While modern antiretroviral therapy is highly safe and effective, agents that could be administered less frequently could improve convenience for people with HIV. A long-acting option could prove especially attractive for maintenance therapy once viral load is suppressed, or for pre-exposure prophylaxis (PrEP) in HIV-negative people.
William Spreen from GlaxoSmithKline and colleagues evaluated the safety and pharmacokinetics of a nanosuspension formulation GSK1265744 an investigational HIV integrase inhibitor similar to dolutegravir, plus TMC278-LA, a long-acting formulation of Janssen's approved non-nucleoside reverse transcriptase inhibitor rilpivirine (Edurant). GSK1265744 has shown good antiviral activity in a ten-day monotherapy study and is now in phase 2b development. A nanosuspension refers to tiny drug crystals suspended in a liquid, enabling it to remain active for longer in the body. Decreasing particle size increases the total drug surface area, allowing for a manageable injection volume.
This phase 1 trial enrolled 47 healthy, HIV-negative volunteers, 40 of whom received at least one injection. Just over half were women, most were white and the mean age was 40 years.
Participants were randomly allocated to four treatment cohorts. Due to limited safety data, all participants received a 14-day lead-in of 30mg/day oral GSK1265744 to assess its safety and tolerability. Following a seven-day 'wash-out' period, they then got a single 800mg 'loading dose' via intramuscular (IM) injection. After this they received:
- Cohort 1 – three doses of 200mg GSK1265744 via subcutaneous (SC) injection at weeks 4, 8 and 12 (no TMC278-LA).
- Cohort 2 – three monthly doses of 200mg GSK1265744 via IM injection at weeks 4, 8 and 12, plus 1200mg TMC278-LA via IM injection at week 8 and 900mg at week 12.
- Cohort 3 – three monthly doses of 400mg GSK1265744 via IM injection at weeks 4, 8 and 12, plus 1200mg TMC278-LA via IM injection at week 8 and 600mg at week 12.
- Cohort 4 – a second 800mg GSK1265744 dose via IM injection at week 12 (no TMC278-LA).
In all dose cohorts, plasma drug concentrations reached levels expected to be therapeutic within three days. Levels of both GSK1265744 and rilpivirine between doses remained well above the IC90, or 90% inhibitory concentration. GSK1265744 reached concentrations that reduced viral load in a previous monotherapy study of people with HIV.
Both drugs had a long PK 'tail', meaning concentrations remained high for a prolonged period and declined slowly. In practice, this would allow for some 'forgiveness' in case of missed or delayed doses, Spreen explained.
All regimens were generally safe and well tolerated. One participant discontinued the study during the oral lead-in phase due to dizziness, and one stopped during the injection phase due to transient skin rash. Overall, headache was the most common non-injection-related side-effect. There were no reported severe (grade 4) side-effects or laboratory abnormalities and no notable electrocardiogram changes.
Most participants reported injection-site reactions such as pain, tenderness, redness or nodules, but these were mostly mild and no one withdrew for this reason. Moderate injection-site pain was more common with IM compared with SC injections, but nodules were more common and somewhat larger with SC administration.
"Co-administration of injectable long-acting nanosuspensions [of GSK1265744 and TMC278] was safe and generally well tolerated in healthy adults," the researchers concluded.
"Monthly or quarterly dosing regimens achieved clinically relevant plasma concentrations" of GSK1265744 and TMC278, they continued, adding that these data support evaluation in longer-term clinical studies.
Spreen noted that a dosing-ranging study is pending, and researchers plan to look at various strategies involving oral lead-in or induction therapy with both drugs for up to six months before proceeding to long-acting injections.
