The Conference on Retroviruses and Opportunistic Infections (CROI 2016) heard results yesterday from the
first phase 2 (safety, acceptability and dose-finding) study of a long-lasting,
injectable formulation of the integrase-inhibitor drug cabotegravir for use as
pre-exposure prophylaxis (PrEP) in HIV-negative people.
The previous day the conference had heard a presentation of a study of the
same injectable drug, plus another injectable drug, rilpivirine, used as
treatment for people with HIV – see
this report.
In the cabotegravir PrEP study, dubbed the ECLAIR study, a
couple of surprises awaited the researchers. Firstly, the rate of absorption of
the drug into the body was faster than expected, meaning that an injection will
probably have to be given every eight weeks, instead of every 12 weeks as
hoped. Secondly, the duration and severity of pain and other effects of the
injections were greater than expected; however few people dropped out of the
study because of them, and three-quarters of participants said they would be
happy to continue taking cabotegravir injections as PrEP should it become
available.
The ECLAIR study lasted for 81 weeks altogether: presenter
Martin Markowitz did not present final results as the final, follow-up phase
has just finished. For the first four weeks, subjects took a daily oral
cabotegravir pill (or a placebo pill – one in five subjects took the placebo).
This oral phase was intended as a precaution to weed out any subjects who have
unusual adverse reactions to cabotegravir – since one of the problems of an
injectable formulation is that is cannot be suddenly stopped.
At weeks five, 17 and 29, three doses of injectable
cabotegravir were given. These consisted of 800 milligrams of cabotegravir
given as two two-millilitre injections, one in each buttock, or of saline as
placebo. The ‘injection phase’ was defined as lasting till week 41, 12
weeks after the last injection. There was then a follow-up phase of 40 weeks
till week 81; not all the data has yet been collected from this phase.
The study population consisted of men aged between 18 and 64
defined as being at low risk of HIV
infection (as this is largely a safety, not a prevention trial). Their average
age was 30.5 years, 57% were white and 32% African-American, and roughly 80%
were gay and 20% heterosexual.
One hundred and twenty-six men entered the trial, 105
allocated to cabotegravir and 21 to placebo.
During the first four weeks on the oral pill, eleven people
withdrew from the study who were taking cabotegravir, and one taking placebo.
During the injection period, a further seven people, all on cabotegravir,
withdrew, four of them due to intolerance of the injections. The fact that more
people withdrew in the oral phase was attributed by Dr Markowitz as being due
to caution on the part of the investigators at ensuring that no-one who showed
any possibility of side-effects went forward to the injection phase. In
particular, three subjects in the oral phase saw an increase in levels of
creatine phosphokinase, an enzyme that indicates injury to muscle tissue, and
although these were almost certainly not drug-related, they were withdrawn from
receiving an intramuscular injection as a precaution.
In the injection phase, the primary adverse event was injection
site reactions: these were almost universal in the subjects receiving
cabotegravir, with 93% reporting them, and 57% receiving placebo. Injection
site reactions largely consisted of pain in the muscle at the injection site.
Pain was generally mild in placebo recipients but in cabotegravir recipients
37% defined it as ‘moderate’ and 10% as ‘severe’ and lasting, on average, for
5.4 days. Other injection site reactions included itching, swelling and heat at
the injection site. The only non-local side-effect was fever, experienced by 7%
of men receiving cabotegravir.
Despite this, 62% of people on cabotegravir said they were
satisfied with their study medication, and 74% said they would be happy to
continue receiving it. In fact more people said they preferred the 12-weekly
injection to having to take a daily tablet.
Drug level measurements of cabotegravir showed that it was
absorbed by the body faster than expected. This meant that the peak level of
drug in the bloodstream, just after the injection, was higher than expected,
and the trough level, just before the next injection, was lower than expected.
A model had forecast that the peak level in blood would be three
micrograms per millilitre (mcg/ml) when in fact the average level was 5-6
mcg/ml, and the average trough level would be 1 mcg/ml when in fact it was
0.3-0 0.6 mcg/ml. This is of concern since it is close to the IC90,
the level of drug that cuts 90% of viral replication, and drug levels should be well
above this to ensure efficacy. The proportion of trial subjects whose trough
drug levels fell below the IC90 was 24% after the first injection,
31% after the second and 15% after the third.
Dr Markowitz said that the reason for the faster absorption
was unknown but it would probably mean that cabotegravir PrEP would have to be given
every two months rather than every three.
There were two cases of HIV infection in the study. One
person receiving placebo tested HIV positive at week 23. The other had received
cabotegravir, but tested positive at week 53, nearly six months after his last
cabotegravir injection. At this point he still tested HIV-antibody negatice but
had a viral load of over three million copies/ml, so it must have been a very
recent infection. He had no detectable cabotegravir in is bloodstream at this
point.
Dr Markowitz concluded that these results indicated that
cabotegravir injections were safe and, despite injection site reactions,
relatively well-tolerated. A parallel trial is happening in women and when this
has concluded the final decision will be taken about taking injectable
cabotegravir PrEP forward into a fully-fledged effectiveness trial, where it
would be compared with oral tenofovir/emtricitabine (Truvada).