Pharmacokinetic Study in Healthy Volunteers Clinical Trial
Official title:
Extracellular and Intracellular TFV/FTC Residues After a Single Dose in HIV-Negative Men and Women: Implications for Pre-exposure HIV Prophylaxis Dosing of Truvada®
This open-label, non-blinded, pharmacokinetic (PK) study will assess both tenofovir and emtricitabine (components of Truvada) concentrations within genital tract of male and females after a single dose of Truvada®. Concentrations of the active drug will be measured in blood (women and men), cervicovaginal aspirates and vaginal tissue (women only), seminal fluid and rectal tissue (men only). Samples will be obtained at 24 hours (1 day), 48 hours (2 days), 5 days, 7 days, 10 days, and 14 days post-dose. Each subject will undergo 2 biopsy days, at least 72 hours apart. Additionally, tissue samples will be evaluated ex-vivo for HIV infectivity.
An estimated 80% of HIV infections worldwide are acquired through sexual transmission.1
Viable methods of preventing the sexual transmission of HIV are urgently needed, especially
in resource-poor countries. As these countries now have increased access to generic
antiretroviral medications, oral administration of antiretroviral drugs as pre-exposure
prophylaxis may serve as a feasible, minimally invasive mechanism of preventing the sexual
transmission of HIV globally.
Antiretroviral prophylaxis with the combination of tenofovir and emtricitabine has recently
been investigated by the U.S. Centers for Disease Control and Prevention in a series of
studies with rhesus macaques. Researchers developed a rectal inoculation model using
concentrations of Simian HIV (SIV) that were representative of HIV exposure in humans. With
this model, researchers demonstrated that standard doses of tenofovir disoproxil fumarate
delayed, or partially protected, animals from the acquisition of Simian HIV during a 14-week
time period. In this same model, high dose tenofovir was fully protective from infection.2
However, it is unknown how concentrations in the macaque mucosal surfaces compare to that in
humans. Notwithstanding, a number of clinical studies are currently investigating daily
dosing of tenofovir or tenofovir with emtricitabine for pre-exposure prophylaxis.3
Since daily dosing of antiretrovirals for pre-exposure prophylaxis is not sustainable
long-term, other coitally-dependent (episodic) dosing strategies are needed. However, the
extent to which these drugs concentrate in tissues, and the duration of intracellular
phosphate exposure after single doses, is currently unknown. This information is required to
inform the potential of success with these dosing strategies.
At steady-state concentrations, the mean blood plasma half-life (t½) of tenofovir and
emtricitabine are 15.9 hours and 10.7 hours, respectively. 4 However, the intracellular t½
of tenofovir diphosphate and emtricitabine triphosphate are >60 hours and 39 hours,
respectively.5 The long intracellular t½ of the active forms of these drugs might hold
advantages for episodic dosing. However, the long t½ might also hold disadvantages in terms
of the development of viral resistance mutations. This phenomenon (the development of
resistance after a single dose of a long t½ drug), has been previously seen with nevirapine
given during delivery to HIV-infected women to prevent mother to child transmission of HIV.6
However, these women were chronically infected, rather than newly infected, as would be the
case with populations exposed to prevention strategies.
The proposed study aims to augment the information gathered in previous studies by examining
intracellular and extracellular tenofovir and emtricitabine drug concentrations in various
human compartments after a single dose, and to describe the potential for HIV infectivity in
selected tissue samples obtained from these compartments.
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