly sought to shoot holes in the
experiment.
The study, conducted at San Francisco General
Hospital from 2003 to 2005 and published Monday
in the journal Neurology, involved 50 patients
suffering from HIV-related foot pain known as
peripheral neuropathy. There are no drugs
specifically approved to treat that kind of pain.

Three times daily for nearly a week, the patients
smoked marijuana cigarettes machine-rolled at the
National Institute of Drug Abuse, the only legal
source for the drug recognized by the federal
government.
Half the patients received marijuana, while the
other 25 received placebo cigarettes that lacked
the drug's active ingredient, tetrahydrocannabinol
.
Scientists said the study was the first one
published that used a comparison group, which is
generally considered the gold standard for
scientific research.

Abrams DI, Jay CA, Shade SB, Vizoso H, Reda H,
Press S, Kelly ME, Rowbotham MC, Petersen
KL.Related Articles, Links Cannabis in painful
HIV-associated sensory neuropathy a randomized
placebo-controlled trial.Neurology. 2007 Feb
1368(7)515-21.

Fifty patients completed the entire trial.
Smoked cannabis reduced daily pain by 34
Greater than 30 reduction in pain was reported
by 52 in the cannabis group and by 24 in the
placebo group .
The first cannabis cigarette reduced chronic pain
by a median of 72 vs 15 with placebo .
Cannabis reduced experimentally induced
hyperalgesia to both brush and von Frey hair
stimuli but appeared to have little effect on the
painfulness of noxious heat stimulation.

6
Rationale for Cannabis-Derived Drugs

A Canadian survey of patients with neuropathic
pain found that 73 suffer from inadequate pain
control (Gilron Bailey, Can J Anaesth, 2003)
While there are some effective treatments for
neuropathic pain of peripheral origin there are
relatively few treatments for central neuropathic
pain
An estimated 15 of people with MS use cannabis
for symptom relief (Clark et al., Neurol, 2004)

7
Epidemiology of medical use of cannabis

2 of Canadian population use cannabis for
medical purposes (Ogborne 2000)
Prospective prevalence studies done in
HIV/AIDS 25 (Sidney 2001, Prentiss 2004)
MS 15 (Clark et al 2004, Page et al 2003)
CNCP 10 (Ware et al 2003)

8
Cannabis use by patients with IBDSimon Lal,
Manijeh Ryan, Sabrina Tangri, Mark S Silverberg,
Allan Gordon, A Hillary Steinhart. APS April
2007

100 patients with ulcerative colitis (UC mean
age 33 (range 18-80) 66 female) and 191 patients
with Crohns disease (CD mean age 33.5 (range
18-71) 105 female) attending the outpatient
clinic
Completed a questionnaire concerning current and
previous cannabis use, socio-economic factors,
disease history, and medication use and QOL.

A comparable proportion of UC and CD patients
reported lifetime (51) UC vs. (48) CD or
current (12) UC vs. (16) CD use of cannabis.
For lifetime cannabis users
14/43 (33) UC and 40/80 (50) CD patients had
used it to relieve IBD-related symptoms
including
abdominal pain 93 UC vs. 95 CD
diarrhea 64 UC vs. 23 CD and
reduced appetite 86 UC vs. 70 CD).

Patients were more likely to use cannabis for
symptom relief if
they had a history of abdominal surgery (29/48
(60) vs. 24/74 (32) p0.002),
chronic analgesic use 29/41 (71) vs. 25/81 (31)
alternative/complimentary medicine use 36/66
(55) vs. 18/56 (32)
a lower IBDQ (QOL) score

11
Ware et al. Pain Res Manage 20027(2)95-99
12
Applications received per month for Authorization
to Possess under the Medical Marijuana Access
Regulations December 2005
http//www.hc-sc.gc.ca/dhp-mps/marihuana/stat/2005
/dec_e.html
13
COMPASS Study

Multicentre, open label study of herbal cannabis
in patients with chronic non-cancer pain
500 patients 1500 Control
In progress

14
Observations

People get high on marijuana even when given
therapeutically
May affect QOL, sleep rather than pain
Large drop out rate in Toronto group
Requires rigorous management

15
Therapeutic options

Nabilone (Cesamet)
Dronabinol (Marinol)
Cannabis-based medicine (Sativex)
Herbal cannabis (MMAR)

16
Synthetic THC Oral Cannabinoids

Narcotics prescription
Nausea, vomiting with chemotherapy, anorexia
associated with HIV/AIDS
Cesamet (Nabilone) (0.5, 1 mg)
purified synthetic cannabinoid
nitrogen analogue to THC
T1/2 8-12 hrs
Marinol (dronabinol) (2.5, 5 mg)
Delta-9-THC
T1/2 4-6 hrs
metabolites long T1/2

17
Molecular Structure?9-THC vs Nabilone
18
Rx Cannabinoid Profile Summary
19
Recent RCT results MS
20
Cannabinoids in MS
21
Cannabinoids and Pain Pathways
Adapted from Di Marzo 2001
22
THCCBD 11

Extracts of 2 Cannabis sativa L strains
Equal amounts of
Tetranabinex high-THC strain
27 mg/mL ?-9 THC
Nabidiolex high-CBD strain
25 mg/mL CBD
Buccal spray
Ethanol/propylene glycol vehicle
2.7 mg THC and 2.5 mg CBD per spray
Therapeutic dose
High inter-patient variability
Administered on self-titration regimen

23
Pharmacokinetics Cannabis
Cannabis clinical effects by route of
administration compared with THCCBD 11
Grotenhermen F (2003), Sativex Product Monograph
(2005)
24
Clinical Review Rog et al, 2005

Objective
Compare efficacy and tolerability of THCCBD 11
with placebo
Adjunctive therapy in central neuropathic pain
Patient population
Adult MS patients with central pain
Dysesthesia, painful spasm
85 screened
66 randomized
THCCBD 11 (n34) and placebo (n32)

25
Clinical Review Rog et al, 2005
Study design
26
Clinical Review Rog et al, 2005

Method
Continuation of existing analgesics
Self-titration of study medication to maximum 48
sprays daily
11-point numerical rating scale (NRS-11) to
measure pain and sleep disturbance
Randomization
Placebo and treatment groups comparable
Patient disposition
64 patients completed study
2 patients withdrew from treatment group
Mean daily sprays
THCCBD 11 9.6
Placebo 19.1
Outcomes
Primary Change in neuropathic pain severity
(NRS-11)
Secondary Change in sleep disturbance due to
pain (NRS-11)
Patients global impression of change (PGIC)

27
Clinical Review Rog et al, 2005
Pain scores at end of randomized treatment phase
7.00
p 0.005
6.00
N 34
N 32
5.00
N 32
4.00
Mean NRS-11 pain score
N 32
3.00
2.00
1.00
0.00
Baseline
On treatment
Scale 0 No pain 10 Worst possible pain
THCCBD 11
Placebo
Active vs placebo
28
Clinical Review Rog et al, 2005
Sleep scores at end of randomized treatment phase
6.00
5.00
p 0.003
N 34
4.00
N 32
N 32
Mean NRS-11 sleep score
3.00
2.00
N 32
1.00
0.00
Baseline
On treatment
Scale 0 Did not disrupt sleep 10 Completely
disrupts sleep, unable to sleep due to pain
THCCBD 11
Placebo
Active vs placebo
29
Clinical Review Rog et al, 2005
Patients global impression of change
30
25
20
Number of patients
15
10
5
0
No change
Much worse
Total improved
Much improved
Total worsened
Minimally worse
Very much worse
Minimally improved
Very much improved
Category
THCCBD 11
Placebo
P0.005 vs placebo
30
Clinical Review Rog et al, 2005
31
Clinical Review Rog et al, 2005

Summary
THCCBD 11 effectiveness demonstrated
Central pain associated with MS
Pain-related sleep disturbance
Adjunctive analgesic
Study provided additional comparative data for
NPS vs traditional NRS used for pain measurement

32
Recent studies