Summary of the Testimony of
Lester
Grinspoon, M.D.
before
the Crime Subcommittee of the Judiciary Committee
U.S.
House of Representatives
October 1,
1997
Summary of
the Statement by Lester Grinspoon, M.D.
Mr. Chairman and members
of the subcommittee, I appreciate the opportunity to
appear before you this morning to share my views on the
use of marihuana as a medicine.
It has been well known for
thousand of years that cannabis has medical uses. It is
far safer than most medicines prescribed by doctors daily
and often works for patients who cannot tolerate the side
effects of other drugs. In many cases no other drug will
do the job as safely or as well. Cannabis has never been
demonstrated to have caused an overdose death. It does
not disturb any physiological functions or damage any
body organ when used in therapeutic doses. It produces
little or no physical dependence or tolerance, and there
is no evidence that medical use of cannabis has ever led
to habitual use as an intoxicant. There are many ways in
which marihuana can be used to reduce human suffering at
small cost. Clinical experience suggests that it is
helpful for patients with severe nausea and vomiting,
arthritis, glaucoma, muscle spasms, premenstrual
syndrome, seizure disorders, the AIDS weight loss
syndrome, asthma, fibromyalgia, Tourette’s syndrome,
and depression, to name a few.
Many thousands of patients
are using cannabis to treat these and other disorders.
Given the legal risks, they would not be doing this if
they did not believe it was helpful to them. These
patients are in urgent need of a legal accommodation that
allow them to use a medicine which they know is important
to their well-being.
[top]
Testimony of
Lester
Grinspoon, M.D.
Associate
Professor of Psychiatry, Harvard Medical School
before the
Crime Subcommittee of the Judiciary Committee
U.S. House
of Representatives
Washington,
D.C.
October 1,
1997
Mr. Chairman and members
of the subcommittee, I appreciate the opportunity to
appear before you this morning to share my views on the
use of marihuana as a medicine.
In September 1928
Alexander Fleming returned from vacation to his
laboratory and discovered that one of the petri dishes he
had inadvertently left out over the summer was overgrown
with staphylococci except for the area surrounding a mold
colony. That mold contained a substance he later named
penicillin. He published his finding in 1929, but the
discovery was ignored by the medical establishment, and
bacterial infections continued to be a leading cause of
death. Had it aroused the interest of a pharmaceutical
firm, its development might not have been delayed. More
than 10 years later, under wartime pressure to develop
antibiotic substances to supplement sulfonamide, Howard
Florey and Ernst Chain initiated the first clinical trial
of penicillin (with six patients) and began the
systematic investigations that might have been conducted
a decade earlier.1
After its debut in 1941,
penicillin rapidly earned a reputation as "the
wonder drug of the ‘40s." There were three
major reasons for that reputation: it was remarkably
non-toxic, even at high doses; it was inexpensive to
produce on a large scale; and it was extremely versatile,
acting against the microorganisms that caused a great
variety of diseases, from pneumonia to syphilis. In all
three respects cannabis suggests parallels:
1) Cannabis is remarkably
safe. Although not harmless, it is surely less toxic than
most of the conventional medicines it could replace if it
were legally available. Despite its use by millions of
people over thousands of years, cannabis has never caused
an overdose death. The most serious concern is
respiratory system damage from smoking, but that can
easily be addressed by increasing the potency of cannabis
and by developing the technology to separate the
particulate matter in marihuana smoke from its active
ingredients, the cannabinoids (prohibition, incidentally,
has prevented this technology from flourishing). Once
cannabis regains the place in the U.S. Pharmacopoeia that
it lost in 1941 after the passage of the
Marihuana Tax Act (1937), it will be among the least
toxic substances in that compendium. Right now the
greatest danger in using marihuana medically is the
illegality that imposes a great deal of anxiety and
expense on people who are already suffering.
2) Medical cannabis would
be extremely inexpensive. Street marihuana today costs
$200 to $400 an ounce, but the prohibition tariff
accounts for most of that. A reasonable estimate of the
cost of cannabis as a medicine is $20 to $30 an ounce, or
about 30 to 40 cents per marihuana cigarette. As an
example of what this means in practice, consider the
following. Both the marihuana cigarette and an 8 mg
ondansetron pill—cost to the patient, $30 to $40 --
are effective in most cases for the nausea and vomiting
of cancer chemotherapy (although many patients find less
than one marihuana cigarette to be more useful, and they
often require several ondansetron pills). Thus cannabis
would be at least 100 times less expensive than the best
present treatment for this symptom.
3) Cannabis is remarkably
versatile. Let me review briefly some of the symptoms and
syndromes for which it is useful.
 Cancer
Treatment
Cannabis has several uses
in the treatment of cancer. As an appetite stimulant, it
can help to slow weight loss in cancer patients.2 It may also act as a mood
elevator. But the most common use is the prevention of
nausea and vomiting of cancer chemotherapy. About half of
patients treated with anticancer drugs suffer from severe
nausea and vomiting, which are not only unpleasant but a
threat to the effectiveness of the therapy. Retching can
cause tears of the esophagus and rib fractures, prevent
adequate nutrition, and lead to fluid loss. Some patients
find the nausea so intolerable they say they would rather
die than go on. The antiemetics most commonly used in
chemotherapy are metoclopramide (Reglan), the relatively
new ondansetron (Zofran), and the newer granisetron
(Kytril). Unfortunately, for many cancer patients these
conventional antiemetics do not work at all or provide
little relief.
The suggestion that
cannabis might be useful arose in the early 1970s when
some young patients receiving cancer chemotherapy found
that marihuana smoking reduced their nausea and vomiting.
In one study of 56 patients who got no relief from
standard antiemetic agents, 78% became symptom-free when
they smoked marihuana.3 Oral tetrahydrocannabinol (THC) has proved
effective where the standard drugs were not.4,5 but smoking generates faster and
more predictable results because it raises THC
concentration in the blood more easily to the needed
level. Also, it may be hard for a nauseated patient to
take oral medicine. In fact, there is strong evidence
that most patients suffering from nausea and vomiting
prefer smoked marihuana to oral THC.2
Oncologists may be ahead
of other physicians in recognizing the therapeutic
potential of cannabis. In the spring of 1990, two
investigators randomly selected more than 2,000 members
of the American Society of Clinical Oncology (one-third
of the membership) and mailed them an anonymous
questionnaire to learn their views on the use of cannabis
in cancer chemotherapy. Almost half of the recipients
responded. Although the investigators acknowledge that
this group was self-selected and that there might be a
response bias, their results provide a rough estimate of
the views of specialists on the use of Marinol
(dronabinol, oral synthetic THC) and smoked marihuana.
Only 43% said the
available legal antiemetic drugs (including Marinol)
provided adequate relief to all or most of their
patients, and only 46% said the side effects of these
drugs were rarely a serious problem. Forty-four percent
had recommended the illegal use of marihuana to at least
one patient, and half would prescribe it to some patients
if it were legal. On average, they considered smoked
marihuana more effective than Marinol and roughly as
safe.6
 Glaucoma
Cannabis may also be
useful in the treatment of glaucoma, the second leading
cause of blindness in the United States. In this disease,
fluid pressure within the eyeball increases until it
damages the optic nerve. About a million Americans suffer
from the form of glaucoma (open angle) treatable with
cannabis. Marihuana causes a dose-related, clinically
significant drop in intraocular pressure that lasts
several hours in both normal subjects and those with the
abnormally high ocular tension produced by glaucoma. Oral
or intravenous THC has the same effect, which seems to be
specific to cannabis derivatives rather than simply a
result of sedation. Cannabis does not cure the disease,
but it can retard the progressive loss of sight when
conventional medication fails and surgery is too
dangerous.7
 Seizures
About 20% of epileptic
patients do not get much relief from conventional
anticonvulsant medications. Cannabis has been explored as
an alternative at least since 1975 when a case was
reported in which marihuana smoking, together with the
standard anticonvulsants phenobarbital and
diphenylhydantoin, was apparently necessary to control
seizures in a young epileptic man.8 The cannabis derivative that is
most promising as an anticonvulsant is cannabidiol. In
one controlled study, cannabidiol in addition to
prescribed anticonvulsants produced improvement in seven
patients with grand mal convulsions; three showed great
improvement. Of eight patients who received a placebo
instead, only one improved.9 There are patients suffering from
both grand mal and partial seizure disorders who find
that smoked marihuana allows them to lower the doses of
conventional anticonvulsant medications or dispense with
them altogether .2
 Pain
There are many case
reports of marihuana smokers using the drug to reduce
pain: post-surgery pain, headache, migraine, menstrual
cramps, and so on. Ironically, the best alternative
analgesics are the potentially addictive and lethal
opioids. In particular, marihuana is becoming
increasingly recognized as a drug of choice for the pain
that accompanies muscle spasm, which is often chronic and
debilitating, especially in paraplegics, quadriplegics,
other victims of traumatic nerve injury, and people
suffering from multiple sclerosis or cerebral palsy. Many
of them have discovered that cannabis not only allows
them to avoid the risks of other drugs, but also reduces
muscle spasms and tremors; sometimes they are even able
to leave their wheelchairs.10
One of the most common
causes of chronic pain is osteoarthritis, which is
usually treated with synthetic analgesics. The most
widely used of these drugs—aspirin, acetaminophen
(Tylenol), and nonsteroidal antiinflammatory drugs
(NSAIDs) like ibuprofen and naproxen—are not
addictive, but they are often insufficiently powerful.
Furthermore, they have serious side effects. Stomach
bleeding and ulcer induced by aspirin and NSAIDs are the
most common serious adverse drug reactions reported in
the United States, causing an estimated 7,000 deaths each
year. Acetaminophen can cause liver damage or kidney
failure when used regularly for long periods of time; a
recent study suggests it may account for 10% of all cases
of end-stage renal disease, a condition that requires
dialysis or a kidney transplant.11,12 Marihuana, as I pointed out
earlier, has never been shown to cause death or serious
illness.
 AIDS
More than 300,000
Americans have died of AIDS. Nearly a million are
infected with HIV, and at least a quarter of a million
have AIDS. Although the spread of AIDS has slowed among
homosexual men, the reservoir is so huge that the number
of cases is sure to grow. Women and children as well as
both heterosexual and homosexual men are now being
affected; the disease is spreading most rapidly among
intravenous drug abusers and their sexual partners. The
disease can be attacked with anti-viral drugs, of which
the best known are zidovudine (AZT) and protease
inhibitors. Unfortunately, these drugs sometimes cause
severe nausea that heightens the danger of
semi-starvation for patients who are already suffering
from nausea and losing weight because of the
illness—a condition sometimes called the AIDS wasting syndrome.
Marihuana is particularly
useful for patients who suffer from AIDS because it not
only relieves the nausea but retards weight loss by
enhancing appetite. When it helps patients regain lost
weight, it can prolong life. Marinol has been shown to
relieve nausea and retard or reverse weight loss in
patients with HIV infection, but most patients prefer
smoked cannabis for the same reasons that cancer
chemotherapy patients prefer it: it is more effective and
has fewer unpleasant side effects, and the dosage is
easier to adjust.
These are the symptoms and
syndromes for which cannabis is most commonly used today,
but there are others for which clinical experience
provides compelling evidence. It is distressing to
consider how many lives might have been saved if
penicillin had been developed as a medicine immediately
after Fleming’s discovery. It is equally frustrating
to consider how much suffering might have been avoided if
cannabis had been available as a medicine for the last 60
years. Initial enthusiasm for drugs is often disappointed
after further investigation, but this is hardly likely in
the case of cannabis, since it is not a new medicine at
all. Its long medical history began 5,000 years ago in
China and extended well into the twentieth century.
Between 1840 and 1900, more than one hundred papers on
its therapeutic uses were published in American and
European medical journals. It was recommended as an
appetite stimulant, muscle relaxant, analgesic, sedative,
anticonvulsant, and treatment for opium addiction. As
late as 1913, the great Sir William Osler cited it as the
best remedy for migraine in a standard medical textbook.
In the United States, what
remained of marihuana’s medical use was effectively
eliminated by the Marihuana Tax Act of 1937, which was
ostensibly designed to prevent nonmedical use but made
cannabis so difficult to obtain that it was removed from
standard pharmaceutical references. When the present
comprehensive federal drug law was passed in 1970,
marihuana was officially classified as a Schedule I drug:
a high potential for abuse, no accepted medical use, and
lack of safety for use under medical supervision.
But in the 1970s the
public began to rediscover its medical value, as letters
appeared in lay publications from people who had learned
that it could relieve their asthma, nausea, muscle
spasms, or pain and wanted to shared that knowledge with
readers who were familiar with the drug. The most
effective spur to the movement for medical marihuana came
from the discovery that it could prevent the AIDS wasting
syndrome. It is not surprising that the Physicians
Association for AIDS Care was one of the medical
organizations that endorsed the California initiative
prohibiting criminal prosecution of medical marihuana
users. The mid-1980s had already seen the establishment,
often by people with AIDS, of cannabis buyers’
clubs, organizations that distribute medical marihuana in
open defiance of the law. These clubs buy marihuana
wholesale and provide it to patients at or near cost,
usually on the written recommendation of a physician.
Although a few of the clubs have been raided and closed,
most are still flourishing, and new ones are being
organized. Some of them may gain legal status as a result
of the initiative.
Until the recent vote in
California, efforts to change the laws had been futile.
In 1972 the National Organization for the
Reform of Marihuana Laws (NORML) entered a petition to move marihuana out of
Schedule I under federal law so that it could become a
prescription drug. It was not until 1986 that the Drug
Enforcement Administration (DEA) finally agreed to the
public hearings required by law. During two years of
hearings, many patients and physicians testified and
thousands of pages of documentation were introduced. In
1988 the DEA’s Administrative Law Judge, Francis L.
Young, declared that marihuana fulfilled the requirement
for transfer to Schedule II. In his opinion he described it as "one of the safest
therapeutically active substances known to man." His
order was overruled by the DEA.
Nevertheless, a few
patients have been able to obtain medical marihuana
legally in the last twenty years. Beginning in the 1970s,
thirty-five states passed legislation that would have
permitted medical use of cannabis but for the federal
law. Several of those states actually established special
research programs, with the permission of the federal
government, under which patients who were receiving
cancer chemotherapy would be allowed to use cannabis.
These projects demonstrated the value of both smoked
marihuana and oral THC. The FDA then approved oral THC as
a prescription medicine, but ignored the data that
suggested that smoked marihuana was more useful than oral
THC for some patients. With the approval of Marinol, this
research came to an end. In 1976, the federal government
introduced the Individual Treatment Investigational New
Drug program (commonly referred to as the Compassionate
IND), which provided marihuana to a few patients whose
doctors were willing to undergo the paperwork-burdened
and time-consuming application process. About three dozen
patients eventually received marihuana before the program
was discontinued in 1992, and eight survivors are still
receiving it—the only persons in the country for
whom it is not a forbidden medicine. It is safe to say
that a significant number of the more than ten million
American citizens arrested on marihuana charges in the
last thirty years were using the drug therapeutically.
The Schedule I classification persists, although in my
view and the view of millions of other Americans, it is
medically absurd, legally questionable, and morally
wrong.
Opponents of medical
marihuana often object that the evidence of its
usefulness, although strong, comes only from case reports
and clinical experience. It is true that there are no
double-blind controlled studies meeting the standards of
the Food and Drug Administration, chiefly because legal,
bureaucratic, and financial obstacles have been
constantly put in the way. The situation is ironical,
since so much research has been done on marihuana, often
in unsuccessful efforts to show health hazards and
addictive potential, that we know more about it than
about most prescription drugs. In any case, individual
therapeutic responses are often obscured in group
experiments, and case reports and clinical experience are
the source of much of our knowledge of drugs. As Dr.
Louis Lasagna has pointed out, controlled experiments
were not needed to recognize the therapeutic potential of
chloral hydrate, barbiturates, aspirin, insulin, or
penicillin.13 Nor was that the way we learned about the
use of propranolol for hypertension, diazepam for status
epilepticus, and imipramine for enuresis. All these drugs
had originally been approved for other purposes.
In the experimental method
known as the single patient randomized trial, active and
placebo treatments are administered randomly in
alternation or succession. The method is often used when
large-scale controlled studies are inappropriate because
the disorder is rare, the patient is atypical, or the
response to treatment is idiosyncratic.14 Several patients have told me that
they assured themselves of marihuana’s effectiveness
by carrying out such experiments on themselves,
alternating periods of cannabis use with periods of
abstention. I am convinced that the medical reputation of
cannabis is derived partly from similar experiments
conducted by many other patients.
Some physicians may regard
it as irresponsible to advocate use of a medicine on the
basis of case reports, which are sometimes disparaged as
merely "anecdotal" evidence which counts
apparent successes and ignore apparent failures. That
would be a serious problem only if cannabis were a
dangerous drug. The years of effort devoted to showing
that marihuana is exceedingly dangerous have proved the
opposite. It is safer, with fewer serious side effects,
than most prescription medicines, and far less addictive
or subject to abuse than many drugs now used as muscle
relaxants, hypnotics, and analgesics.
Thus cannabis should be
made available even if only a few patients could get
relief from it, because the risks would be so small. For
example, as I mentioned, many patients with multiple
sclerosis find that cannabis reduces their muscle spasms
and pain. A physician may not be sure that such a patient
will get more relief from marihuana than from the
standard drugs baclofen, dantrolene, and
diazepam—all of which are potentially dangerous or
addictive—but it is almost certain that a serious
toxic reaction to marihuana will not occur. Therefore the
potential benefit is much greater than any potential
risk.
During the past few years,
the medical uses of marihuana have become increasingly
clear to many physicians and patients, and the number of
people with direct experience of these uses has been
growing. Therefore the discussion is now turning from
whether cannabis is an effective medicine to how it
should be made available. It is essential to relax legal
restrictions that prevent physicians and patients from
achieving a workable accommodation that takes into
account the needs of suffering people. H.R. 1782 (the
Medical Use of Marihuana Act) is a worthwhile move in
that direction because it gets the federal government out
of the way and allows the states to experiment with their
own solutions to the problem. I strongly urge that you
pass this law.
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1997.
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