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Since 1971 British doctors have been barred
from prescribing cannabis under the Misuse of Drugs Act. Many
otherwise law abiding people have subsequently thought it
worthwhile to expose themselves to the risk, inconvenience,
and expense of obtaining illegally a drug they believe can
ease symptoms inadequately controlled by conventional
medicines. Patients have told me how effective cannabis can
be in relieving aches and pains, numbing the symptoms of
opiate withdrawal, improving sleep, reducing anxiety, and
alleviating the vomiting, anorexia, and depression associated
with AIDS related disorders. Anecdotes such as these are all
very well, but is there any scientific evidence that cannabis
has real therapeutic value?
The BMA has addressed this question with an excellent
report, which begins by reviewing the pharmacology.
1
Only a few of the 60 or so chemicals unique
to
Cannabis sativa (cannabinoids) have so far been
studied, the best known of which is the main psychoactive
ingredient, delta-9-tetrahydrocannabinol (THC). Specific
cannabinoid receptors in the brain and in spleen macrophages,
and naturally occurring substances which bind to these
(anandamides), have been identified in recent years. These
findings open the door to developing novel agents for
therapeutic use or exploring the physiological role of the
anandamide system -- which may be concerned with mood, memory
and cognition, perception, movement, coordination, sleep,
thermoregulation, appetite, and immune response.
2
The report evaluates the scientific literature on cannabis
and cannabinoids in relation to the strengths and
shortcomings of existing medicines and proposes directions
for research. The strongest evidence relates to the
effectiveness of delta-9-tetrahydrocannabinol and the
synthetic cannabinoid nabilone in relieving nausea and
vomiting secondary to cancer chemotherapy. Nabilone is
licensed for this use in Britain, but
delta-9-tetrahydrocannabinol (as dronabinol) is not. A pilot
study suggests that the non-psychotropic
delta-8-tetrahydrocannabinol has promise as an antiemetic in
children.
3
Proposals for research contained in this section are
applicable to most of the others: exploration of optimal
regimens and the relative usefulness of different
cannabinoids; controlled comparisons with newer medicines
alone and as adjunctive therapy; specification of patient
categories; and a focus on other conditions producing similar
symptoms.
Many anecdotal accounts indicate that cannabis and some
cannabinoids can relieve symptoms related to muscle
spasticity, but the few controlled studies offer only modest
support for this. Good evidence exists from basic research
that several cannabinoids have analgesic and
anti-inflammatory properties, but eight small scale human
studies listed here give equivocal results. Again animal
studies suggest that cannabidiol has possibilities as an
anticonvulsant, but the human data are lacking.
Delta-9-Tetrahydrocannabinol definitely reduces intraocular
pressure and produces bronchodilatation but its potential in
glaucoma and asthma is not compelling on current
evidence.
Relief of symptoms in AIDS related disorders is one of the
most interesting possibilities. The appetite stimulating
effect of oral dronabinol in patients with AIDS
4
was convincing enough to win approval from the American
Food and Drug Administration for this indication. This
attribute, combined with antiemetic and possible analgesic,
anxiolytic,
5
hypnotic,
6
and antidepressant
7
properties, suggests a profile uniquely relevant to this
condition and a compelling reason for research.
Adverse effects relevant to clinical use are discussed. No
deaths have been attributed to cannabis toxicity alone.
Common acute effects include sedation; psychological symptoms
(euphoria, anxiety, paranoia, impaired memory); and physical
symptoms such as dry mouth, ataxia, blurred vision, weakness
and incoordination, and tachycardia. Impaired psychomotor
performance may persist as long as 24 hours after
a single dose. Interactions with central nervous system
depressants are possible, as is aggravation or precipitation
of psychosis in vulnerable individuals. Physical and
psychological dependence can occur, but withdrawal symptoms
are usually mild. Inconsistent effects on sex hormones and
immunosuppression in animals have been reported. Cannabis
smoke is as rich in toxic gases and particulates as tobacco
smoke, so regular heavy smokers probably face an increased
risk of cardiovascular and respiratory diseases.
The report concludes that individual cannabinoids have a
therapeutic potential in several conditions in which other
treatments are not fully adequate and that they are safe
drugs with a side effect profile better than that of many
drugs used for the same indications. The BMA recommends that
the government should amend the Misuse of Drugs Act to allow
cannabinoids to be prescribed in a range of medical
conditions, calls for the setting up of controlled clinical
trials, and suggests that pharmaceutical companies should
search for novel analogues to open up new therapeutic
possibilities.
The BMA is not alone in arguing for enhanced access to
cannabinoids in clinical practice. Others include the Royal
Pharmaceutical Society,
8
the previous president of the Royal College of
Physicians (L Turnberg, personal communication), and many
British doctors.
9
The role of cannabinoids in modern therapeutics remains
uncertain, but the evidence in this report shows that it
would be irrational not to explore it. The active components
of a plant which has been prized as a medicine for thousands
of years should not be discarded lightly, and certainly not
through political expediency or as a casualty of the war on
drugs.
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British Medical Association.
Therapeutic uses of cannabis. Amsterdam: Harwood
Academic , 1997.
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Pertwee RG. Pharmacological, physiological and
clinical implications of the discovery of cannabinoid
receptors: an overview. In: Pertwee R, ed.
Cannabinoid receptors. London: Harcourt Brace ,
1995.
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Abrahamov A, Abrahamov A, Mechoulam R. An efficient
new cannabinoid antiemetic in pediatric oncology.
Life Sciences 1995; 56: 2097-2102.
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Beal JE, Olson R, Lauberstein L, Morales JO, Bellman
P, Yangco B, et al. Dronabinol as a treatment for
anorexia associated with weight loss in patients with
AIDS.
Journal of Pain and Symptom Management 1995; 10:
89-97.
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Fabre LF, McLendon D. The efficacy and safety of
nabilone (a synthetic cannabinoid) in the treatment of
anxiety.
J Clin Pharmacol 1981; 21: 377-382S.
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Carlini EA, Cunha JM. Hypnotic and anti-epileptic
effects of cannabidiol.
J Clin Pharmacol 1981; 21: 417-427.
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Regelson W, Butler JR, Schulz J, Kirk T, Peel L, Gleem
ML, et al. Delta-9-THC as an effective antidepressant and
appetite-stimulating agent in advanced cancer patients.
In: Braude MC, Szara S, eds.
The pharmacology of marihuana. New York: Raven
Press , 1976.
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Gray C. Cannabis: the therapeutic potential.
Pharmaceutical J 1995; 254: 771-773.
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Meek C. Doctors want cannabis prescriptions
allowed.
BMA News Review 1994;Feb:15.
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