Doctors have long been mystified as to
why HIV-1 rapidly sickens some individuals, while in others the virus
has difficulties gaining a foothold. Now, a study of genetic variation
in HIV-1 and in the cells it infects reported by University of Minnesota
researchers in this week’s issue of PLOS Genetics has
uncovered a chink in HIV-1’s armor that may, at least in part, explain
the puzzling difference – and potentially open the door to new
treatments.
Suspecting differential susceptibility to
HIV-1 might be related to genetic variations in this system, a research
team led by doctoral student Eric Refsland and Reuben Harris of the
University’s College of Biological Sciences and Medical School took a
closer look. First, the researchers found that HIV-1 infection boosts
the production of one kind of APOBEC3, APOBEC3H – suggesting it’s a key
player in fighting back. Then, using an experimental technique known as
separation of function mutagenesis, they discovered that different
people have different strengths/potencies of APOBEC3H, with some
proteins expressed stably and others inherently unstable. The stable
variations, the researchers found, were able to successfully limit
HIV-1’s ability to replicate if the infecting virus had a weak version
of Vif – but not for HIV-1 viruses that had strong Vif.
“This work shows that the competition
between the virus and the host is still ongoing,” Refsland says. “The
virus hasn’t completely perfected its ability to replicate in humans.”
Armed with this clearer picture of the
multifaceted interactions between Vif and APOBEC3, Harris says, the next
step is to figure out how to stop Vif from disabling the APOBEC3
enzymes. “One could imagine drugs that stop Vif from binding with
APOBEC,” he said. “This is a bonafide HIV killing pathway, and we just
have to devise clever ways to activate it in infected persons. Such an
approach could indefinitely suppress virus replication, and even result
in curing it.”
Source: sciencedaily.com
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