HIV Clinical Trial
Official title:
Clinical Trial to Evaluate Pharmacological Interactions Between γ-hydroxybutyrate (GHB) and Cobicistat
Gamma-hydroxybutyric acid (GHB) is a popular "party drug" because it is inexpensive and easy
to ingest. The calming and euphoric effects of GHB in low doses have given the drug the
nickname "liquid ecstasy". However, at doses >60 mg/kg coma, convulsions, and respiratory
depression can occur. If the drug combinates with alcohol these effects intensify, especially
respiratory depression and hypotension.
Lately a phenomenon called Chemsex has been spreading across big European cities. This is a
form of recreational drug use and it is believed that can be, in part, the cause of the
increasing in consumption of GHB. Chemsex is especially common among men who have sex with
other men (MSM) and in people living with HIV, with up to 50% of HIV-positive MSM reporting
to be engaged in chemsex in recent months. This population is specially concerning since the
combination of ART with the drug can cause pharmacological interactions leading to overdose.
Specifically, this study intends to evaluate the drug interaction with low doses of
cobicistat, an antiretroviral drug enhancer, since there are two case reports of
life-threatening overdoses in patients on treatment with high doses of another enhancer that
has a similar effect than cobicistat, but there are no studies about interactions with low
doses.
Gamma-hydroxybutyric acid (GHB) is an endogenous compound present in most mammalian tissues
at nanomolar concentrations and a minor metabolite or precursor of gammaaminobutyric acid
(GABA). GHB was first synthesized in 1960 by the French biochemist H.-M. Laborit who was
searching for analogues of GABA. Currently, medically formulated GHB sodium oxybate (Xyrem®)
is approved in different countries for such varied uses as general anaesthesia, the treatment
of alcohol withdrawal and addiction, and cataplexy associated with narcolepsy.
Pharmacokinetics of GHB are characterized by rapid oral absorption, with peak concentrations
in plasma 20-45 min after dosing, and half-life of 20-30 min. The majority of the dose is
eliminated completely within 4-8 h. Metabolism of GHB occurs via GHB dehydrogenase, which
transforms it into succinic semialdehyde and, by a second oxidation step with transformation
into succinic acid, it is then ultimately metabolized to water and excreted through breath as
carbon dioxide. However, GHB exposure is increased in patients with liver function impairment
and has been suggested presystemic (hepatic first pass) metabolism mediated by the CYP450
system in humans.
During the 1980s, easy access to GHB-containing products led to various unapproved uses,
including weight loss, bodybuilding and the treatment of sleeplessness, sometimes with
serious long-term effects. During the last years, GHB has become a major concern in emergency
rooms of some countries due to an important increase in the number of cases of intoxications.
Since the drug is both inexpensive and easy to ingest, it has been popular as a "party drug."
The calming and euphoric effects of GHB in low doses (20-30 mg/kg) have given the drug the
nickname "liquid ecstasy". At higher doses (> 50 mg/kg), the hypnotic effects are more
prominent and at doses >60 mg/kg coma, convulsions, and respiratory depression can occur. The
clinical hallmark of GHB poisoning is rapid onset of coma, with respiratory depression,
hypoventilation and bradycardia. Combination with alcohol potentiates these effects,
especially respiratory depression and hypotension.
Regular use of GHB is thought to be relatively higher in the lesbian, gay, bisexual, and
transgender community. Anecdotal evidence suggests that GHB use is increasing and this may be
driven in part by an increase in the incidence of chemsex. Chemsex is a specific form of
recreational drug use involving specific drugs such as GHB/γ-butyrolactone (GBL),
methylamphetamine and mephedrone, alone or in combination, to enhance or prolong sexual
sessions. Such sessions can last for several days, involve multiple partners and include high
risk behaviour.
Although the phenomenon of chemsex was initially limited to the metropolitan area of London,
it is getting spread across other big European cities, making of this an emerging global
health issue. Chemsex is especially common among men who have sex with other men (MSM) and in
people living with HIV (PLWH), with up to 50% of HIV-positive MSM reporting to be engaged in
chemsex in recent months.
Consumption of recreational drugs in PLWH has been associated with high-risk practices for
sexually transmitted diseases. In addition, use of drugs in patients taking antiretroviral
therapy (ART) might result in pharmacological interactions with potential risk of overdosing.
Noteworthy, widespread use of chemsex drugs has resulted in increased rates of overdose and
associated deaths, and Handley & Flanagan have reported an increase in the number of cases of
fatal poisoning with GHB, mephedrone and ketamine in England and Wales since 2008. Also,
GHB-associated deaths have been reported from the USA, Canada, Europe and Australia.
Cobicistat (GS-9350) is a pharmacokinetic enhancer that was developed to inhibit CYP3A
activity in a time- and concentration-dependent manner, thus boosting other antiretroviral
drugs. Results from clinical trials showed that it can increase the plasma exposure of
elvitegravir, atazanavir, and darunavir. Similarly, cobicistat increases the exposure to many
other xenobiotics. For example, it is well known that CYP3A4 inhibition leads to a
significant increase in concentrations of sildenafil and other erectile dysfunction agents,
and that a dose adjustment is needed in this scenario. Similarly, CYP3A4 inhibition increased
ketamine exposure in a small clinical trial in healthy volunteers.
There are two case reports in the literature of well documented life-threatening overdoses on
GHB and MDMA in HIV-positive patients on treatment with high-doses of ritonavir (600 mg bid).
However, the possibility for this drug interaction with the low doses of pharmacoenhancers
currently used (ritonavir 100 mg qd, cobicistat 150 mg qd) is still a matter for debate,
Despite data suggesting the possibility of drug interactions between cobicistat and GHB,
formal pharmacokinetic studies assessing this issue are lacking.
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