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Engineering a ‘Trojan horse’ to sneak drugs into the brain
September 13, 2006
by Terry Devitt
 
 Beset by a host of debilitating and potentially fatal disorders, the human 
brain is in desperate need of a few good drugs. 
 The catch, however, is that nature has set up a roadblock known as the 
blood-brain barrier — intended to keep harmful agents out — that prevents 
clinicians from administering effective medicine. 
 Now, scientists have hit upon a scheme that could be used to sneak drugs past 
the barrier to treat afflictions such as Parkinson's, Alzheimer's, brain 
tumors and stroke. The idea, according to Eric V. Shusta, a University of 
Wisconsin-Madison professor of chemical and biological engineering, is to 
exploit human antibodies by transforming them into "Trojan horses" capable of 
ferrying payloads of drugs from the blood across the barrier and into the 
parts of the brain where they will do the most good. 
 Describing the new work in San Francisco today (Sept. 13) at a meeting of the 
American Chemical Society, Shusta described a system where antibodies capable 
of penetrating the blood-brain barrier could be used to carry drugs, DNA or 
even therapeutic nanoparticles to the brain. 
 "There are many drugs that show promise in the Petri dish," Shusta explains. 
"We just can't deliver them." 
 The scheme being explored by Shusta and his colleagues rests on the ability 
of antibodies, protein molecules that circulate in the blood and whose job, 
typically, is to seek out and neutralize foreign pathogens and toxins before 
they do harm. Antibodies are good at such work because they are built to 
recognize the surface features of targeted cells. 
 Using engineered yeast as microscopic factories to produce human antibodies 
customized to recognize the surface features of cells that compose the 
blood-brain barrier, Shusta has developed a set of unique antibodies that may 
one day be used to ferry drugs to specified regions of the brain. 
 "Antibodies bind tightly and specifically to cells, and we're trying to find 
those that home in on the blood-brain barrier endothelial cells," Shusta 
says. 
 When antibodies bind to cells, they can sometimes gain access to the cell 
and, potentially, open a gateway for the delivery of drugs or other 
therapeutic agents. 
 "We'd like to use the bloodstream to deliver drugs, but most small molecule 
pharmaceuticals as well as larger protein and gene medicines cannot pass the 
blood-brain barrier," he says. 
 With roughly 400 miles of blood vessels, the human brain is equipped with its 
own expansive delivery network for therapy — provided scientists are able to 
figure out a way to get past the blood-brain barrier. With different cell 
surface features in different parts of the circulatory system and also in 
different regions of the brain, it might be possible to customize antibodies 
to carry drugs to only those parts of the brain that would benefit from 
treatment. 
 So far, Shusta and his colleagues have identified a panel of unique 
antibodies that avidly bind to the plasma membranes of brain endothelial 
cells. In some cases, the antibodies engineered by the Wisconsin team have 
demonstrated the capacity to gain access to the cell, showing their 
"potential to act as molecular Trojan horses and allow blood-to-brain 
transfer of a wide range of pharmaceuticals." 
 The idea of using antibodies to tote drugs into the brain is not new, 
according to Shusta, but the antibodies used to date are not particularly 
efficient. The work of Shusta's group, however, has shown it is possible to 
identify novel transporting antibodies that could one day provide effective 
alternatives. "Ours is a novel system," Shusta adds. "We're still trying to 
work out the specifics, but we're pretty excited." 
 The work in Shusta's lab was supported by grants from the Whitaker 
Foundation, the Camille and Henry Dreyfus Foundation and the National 
Institutes of Health.

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