Gen Pharmacol. 1997 Oct;29(4):497-511. Unique Identifier : AIDSLINE
The inhibitory effects of polyanionic substances on the replication of
herpes simplex virus (HSV) and other viruses were reported almost four
decades ago. However, these observations did not generate much interest,
because the antiviral action of the compounds was considered to be
largely nonspecific. Shortly after the identification of human
immunodeficiency virus (HIV) as the causative agent of the acquired
immune deficiency syndrome (AIDS) in 1984, heparin and other sulfated
polysaccharides were found to be potent and selective inhibitors of
HIV-1 replication in cell culture. Since 1988, the activity spectrum of
the sulfated polysaccharides has been shown to extend to various
enveloped viruses, including viruses that emerge as opportunistic
pathogens e.g., herpes simplex virus [HSV] and cytomegalovirus [CMV]) in
immunosuppressed (e.g., AIDS) patients. As potential anti-HIV drug
candidates, sulfated polysaccharides offer a number of promising
features. They are able to block HIV replication in cell culture at
concentrations as low as 0.1 to 0.01 microgram ml-1 without toxicity to
the host cells at concentrations up to 2.5 mg ml-1. We noted that some
polysulfates show a differential inhibitory activity against different
HIV strains, suggesting that marked differences exist in the target
molecules with which polysulfates interact. They not only inhibit the
cytopathic effect of HIV, but also prevent HIV-induced syncytium (giant
cell) formation. Furthermore, experiments carried out with dextran
sulfate samples of increasing molecular weight and with sulfated
cyclodextrins of different degrees of sulfation have shown that
antiviral activity increases with increasing molecular weight and degree
of sulfation. A sugar backbone is not strictly needed for the anti-HIV
activity of polysulfates because sulfated polymers composed of a
carbon-carbon backbone have also proved to be highly efficient anti-HIV
agents in vitro. Other, yet to be defined, structural features may also
play an important role. Sulfated polysaccharides may act synergistically
with other anti-HIV drugs (e.g., azidothymidine [AZT]). They are known
to lead very slowly to virus-drug resistance development and they show
activity against HIV mutants that have become resistant to reverse
transcriptase inhibitors, such as AZT, tetrahydro-imidazo [4,5,l-jk]
[1,4]-benzodiazepin-2(1H)-thione (TIBO) and others. From studies on
their mechanism of action we concluded that polysulfates exert their
anti-HIV activity by shielding off the positively charged sites in the
V3 loop of the viral envelope glycoprotein (gp120). The V3 loop is
necessary for virus attachment to cell surface heparan sulfate, a
primary binding site, before more specific binding occurs to the CD4
receptor of CD4+ cells. This general mechanism also explains the broad
antiviral activity of polysulfates against enveloped viruses. Variations
in the viral envelope glycoprotein region may result in differences in
the susceptibility of different enveloped viruses to compounds that
interact with their envelope glycoproteins. The efficacy of polysulfates
in the therapy and/or prophylaxis of retroviral infections and
opportunistic infections remains to be demonstrated both in animal
models and humans. It is important to consider not only treatment of
patients who are already infected with HIV, but also prophylaxis and
protection from HIV and/or other virus infections. Because (i) sexual
transmission is responsible for the large majority of HIV infections
worldwide; (ii) this transmission is mostly mediated via mononuclear
cells that infect epithelial cells of the genital tract; and because
(iii) polysulfates effectively inhibit cell-cell adhesion, polysulfates
may be considered as potentially effective in a vaginal formulation to
protect against HIV infection.
*Algae *Antiviral Agents/PHARMACOLOGY *Polysaccharides/PHARMACOLOGY