The anti-HIV drugs abacavir, efavirenz, lopinavir, and
ritonavir are all associated with an increased risk of heart attack in a
Canadian study published in the online edition of the Journal of Acquired Immune Deficiency Syndromes.
The research also showed that patients with HIV had twice
the risk of heart attack compared to matched HIV-negative controls.
However, the investigators are cautious about their
findings, writing: “Concerns remain about the presence of confounders that
could not be captured, in particular smoking, family history of cardiovascular
disease, creatinine, viral load and CD4 levels.”
Moreover, a
recent meta-analysis of randomised studies showed that therapy with one of
these drug - abacavir (Ziagen, also in the combination pills Kivexa and Trizivir) - did not
increase the risk of heart attack.
Nevertheless, the results of this latest study are of note
in light of the recent decision on cost grounds that most patients starting
HIV therapy in London should take an abacavir-based regimen.
A number of studies have now shown that patients with HIV
have an increased risk of cardiovascular disease. There has been debate about
the reasons for this. Untreated HIV infection may be a risk factor, but therapy
with some antiretroviral drugs has also been implicated.
In some observational research, both the nucleoside reverse
transcriptase inhibitor (NRTI) abacavir and the protease inhibitor Kaletra (lopinavir/ritonavir) have been
associated with a significant increase in the relative risk of heart attack.
Investigators in Montreal wished to clarify the impact of
HIV and antiretroviral therapy on the risk of heart attack.
They designed an observational study involving 7,053
HIV-positive patients who received care between 1985 and 2007. Each of these
patients was matched with up to five HIV-negative controls of the same sex and
similar age.
In addition, each HIV-positive patient who had a heart
attack was matched with to up to ten HIV-positive controls of the same sex and age
and who entered care at the same time.
Most of the patients were men (78%) and their median age was
37 years.
There were 139 heart attacks among the HIV-positive
patients, providing an incidence of 3.88 per 1000 person-years of follow-up.
This compared to a total of 226 heart attacks among the HIV-negative controls,
an incidence of 2.21 per 1000 person-years.
The investigators calculated that HIV infection doubled the relative
risk of heart attack (adjusted hazard ratio, 2.11; 95% CI, 1.69-2.63).
Incidence of heart attack was steady in the control
population, but increased by approximately 8% per year among the patients with
HIV. However, after adjusting for age and other confounding factors this
temporal trend ceased to be significant.
The125 HIV-positive heart attack patients were matched with
1084 HIV-positive controls who did not have a heart attack. The first heart
attack was recorded in 1989, and 92% of events occurred between 1997 and 2007.
Any exposure to abacavir (p =0,008), lopinavir (p = 0.004),
ritonavir (p < 0.01) and efavirenz (p = 0.004) was associated with an
increased risk of heart attack.
Recent therapy (within the previous six months) with
abacavir (p = 0.02), lopinavir (p = 0.02) and ritonavir (p = 0.003) was also
associated with an elevated risk of heart attack.
However, the investigators were eager to place these
findings into context. They
emphasised that the level of increased risk associated with each of these drugs
“is minimal compared to traditional risk factors such as smoking, family
history, hypertension, diabetes, and dyslipidaemia.”
The researchers were surprised by the association with
efavirenz, and comment: “Although efavirenz is known to have a small lipid
effect, no other biological mechanism can be offered at this time to explain
this finding.”
However, they suggest that the finding could be because
patients who were perceived to have an increased risk of cardiovascular disease
were treated with efavirenz rather than the protease inhibitor.
“Our study found an increased risk of AMI [acute myocardial
infarction] in HIV+ compared to HIV- individuals…we also found that any and
recent exposure to some antiretrovirals as associated with increased AMI risk,”
conclude the investigators.
But,they add: “Given limitation about data on confounders,
these data should be interpreted with caution and in the light of other data
existing on this subject. Meta-analysis of existing observational data, as well
as long term randomized-controlled trials that focus on cardiovascular
morbidity and mortality in HIV infected patients are needed to guide
therapeutic choices.”