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GHB (gamma-hydroxybutyrate)
Source: ceri.com
by John Morgenthaler and Dan Joy
GHB, or gamma-hydroxybutyrate, is a normal component of mammalian
metabolism. It is found naturally in every cell in the human body and is
most properly considered a nutrient. In the brain, the highest amounts are
found in the hypothalamus and basal ganglia. GHB is found in greater
concentrations in kidney, heart, skeletal muscles, and brown fat tissues.
It is believed to be a neurotransmitter, although the jury is still out as
to whether it exhibits all of the properties required for fulfillment of
this function. It is both a metabolite and precursor of the inhibitory
neurotransmitter GABA (gamma-aminobutyric acid, or gamma-aminobutyrate),
another nutrient to which it bears a close structural relationship. GHB,
however, does not act directly on GABA receptor sites.
GHB was first synthesized about thirty years ago by Dr. H. Laborit, a
French researcher interested in exploring the effects of GABA in the
brain. Because little or no GABA crosses the blood-brain barrier, Laborit
synthesized GHB, which substitutes a hydroxy group for an amino group.
This difference allows GHB to cross the blood brain barrier where some of
it is metabolized into GABA.
As it turned out, Laborit found that GHB exhibited a range of effects
beyond those expected from GABA. Over the intervening years, numerous
researchers have extensively studied GHB's effects. It is has come to be
used in Europe as a general anesthetic, a treatment for insomnia and
narcolepsy (a daytime sleeping disorder), an aid to childbirth (increasing
strength of contractions, decreasing pain, and increasing dilation of the
cervix), a treatment for alcoholism and alcohol withdrawal syndrome, and
for many other uses.
During the 1980s, GHB was widely available over-the-counter in health-food
stores, purchased largely by body-builders for its ability to stimulate
growth hormone release which aids in fat reduction and muscle building. In
the last few years it has been gaining popularity as a "recreational" drug
offering a pleasant, alcohol-like, hangover-free "high" with potent
prosexual effects.
Scientific Reports on GHB
For the thirty years prior to 1990, the scientific papers on GHB were
unanimous in reporting numerous beneficial physiological effects and the
absence of long-term negative effects. In 1964, Laborit listed "very low
toxicity" as one of the "principle elements" of the compound's
pharmacology. In a 1969 report on GHB's anesthetic uses, Vickers referred
to GHB as "a truly nontoxic hypnotic" and repeatedly emphasized its "lack
of toxicity." Vickers cited evidence that GHB demonstrates "no toxic
effects on the liver and kidney." In 1972, Laborit described the body's
metabolism of GHB and stressed "the absence of any need of detoxification
by the organism."
As recently as 1989, this scientific consensus on GHB's benign nature
remained unchanged. Gallimberti's study from that year on its uses in
treating alcohol withdrawal in humans notes that "GHB's action...seems to
be without serious side effects." His almost off-hand reference to the
"safety of GHB" shows how well-established this property of the nutrient
had become.
Then, on November 8th, 1990, the FDA banned the over-the-counter sale of
GHB in the United States. In 1991, two scientists from the California
Department of Health Services wrote a report on ten "poisonings"
associated with GHB. The authors, Chin and Kreutzer, warned of GHB's
"tremendous potential for abuse." They observed that "all interviewed
patients reported a pleasurable sensation or a 'high.' Several of
them...continued taking [GHB] because it made them 'feel good'."
Apparently, the authors construed feeling good in and of itself as a
potential threat to public health. Despite such dire language, the report
acknowledged that "there are no documented reports of long-term
[detrimental] effects. Nor is there any evidence for physiologic
addiction."
Of the ten "poisonings" reported, four involved "unknown doses," four
featured the "coingestion" of other drugs (usually alcohol), one involved
unmedicated epilepsy, and another a history of grand mal seizures. Since
alcohol and other central nervous system (CNS) depressants are not
recommended with GHB, and because GHB is contraindicated for epileptics,
such cases are not unexpected. Chin and Kreutzer acknowledge that the
"more severe reactions...generally occurred when patients took an
unmeasured dose, a particularly large dose, or several doses within a
short period of time." Such problems are easily avoided by following the
directions for GHB's use.
Although the specific clinical details of these ten cases are too lengthy
to go into here, one point needs addressing - the use of the terms "coma"
and "seizures" in descriptions of these cases. At a sufficiently high
dose, GHB can cause clonus, a rapid, rhythmic contraction and relaxation
of muscles which would be better described as muscle spasm or
uncontrollable twitching than a seizure. GHB can also cause intense
drowsiness, abrupt sedation, and deep sleep which is probably better
described as unarrousability or deep sedation than coma. Vickers [1969]
described it as a "nontoxic coma," which blunts some of the inflammatory
connotations of the term coma.
Regardless of their alarmist tone, the authors confirm that "there have
not been any reported deaths" and that "if product use is discontinued,
full recovery with no long-term side effects is universal." They concluded
that "the prognosis for people who experience GHB poisoning is quite
good."
The degree to which the pleasant state of GHB euphoria may be
psychologically addicting may not be fully appreciated. Anybody with known
attraction or addiction to tranquilizers or alcohol should pay special
heed to this possibility. In the few cases of GHB abuse that we have
investigated, there were pre-existing use/abuse patterns with alcohol
and/or tranquilizers. Ironically, it was GHB's lack of toxicity that led
to increased frequency of use (numerous times per day) that characterized
what can only be called classic cases of psychological addiction. Without
the dehydration and CNS irritation of alcohol, or the side effects of
tranquilizers, there was no incentive to moderate or curtail GHB use.
Fortunately, few people seem to have such overwhelming attraction to the
GHB state. Even Chin and Kreutzer minimize GHB's abuse potential by
stating, "No investigator [has] reported any long-term adverse effects,
addictive or dependent qualities associated with discontinued usage of the
drug."
Why Was GHB Banned?
It seems likely, then, that at least some of the motives behind the 1990
FDA ban of GHB were other than those of public safety. Such a ban
constitutes the only means of Federal control of a substance neither
scheduled by the DEA nor approved by the FDA as a drug. In the absence of
a genuine public-health concern, such control might have been motivated by
a desire to protect the pharmaceutical industry (with which the FDA is
closely intertwined) from competition from a safer, more effective and
less expensive alternative to sleeping pills. Is it a coincidence that the
FDA has also banned L-tryptophan, another nutrient that functions as a
safe and effective sleep aid?
What Are the Real Concerns?
As with most substances, unpleasant and possibly dangerous side effects
can be associated with excessive doses of GHB. A dose usually only about
twice the amount required for relaxation or a prosexual effect can, as one
user put it, "knock you out but fast." In this respect, GHB is probably
comparable to alcohol: if you drink twice as much as you normally would,
you probably wouldn't function very well. Despite its general safety and
lack of toxicity, the safe use of GHB requires information, preparation,
caution, and good judgment. In other words, follow the usage guidelines!
How Does It Feel?
Most users find that GHB induces a pleasant state of relaxation and
tranquility. Frequent effects are placidity, sensuality, mild euphoria,
and a tendency to verbalize. Anxieties and inhibitions tend to dissolve
into a feeling of emotional warmth, wellbeing, and pleasant drowsiness.
The "morning after" effects of GHB lack the unpleasant or debilitating
characteristics associated with alcohol and other relaxation-oriented
drugs. In fact, many users report feeling particularly refreshed, even
energized, the next day.
The effects of GHB can generally be felt within five to twenty minutes
after ingestion. They usually last no more than one and a half to three
hours, although they can be indefinitely prolonged through repeated
dosing. The effects of GHB are very dose-dependent. Small increases in the
amount ingested lead to significant intensification of the effect. Higher
levels feature greater giddiness, silliness, and interference with
mobility and verbal coherence, and maybe even dizziness. Even higher doses
usually induce sleep.
The Actions of GHB in the Body
GHB temporarily inhibits the release of dopamine in the brain. This may
cause increased dopamine storage, and later increased dopamine release
when the GHB influence wears off . This effect could account for the
middle-of-the-night wakings common with use of higher GHB doses, and the
general feelings of increased well-being, alertness and arousal the next
day.
GHB also stimulates pituitary growth hormone (GH) release. One
methodologically rigorous Japanese study reported nine-fold and
sixteen-fold increases in growth hormone 30 and 60 minutes respectively
after intravenous administration of 2.5 grams of GHB in six healthy men
between the ages of twenty-five and forty. GH levels were still seven-fold
higher at 120 minutes.
The mechanism by which GHB stimulates growth-hormone release is not known.
Dopamine activity in the hypothalamus is known to stimulate pituitary
release of growth hormone, but GHB inhibits dopamine release at the same
time that it stimulates GH release. This suggests that GHB's GH-releasing
effect takes place through an entirely different mechanism.
At the same time GH is being released, prolactin levels also rise. Serum
prolactin levels increase in a similar time-dependent manner as GH,
peaking at five-fold above baseline at 60 minutes. This effect, unlike the
release of GH, is entirely consistent with GHB's inhibition of dopamine.
Other compounds which lessen dopamine activity in the brain (such as the
neuroleptic Thorazine) have been shown to result in prolactin release.
Although prolactin tends to counteract many of the beneficial effects of
GH, the sixteen-fold increases in GH probably overwhelm the five-fold
increases in prolactin.
GHB induces "remarkable hypotonia" (muscle relaxation). It is now gaining
popularity in France and Italy as an aid to childbirth. GHB causes
"spectacular action on the dilation of the cervix," decreased anxiety,
greater intensity and frequency of uterine contractions, increased
sensitivity to oxytocic drugs (used to induce contractions), preservation
of reflexes, a lack of respiratory depression in the fetus, and protection
against fetal cardiac anoxia (especially in cases where the umbilical cord
wraps around the fetus' neck).
GHB is completely metabolized into carbon dioxide and water, leaving
absolutely no residue of toxic metabolites. Metabolism is so efficient
that GHB can no longer be detected in urine four to five hours after it is
taken by injection.
GHB activates a metabolic process known as the "pentose pathway" which
plays an important role in the synthesis of protein within the body. It
also causes a "protein sparing" effect which reduces the rate at which the
body breaks down its own proteins. These properties, along with GHB's
effect on growth hormone, underlie its common use as an aid to
muscle-building and fat loss.
Anesthetic (large) doses of GHB are accompanied by a small increase in
blood sugar levels, and a significant decrease in cholesterol. Respiration
becomes slower and deeper. Blood pressure may rise or fall slightly, or
remain stable, but a moderate bradycardia (slowing of the heart) is
consistent. A slight drop in body temperature also occurs. GHB also
stimulates the release of acetylcholine in the brain.
GHB and Sleep
GHB has been called "almost an ideal sleep inducing substance" [Smart
Drugs II, p. 245]. Small doses produce relaxation, tranquility and
drowsiness which make it extremely easy to fall asleep naturally. Higher
doses increase the drowsiness effect and decrease the time it takes to
fall asleep. A sufficiently large dose of GHB will induce sudden sleep
within five to ten minutes. Many other hypnotics interfere with various
stages of the sleep cycle thus preventing the body from achieving a
complete and balanced session of rest and recuperation. The most
remarkable facet of GHB-induced sleep is its physiological resemblance to
normal sleep. For instance, GHB sleep is characterized by increased levels
of carbon dioxide in the arteries, as in normal sleep. During normal and
GHB sleep, the CNS continues to be responsive to "noxious stimuli" (pain
and other irritations), a factor which sets limits on GHB's uses in
anesthesia. GHB facilitates both REM (rapid eye movement) sleep, and
"slow-wave" (non-REM) sleep, the stage of sleep featuring increased
release of growth hormone. And unlike the unconsciousness induced by other
anesthetics, that triggered by GHB does not feature a systemic decrease in
oxygen consumption.
The primary disadvantage to GHB's use as a sleep aid is it's short-term
influence - about three hours. During GHB's influence, sleep is deeper and
more restful, but after the GHB has worn off, people have a tendency to
wake up. The higher the dose, the greater is this tendency. Some have
called this pattern the "dawn effect" and have speculated that it is
related to the release of stored-up dopamine. Some people minimize this
effect by taking minimal doses of GHB. Others take advantage of this
effect by getting a couple of hours of work done in the middle of the
night. Still others choose to take a second dose of GHB to sleep for
another three hours.
It should be noted that not everyone can be put to sleep by GHB. We have
spoken to three men who have never achieved sleep even with the doses
normally used for such purposes. In addition, Takahara [1977] reported
that one of the six men in the growth hormone study cited above remained
conscious even though he had received two and a half grams of GHB
intravenously, a dosage which rendered the rest of the participants
unconscious.
GHB, Alcohol and Alcoholism
GHB shows great promise in the treatment of alcoholism. In Europe, one of
its primary uses is to relieve withdrawal symptoms, cravings, and anxiety
among alcoholics.
In laboratory rats addicted to alcohol, withdrawal symptoms closely
resemble those exhibited by humans, including tremors, convulsions, and
hypersensitivity to sound. All of these symptoms were blocked by
sufficiently high doses of GHB. Administration of GHB has also been found
to prevent alcohol consumption among rats that voluntarily ingest alcohol.
In a rigorous, double-blind, placebo-controlled study conducted of human
alcoholics, "nearly all withdrawal symptoms disappeared within two to
seven hours" after administration of GHB. On a
severe-moderate-mild-or-none scale, withdrawal symptoms remained below
moderate during the entire period. The only side effect observed was
slight, occasional, and transient dizziness. The researchers concluded,
"the results clearly indicated that GHB is effective for the suppression
of withdrawal symptoms in alcoholics".
Other Uses of GHB
GHB has a decades long track record of use as a general anesthetic.
Administered intravenously, an anesthetic dose of GHB is in the range of
4-5 grams for a 150-pound person. Its advantages as an anesthetic include
low toxicity, relatively few contraindications, slowing of the heart rate
without loss of blood pressure, the absence of irritation to the veins
with intravenous administration, muscle relaxation, absence of respiratory
depression (usually), reduction of body temperature (hypothermia), and
various protective and anti-shock actions. However, GHB can almost never
be used in anesthesia without the additional administration of other drugs
because it does not produce complete surgical anesthesia except in
children. The autonomic nervous system remains active during GHB-induced
anesthetic coma, and thus the body continues to respond to surgical
stimuli through increases in heart rate, blood pressure, and cardiac
output, as well as through sweating, peripheral vasoconstriction,
vocalization, and reflex muscle action. Local anesthetics or other drugs
which suppress these responses must therefore also be used, like the way a
dentist or orthodontic surgeon might use Novocaine to kill pain along with
nitrous oxide to render a patient unconscious.
It is suspected that part of GHB's protective function involves a slowing
of the metabolism of brain cells, thus reducing their requirements for
oxygen and glucose. Another factor in GHB's anti-shock capability may be
the marked vasodilation induced in the liver and kidney, thus increasing
blood flow to those vital organs.
GHB's efficacy for treating anxiety has been positively demonstrated in
tests involving schizophrenic subjects. Its sedative properties have
earned it a role as a psychotherapeutic adjunct. It has also been used to
assist the process of "abreaction," or the release (usually through
verbalization) of repressed emotion. Unlike other "anxiolytic" (or
anti-anxiety) drugs, GHB's effect is non-toxic.
Furthermore, GHB's reduction of inhibitions, its tendency to encourage
verbalization, and the typical lack of fear during the GHB experience
would seem to provide an ideal context for the verbal exploration of
difficult emotional territory during therapy.
GHB and Sex
Scientists and doctors have traditionally been reluctant to ascribe
aphrodisiac properties to any substance, although this tendency may have
abated somewhat in recent years. It is a testament, then, to the power the
GHB's sexual effects that they were clearly acknowledged in the scientific
literature by 1972. Dr. Laborit wrote:
"A last point should still be mentioned: the [GHB] action on Man which
could be called 'aphrodisiac.' We cannot present any animal experiments on
this subject. However, the oral form has now been sufficiently used so
that, as generally agreed, no doubt can subsist as to its existence."
We have identified four main prosexual properties: 1) disinhibition, 2)
heightening of the sense of touch (tactility), 3) enhancement of male
erectile capacity, and 4) increased intensity of orgasm.
Perhaps the foremost prosexual property of GHB is disinhibition. Some
users suggest that GHB's other sexual benefits are secondary effects, made
possible (or at least amplified) by this loosening of psychosomatic
constraint. A number of people have commented that this disinhibition is
particularly marked among women.
Women often report that GHB makes their orgasms longer and more intense,
as well as more difficult or time-consuming to achieve, especially at
higher doses. As with its other effects, GHB's impact on female orgasm
seems highly sensitive to small adjustments in dosage.
Legal Status and
Availability
GHB is not approved in the US and has been banned from over-the-counter
sale by the FDA. GHB has not yet been "scheduled" as a "controlled
substance" by the DEA, and therefore simple possession is not illegal. GHB
continues to be sold to legitimate laboratories and scientists for
research purposes, but selling it specifically for human consumption,
especially while making claims about its health benefits, is a violation
of current FDA regulations and policy.
In some European countries, GHB is an approved drug available by
prescription. Local doctors, pharmacists and government bureaucrats should
be able to provide country-by-country specifics.
GHB is growing in popularity and seems to be widely available in the
underground "gray market." Since most of the GHB available through such
channels is of the "bootleg" variety, manufactured by non-professional
"kitchen" chemists, concerns about quality and purity should be kept in
mind. Caveat emptor (buyer beware)!
Safety Issues
As has been emphasized, the overall safety of GHB is well-established, and
no deaths attributable to GHB have been reported over the thirty year
period that this compound has been in use. In fact, as of 1990, only
forty-six adverse reactions had been reported in the United States surely
constituting only an infinitesimal fraction of actual usage, all followed
by rapid and complete recovery. Unlike a large proportion of other drugs
including alcohol and even Tylenol, GHB has no toxic effects on the liver,
kidney or other organs. One program of sleep therapy using six to eight
grams daily for a period of eight to ten days produced no side effects.
Vickers [1969] even reports that doses as high as twenty to thirty grams
per twenty-four hour period have been used for several days without
negative consequences (don't do this at home kids!). In the Canadian
studies of narcolepsy mentioned earlier, the nightly use of two to six
teaspoons (one teaspoon equaling roughly 2.5 grams) for several years
resulted in no reports of long-term adverse effects, or problems with
issues of addiction or dependence. In one of these studies, one patient
inadvertently ingested fifteen teaspoons without adverse consequence
"other than deep sedation and headache the next day". And in France,
sub-anesthetic oral doses were used by "a large number of patients for
about six years" without untoward effect.
Side Effects
According to Dr. Gallimberti [1989], the action of GHB is "without serious
side effects." Some research programs have reported no side effects at
all. Nonetheless, it's clear that some minor side effects can occur. Those
most commonly experienced are drowsiness, dizziness, nausea, and sometimes
vomiting. As a sedative-hypnotic, GHB's effects bear some similarity to
those of alcohol and tranquilizers. GHB not only "may cause drowsiness"
like these other drugs, it will almost invariably do so. Ataxia, or
incoordination, can also be a side effect of GHB. Do not drive a vehicle
or operate dangerous machinery while under the influence of GHB.
As mentioned, clonic movements (muscle contractions or "seizures") have
been observed during the onset of GHB-induced sleep. Headache is sometimes
reported. A moderate slowing of the heart rate is a consistent effect, and
small changes in blood pressure can take place. Likewise, orthostatic
hypotension (a sudden drop in blood pressure caused by standing up
quickly) has also been reported. Sometimes this is experienced as brief
dizziness, and rarely people can briefly lose consciousness. At very high
doses, cardiac and respiratory depression can occur.
Sufficiently large doses of GHB can cause sudden sedation and loss of
consciousness. Do not take such doses except when reclining on a bed or
sofa. It is also a bad idea to take such doses in the presence of people
who don't know anything about GHB. You may alarm your family or friends
and wake up in an emergency room (with a large medical bill). More unusual
and extreme reactions have included diarrhea, lack of bladder control,
temporary amnesia, and sleep-walking. Whatever side effects may be noted,
they are often much more severe when GHB is combined with other central
nervous system depressants.
Contraindications
Although contraindications for GHB have been described as "remarkably
few", those who suffer from any of the following conditions should not use
GHB: severe illness of any kind, epilepsy, eclampsia (convulsions),
bradycardia (slowed heart-beat) due to conduction problems
[left-bundle-branch-block is an example of conduction difficulty],
Cushing's syndrome, severe cardiovascular disease, hyperprolactinemia, and
severe hypertension.
Severe alcoholism is sometimes mentioned as a contraindication for GHB
[Smart Drugs II, page 244] even though GHB has been used quite
successfully in the treatment of withdrawal symptoms. The explanation for
this seeming contradiction probably lies in the likelihood that severe
alcoholics may combine GHB with alcohol.
GHB should not be used with benzodiazepines ("minor tranquilizers" such as
Valium and Xanax), phenothiazines ("major tranquilizers" like Thorazine
and Stellazine), various painkillers (barbiturates and opiates), alcohol,
anticonvulsants (Dilantin and phenobarbital) and even many
over-the-counter allergy and sleep remedies - without direct medical
supervision.
Dosage
Determining the ideal dose is probably the trickiest aspect of working
with GHB. The amount required for a given level of effect will vary from
person to person, and the dose-response curve is fairly steep.
Overestimating the dose can have consequences ranging in seriousness from
ruining your plans for the evening to waking up in the emergency ward as a
result of panic on the part of concerned-but-uninformed friends or
relatives.
Once you have found the levels that give you the effects you desire, they
will remain consistent. Tolerance to GHB does not develop. However, recent
(not current) alcohol consumption may decrease the effect of a given dose
of GHB.
Most people find that a dose in the range of 0.75-1.5 grams is suitable
for prosexual purposes, and that a quantity in the range of 2.5 grams is
sufficient to force sleep.
Some people think that GHB might lower potassium levels and should
therefore be taken with potassium supplementation. Some research papers
have identified such an effect, others have not. If you want to play it
safe, take a potassium supplement equal to 10% of the GHB dose.
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