News from the field of HIV research has been pretty promising of late  — this summer, we heard good news that antiretroviral treatment is superbly effective, at least when it's used correctly. And thanks to some video gamers, scientists' understanding of proteins involved in HIV keeps getting better. 
Now researchers have another tool in their arsenal: Stripping the virus itself of its ability to trick the human immune system. 
 HIV infection sends the immune system into overdrive and eventually  exhausts it, which is what leads to AIDS. But removing cholesterol from  HIV seems to cripple the virus' ability to over-activate part of the  immune system, so it could potentially lead to a vaccine that lets the  adaptive immune system attack and destroy the virus — just as it would  if HIV was any other pathogen. 
Dr. Adriano Boasso, an immunologist and research fellow at Imperial  College London, said keeping the body’s first-responder immune cells  quiet could have some benefits — the whole system may not burn out so  quickly, and could potentially fight off HIV.
“Think of the immune system as a car. HIV forces the car to stay in  first gear, and if you do that too long, the engine is not going to last  very long,” he said in an interview. “But if we take the cholesterol  away, HIV is not capable of attacking the immune system quite as well.  Practically, what we’ve done is turn HIV into a normal jump-start of a  car.”
Viruses replicate by invading cells and hijacking their machinery, which  they use to churn out new copies of their genetic material. Among the  repurposed material is cholesterol, which is important in maintaining  cellular fluidity, something viruses require to interact with other  cells. (This is not related to the way everyone thinks of cholesterol,  which is cholesterol in the blood. That type of cholesterol, made of  high-density and low-density lipoproteins, is related to heart disease,  not HIV and AIDS.)
HIV quickly activates plasmacytoid dendritic cells, or pDCs, which  are the first immune cells that respond to the virus. PDCs produce  molecules called interferons, which both interfere with the virus’  replication and also switch on adaptive immune cells, like T cells.  Boasso and other researchers believe this hyperactivation weakens the  secondary immune system, undermining the body’s ability to respond.
But in a new study, Boasso and colleagues show that removing the  cholesterol changes HIV, so that it cannot activate the pDCs like it  normally would. By preventing these first responder cells from turning  on in the first place, the secondary responders — the T cells — can  organize a more effective counterassault. 
 “Modifying the virus affects the way the immune system sees it,”  Boasso said. He said it’s like removing the weapons from HIV’s arsenal:  “By removing cholesterol, we can turn those little soldiers into an  armorless enemy, which can be recognized by the opponent’s army.”
Emily Deal is a postdoctoral fellow at the Gladstone Institute of  Virology and Immunology, which is affiliated with the University of  California-San Francisco. She studies pDC activation in viral  infections, and said the cholesterol removal is allowing less of the HIV  into the dendritic cells in the first place — which means there’s less  of the virus for the cells to detect, which leads them to produce fewer  interferons.
But keeping the pDCs from turning on could be both good and bad, she said.
 “What is better for the host in the long run? Is it better to  suppress replication early on, but potentially have some of your T cells  die? Or what are the lon-term effects of having replication proceed in  the absence of interferons, but have your T cells live?” she said. "It's  a complicated system."
Ideally, further studies would look at this give-and-take  relationship in monkeys, so researchers could determine if a  de-cholesterolized version of HIV could be an effective form of vaccine,  she said. 
 “I think it has a shot," she said. "However, pDCs control a lot of  the immune system, and if they’re not getting turned on at all, that may  have other effects. If you’re trying to use it as a vaccine, it may not  induce enough of a response to be protective." 
Boasso said the de-cholesterolized HIV could be studied for use in a  potential vaccine, but it’s difficult to stimulate the immune system to  fight off an invader when the system itself is the target. 
 “There’s going to be a lot of work to do,” he said.
by "environment clean generations" 

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