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CDC Morbidity and Mortality Weekly Report
Vol. 46, No 13, April 4, 1997 

Gamma Hydroxy Butyrate Use --
New York and Texas, 1995-1996

Gamma hydroxy butyrate (GHB) is a central nervous system depressant
approved as an anaesthetic in some countries; however, with the exception
of investigational research, it is not approved for any use in the United
States. Primary groups using GHB include party and nightclub attendees and
bodybuilders. In addition, GHB is one of several agents characterized as a
"date rape"  drug. During August 1995- Septem ber 1996, poison control
centers in New York and Texas received reports of 69 acute poisonings and
one death attributed to ingestion of GHB. This report describes two cases
and summarizes the investigations of GHB use in Texas and New York. The
findings of these investigations underscore the health hazards associated
with use of GHB. 


At 12:30 p.m. on August 5, 1996, a 17-year-old girl with no previous
history of drug or alcohol use was admitted to an emergency department
(ED) because of cardiac arrest with cardiopulmonary resuscitation in
progress. She was pronounced dead at 12:40 p.m. On the night of August 4,
she had been at a local dance club, where she was reported to have
ingested soft drinks. An autopsy was performed; multiple toxicologic
screens of blood and bile samples did not detect alcohol or other drugs.
However, on September 13, a test on previously obtained serum detected a
serum level of 27 mg/L of GHB. 

From November 14, 1995, through September 30, 1996, the Texas Department
of Health received reports of 57 persons who had adverse hea lth effects
attributed to ingestion of GHB, including the one death described in this
report. Of the 57 reports, 30 were received from the Dallas Poison Control
Center, and 26 were received from the Galveston Poison Control Center. The
death was reported by the Assistant Medical Examiner in Harris County, who
listed the death as a homicide as the result of GHB toxicity. Of the 56
reports from the poison control centers, 34 involved males; 10 reports
involved teenagers aged 16-18 years. Nineteen persons were treated in and
released from hospital EDs, and 25 were admitted to intensive-care units
with severe clinical symptoms, including coma (15), respiratory depression
(three), and agitation (one); six required intubation. Of the 56 reports,
12 included ingestion of both alcohol and GHB, and three included the use
of GHB with other drugs. 


On October 30, 1996, a 20-year-old man who was unresponsive after several
episodes of vomiting was taken to an ED 21/2 hours after ingesting a
mixture of GHB and sodium hydroxide. He was intubated and admitted to the
intensive-care unit, where a bronchoscopy indicated friable lung tissue
that was attributed to aspiration of gastric contents containing sodium
hydroxide. He developed bilateral pneumothoraces and had generalized
seizures and was transferred to a third hospital for possible
extracorporeal membrane oxygen therapy and lung transplant. However, his
condition improved, and he was extubated and placed on supportive care and
recovered. 

During August 27, 1995-October 30, 1996, the Long Island Regional Poison
Control Center received reports of 13 persons with exposure to GHB. All 13
were evaluated in hospital EDs. Four of the 13 also consumed ethanol. All
five persons initially had altered mental status, including coma (three),
stupor (one), and inebriation (one). Eight of the 13 persons had prepared
GHB at home using sodium hydroxide and butyrol lactone; of the eight,
three required admission to a hospital. 

Reported by: J Carter, DO, H Mofenson, MD, T Caraccio, PharmD, Long Island
Regional PoisonControl Center, Winthrop-Univ Hospital, New York; P Smith,
MD, State Epidemiologist, D Morse, MD, New York State Dept of Health. C
Keys, MD, L Williams, Poison Center Network, Div of Emergency Medicine,
Univ of Texas Southwestern School of Medicine, Dallas; G Coody, Drug and
Medical Devices Div, Bur of Food and Drug Safety, Texas Dept of Health.
Office of DiversionControl, Drug Enforcement Administration. Environmental
Hazards Epidemiology Section, Health Studies Br, Div of Environmental
Hazards and Health Effects, National Center for Envi-ronmental Health,
CDC.

Editorial Note: GHB increases dopamine levels in the brain and has effects
thr ough the endogenous opioid system; most GHB is excreted during the
first hours after ingestion (1 ). Manifestations of acute GHB toxicity
include coma, seizures, respiratory depression, and vomiting. Other
documented effects of GHB include amnesia and hypotonia (associated with
doses of 10 mg/kg body weight); a normal sequence of rapid eye movement
(REM) and non-REM sleep (doses of 20-30 mg/kg body weight); and anesthesia
(doses of approximately 50 mg/kg body weight). Doses of >50 mg/kg body
weight can decrease cardiac output and produce severe respiratory
depression, seizure-like activity, and coma (2 ); coma and respiratory
depression may be potentiated by concomitant use of alcohol ( 3 ). There
is no antidote for GHB overdose, and treatment is restricted to
nonspecific supportive care. Patients in New York and Texas have required
ED care; many of those hospitalized have required ventilatory support and
intensive care. 

In the United States, GHB has been produced clandestinely in widely
varying degrees of purity. GHB has been marketed as a liquid or powder and
has been sold on the street under names such as "Grevious Bodily Harm,"  " 
Georgia H ome Boy," "Liquid Ecstasy,"  "Liquid X," "Liquid E,"  "GHB," 
"GBH,"  "Soap,"  "Sc oop," "Easy Lay,"  "Salty Water,"  " G-Riffick," 
"Cherry Menth,"  and "Organic Quaalude."  Improper preparation of GHB can
result in a mixture of GHB and sodium hydroxide that can be severely toxic
because of the combined e ffects of the GHB and the direct caustic effects
of sodium hydroxide. 

In Dallas, GHB use has been associated with events at which several
persons have been found comatose. Some persons who have sustained adverse
effects of GHB have reported being given the drug surreptitiously (e.g.,
having it slipped into their drink), while others have admitted to
intentional use. The Drug Enforcement Administration (DEA) is examining
the distribution and abuse of GHB in the United States; al though
distribution has been documented in 27 states, GHB use is highly prevalent
in California, Florida, Georgia, and Texas. 

In the United States, GHB is under specific Food and Drug Administration
exemptions for investigational research protocols for the treatment of
narcolepsy. Although possession of GHB is not illegal under federal law,
its manufacture and sale is prohibited under the Food, Drug, and Cosmetic
Act. In Georgia and Rhode Island, state controlled substances acts have
classified GHB into Schedule I*, and other states are considering similar
action. In addition, the DEA is gathering information and considering a
scheduling review for possible control of GHB under the Federal Controlled
Substances Act#. Public health officials should report episodes of adverse
effects of GHB use to DEA, telephone (202) 307-7183.

References

1. Vayer P, Mandel P, Maitre M. Gamma-hydroxy butyrate, a possible
neurotransmitter. Life Sci 1987;41:1547-57.

2. CDC. Multistate outbreak of poisonings associated with illicit use of
gamma hydroxy butyrate. MMWR 1990;39:861-3.

3. Mamelak M. Gammahydroxybutyrate: an endogenous regulator of energy
metabolism. Neurosci Biobehav Rev 1989;13:187-98. 

* Drugs that do not have currently accepted medical use in the United States, have a high abusepotential, and are not proven to be safe under medical supervision.

# Public Law no. 91-513.