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02/17/05
-- Researchers at Purdue University have built and demonstrated a prototype
for a new class of miniature devices to study synthetic cell membranes in an
effort to speed the discovery of new drugs for a variety of diseases,
including cancer.
The
researchers created a chip about one centimeter square that holds thousands
of tiny vessels sitting on top of a material that contains numerous pores.
This "nanoporous" material makes it possible to carry out reactions inside
the vessels.
The goal is
to produce "laboratories-on-a-chip" less than a half-inch square that might
contain up to a million test chambers, or "reactors," each capable of
screening an individual drug, said Gil Lee, the project's leader and an
associate professor of chemical engineering.
"What we are
reporting now is a proof of concept," said Lee, one of three researchers who
wrote a paper that details new findings in the current issue (Feb. 15) of
the journal Langmuir. The two other researchers are Zhigang Wang, a
postdoctoral fellow at Purdue; and Richard Haasch, a research scientist at
the University of Illinois at Urbana-Champaign.
The work is
part of overall research being carried out by an interdisciplinary team of
scientists and engineers who are members of a Center for Membrane Protein
Biotechnology. The center was created at Purdue in 2003 through a grant from
the Indiana 21st Century Research and Technology Fund, established by the
state of Indiana to promote high-tech research and to help commercialize
innovations.
The vessels
discussed in the research paper are cylindrical cavities that are open at
the top and sealed at the bottom with a material called alumina, which
contains numerous pores measured in nanometers, or billionths of a meter.
Researchers
are working to duplicate how cell membranes function on chips in order to
test the potential effectiveness of new drugs to treat diseases. Membranes,
which surround cells and regulate the movement of molecules into and out of
the cells, contain a variety of proteins, some of which are directly
responsible for cancer's ability to resist anti-tumor chemotherapy drugs.
These proteins act as tiny pumps that quickly remove chemotherapy drugs from
tumor cells, making the treatment less effective. Cancer cells exposed to
chemotherapy drugs produce a disproportionately large number of the pumps,
causing the cells to become progressively more resistant to anticancer
drugs.
Engineers and
scientists in the Purdue center are trying to find drugs that deactivate the
pumps, which would make the chemotherapy drugs more effective. The
researchers are developing synthetic cell membranes to mimic the real thing
and then plan to use those membranes to create chips containing up to 1
million test chambers. Each chamber would be covered with a membrane
containing the proteins, and the chambers could then be used to search for
drugs that deactivate the pumps, Lee said.
Such an
advanced technology could be used to quickly screen millions of untested
drug compounds that exist in large pharmaceutical "libraries." The chips
could dramatically increase the number of experiments that are possible with
a small amount of protein.
"ItŐs been
very hard to study these proteins because they are difficult to produce in
large quantities," Lee said. "The devices we have created offer the promise
of making chips capable of running thousands of reactions with the same
amount of protein now needed to run only about 10 reactions."
Findings
being reported in the paper detail how researchers created the device with
the same "microfabrication" techniques used to make computer chips. The
reactors range in diameter from about 400 to 60 microns, or millionths of a
meter. Human hairs are about 100 microns wide.
"You can
think of it as a micro-petri dish for studying biochemical reactions," Lee
said.
The alumina
contains pores smaller than 100 nanometers, and the total volume of the
reactors varies from 1-10 nanoliters.
"What's
unique about this device is that the surface has nanometer-scale pores in
it," Lee said. "The concept is fairly simple - there is an inorganic porous
membrane - in this case alumina, which separates the reaction chamber from a
solution. The pores in this membrane are nanometer in scale, so they do not
allow proteins to readily pass through the membrane but will allow smaller
molecules to pass.
"This allows
us to do separation right in the reactor, which means we can do reactions
that could not be done before in such a small device. We can study membrane
proteins in a fundamentally new way, which is very important because many
future drugs to treat diseases will likely work by controlling proteins in
cell membranes."
Researchers
tested the devices with an enzyme that produces a blue color when combined
with a liquid that contains molecules small enough to easily pass through
the pores. The enzyme, which is a protein, was placed inside the vessels -
on the inner surface of the alumina membranes - and the liquid was placed
outside each vessel so that it covered the opposite side of the membranes.
When the liquid diffused through the membrane's pores, it mixed with the
enzyme, causing a reaction and turning blue in the process, which
demonstrated that the device works.
The Center
for Membrane Protein Biotechnology combines a diverse range of researchers,
from engineers to chemists, and pharmaceutical scientists to physicists. The
research is supported by the Bindley Bioscience Center, which is part of
Discovery Park, Purdue's hub for interdisciplinary research.
Source: Purdue University |