Does
HIV Cause Cardiovascular Disease?
In the HAART era,
as the rate of death due to AIDS-related conditions has declined, cardiovascular
disease has become a growing concern for people with HIV and their providers.
Andrew Carr and Daniel Ory reviewed the current state of knowledge about
the relationship between HIV infection, antiretroviral therapy, and heart disease
in the November 28, 2006 issue of the open-access journal PLoS Medicine,
reprinted below.
HIV, Antiretroviral Therapy,
and Cardiovascular Disease Cardiovascular
disease is an increasing cause of morbidity in HIV-infected adults receiving antiretroviral
therapy (ART). ART, particularly protease inhibitors and to a lesser extent nucleoside
analogue reverse transcriptase inhibitors, can adversely affect lipid and glucose
metabolism [1]. Moreover, there is a strong correlation between ART duration and
the risk of myocardial infarction, an association in part linked to higher plasma
levels of total cholesterol and triglyceride and to lower levels of high-density
lipoprotein (HDL) cholesterol [2]. Paradoxically, interruption of ART also appears
to be associated with an increased short-term risk of cardiovascular disease [3].
These findings suggest that HIV itself may also increase cardiovascular risk,
and that control of HIV replication might reduce this risk. HDL
cholesterol levels are reduced in untreated HIV infection [4] and in healthy volunteers
exposed for a short term to the HIV protease inhibitors ritonavir-boosted atazanavir
and lopinavir [5,6]. In HIV-infected individuals who start ART that effectively
suppresses HIV replication, HDL cholesterol levels increase, regardless of whether
a protease inhibitor is used [7-9], implying that the HIV effect on HDL cholesterol
levels is greater than the ART effect. How
Does HIV Lower HDL Cholesterol Levels? The
pathogenesis of low HDL cholesterol levels in untreated HIV infection is unknown.
In a study recently published in PLoS Biology, Mujawar et al. investigated
whether these lower levels might be due to impaired cholesterol efflux from macrophages
[10], a process mediated by the ABCA1 cell-surface cholesterol transporter. ABCA1
lipidates apoA-I, the major apolipoprotein in HDL, and thus plays a central role
in formation of nascent HDL. Mutations in ABCA1 cause Tangier disease, which is
associated with low HDL cholesterol and accelerated atherosclerosis [11]. The
researchers found that expression of HIV nef, a protein that enhances HIV replication
and infectivity, specifically inhibited ABCA1-dependent cholesterol efflux from
macrophages (the precursors of foam cells in atherosclerotic plaque) and re-localized
ABCA1 to an exclusive plasma membrane distribution. While nef-transfected cells
exhibited increased apoA-I binding, apoA-I internalization was blocked, suggesting
that nef at the plasma membrane may prevent ABCA1 internalization and subsequent
apoA-I lipidation. As cholesterol is required for HIV replication [12], Mujawar
et al. next examined whether enhancing cholesterol efflux from HIV-infected macrophages
affected HIV replication. Using a liver X receptor (LXR) agonist to transcriptionally
upregulate ABCA1, cholesterol efflux was augmented, significantly reducing virion-associated
cholesterol and infectivity. What
Do the Findings Mean? Mujawar
et al. propose that HIV nef redirects cholesterol from an ABCA1-mediated efflux
pathway to virus-controlled cholesterol transport in order to ensure sufficient
cholesterol for virion assembly. The interruption of a host cholesterol trafficking
pathway by an intracellular pathogen is also employed by Toxoplasma gondii, in
which endocytosed low-density lipoprotein cholesterol is diverted to a specialized
vacuole to support parasite growth and replication [13]. Given that impaired ABCA1
function results in decreased HDL cholesterol and accelerated atherosclerosis
[14], the findings of Mujawar et al. provide a possible mechanism to explain low
HDL cholesterol in HIV infection and increased cardiovascular risk in HIV-infected
adults. It remains
to be determined, however, if this mechanism is the greatest contributor to these
low levels. If so, one would expect that HDL cholesterol levels would fall rapidly
after primary HIV infection and return to pre-infection levels with effective
ART that did not affect lipid metabolism. In addition, the observed reductions
might be inversely proportionate to plasma HIV RNA levels. Alternatively, low
HDL cholesterol levels may also be caused by ART-induced lipodystrophy. This ART
side effect is characterized by peripheral lipoatrophy and relative central adiposity
and is strongly associated with low HDL cholesterol levels as well as insulin
resistance and hypertriglyceridemia, all features of congenital lipodystrophies
in which abnormalities of ABCA1 have not been identified [2,15,16]. The
Strengths and Limitations of the Study The
findings of Mujawar et al. raise several important questions. Is the apparent
nef-stimulated decrease in ABCA1 protein levels due to ABCA1 degradation, or possibly
due to altered partitioning of ABCA1 into detergent-resistant lipid domains? Does
nef physically interact with ABCA1? Use of the myristoylation-deficient nef in
this study only suggests that nef must be targeted to the plasma membrane-likely
to cholesterol rafts [17]. Furthermore, experiments involving immunoprecipitation
of raft-associated proteins must be interpreted with caution, and should be followed
up with more rigorous studies (e.g., identification of interaction domains and
fluorescence resonance energy transfer) that provide support for a specific ABCA1-nef
interaction at the plasma membrane. Finally, might LXR ligands activate target
genes, other than ABCA1, that could attenuate virion-associated cholesterol? Treatment
of HIV-infected ABCA1-deficient macrophages with LXR ligands should establish
a definitive role for ABCA1 in countering HIV replication. Where
To From Here? The
present data provide a clue as to why HIV infection, as well as ART, might accelerate
atherosclerosis. The data support the shift away from a paradigm of delaying or
stopping ART to reduce the risk of cardiovascular disease and raise the possibility
that antiretroviral drugs without direct metabolic effects may actually reduce
cardiovascular risk. The data also emphasize the need for clinicians to consider
all the metabolic effects (in particular the ratio of total cholesterol to HDL)
of each antiretroviral drug, not just total cholesterol levels, in the management
of cardiovascular risk in HIV-infected adults. The
study by Mujawar et al. also has important implications for developing new approaches
for suppression of HIV replication. Selective LXR modulators under active development
for treatment of atherosclerosis may prove useful as ART. The
long-term effects of each antiretroviral drug on HDL cholesterol, as well as other
lipid and glycemic parameters, need to be more completely analyzed in randomized
trials, as well as in shorter healthy volunteer studies. It remains to be determined
whether new antiretroviral drug classes, such as HIV fusion, CCR5, and integrase
inhibitors, will be free of these metabolic complications.
12/01/06
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Source
A
Carr, D Ory. Does HIV Cause Cardiovascular Disease? PLoS Medicine 3(11): e496.
doi:
10.1371/journal.pmed.0030496. November 28, 2006. | |
