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Researchers
make synthetic DNA 'barcodes' to tag pathogens,
providing an inexpensive, off-the-shelf monitoring
system
By
Bill Steele
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| ITHACA,
N.Y. -- A supermarket checkout computer can identify
thousands of different items by scanning the tiny barcode
printed on the package. New technology developed at
Cornell University could make it just as easy to identify
genes, pathogens, illegal drugs and other chemicals
of interest by tagging them with color-coded probes
made out of synthetic tree-shaped DNA. |

When DNA chains interact, adenine always bonds
to thymine, and cytosine always bonds to guanine.
Three DNA chains with complementary patterns along
half their length will combine to form a Y. Copyright © Cornell
University
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A
research group headed by Dan Luo, Cornell assistant
professor of biological engineering, has created "nanobarcodes" that
fluoresce under ultraviolet light in a combination
of colors that can be read by a computer scanner
or observed with a fluorescent light microscope.
Other
methods of identifying biological molecules that
are available or being developed mostly involve
expensive equipment, Luo said. "We wanted something
that could be done with inexpensive, readily available
equipment," he said. Several years ago researchers
created probes consisting of nanoscale bars of metal
actually etched with conventional bar codes. Since
then, most molecular tagging devices have been referred
to as "barcodes," even though there are no bars involved.
The researchers have tested their system using samples
containing various combinations of E. coli, anthrax
and tularemia bacteria and ebola and SARS viruses,
and have found the color codes could clearly distinguish
several different pathogens simultaneously.
The
research is described in a paper, "DNA fluorescence
nanobarcodes for multiplexed pathogen detections," by
Luo, Yougen Li, a former Cornell graduate student
now at California Institute of Technology, and Yen
Thi Hong Cu, a current graduate student, to be published
in the July 2005 issue of the journal Nature Biotechnology
and available after June 12 in the online version
of the journal
|

Several Ys can be joined to form a tree with many
open ends, to which dye molecules or probes can be
attached with precision. Copyright © Cornell
University
|
The
idea is one of several applications the researchers
have found for what they call "dendimer-like DNA," consisting
of many short Y-shaped strands of DNA linked together
in a treelike structure. The DNA that carries the
genetic code in living cells consists of two complementary
strands that attach to one another along their length.
But Luo's research purposely and completely ignores
the DNA's genetic coding properties. He uses DNA,
he said, as a "generic instead of a genetic material."
By
synthesizing three short strands of DNA, each of
which is complementary to one of the others along
half its length, the researchers can create a Y-shaped
structure. Combining several of these structures
creates a web with many branching ends. "While DNA
is flexible, the short strands used here are quite
rigid," Luo said. "A long piece of spaghetti is floppy,
but a short bit of it is quite stiff." |

Probes with different combinations of dye molecules will produce different ratios
of color intensity that can be read by a computer scanner or in some cases seen
with the naked eye. Copyright © Cornell
University
|
An
antibody or some other molecule that will bind to
the molecule to be detected is attached to one of
the loose ends of the DNA. To other ends are attached
molecules of fluorescent dye in a predetermined pattern.
For
example, one probe might contain four molecules
of green dye and one of red. Another might have
three molecules of green and two of red, and so
on. If a mixture of several probes is added to
a solution containing, for example, E. coli bacterial
DNA, only probes with a particular color code will
be programmed to bind to that DNA. The results
can be seen under a fluorescent light microscope
using colored filters that pass only one color
at a time. A signal in which the ratio of intensity
of green light is four times that of red light,
for example, identifies a "4G1R" probe.
The researchers say that up to 1,000 different codes
can be created using only three fluorescent dyes.
To amplify the signals, the researchers attached
many DNA probes to the surface of polystyrene microbeads
5.5 microns (millionths of a meter) in diameter.
The results can be read in several ways. One is in
a flow cytometer, in which samples move rapidly past
a window where a computer reads the color codes of
individual beads. Another is by dot blotting, in
which the sample is spread on a sheet of absorbent
paper and made visible to the naked eye. Or the color
can be observed directly through a fluorescent light
microscope, which is useful in situations where the
geographic distribution of the target molecules is
important, Luo said.
For
convenience, a computer can convert the subtle
differences in light intensity between, say 4G1R
and 3G1R, into "pseudo colors," perhaps
making one appear as orange and the other as pink,
to make the difference clear to a human eye.
The researchers point out that the nanobarcode detection
system does not require complex preparation of a
sample and can be applied to living cells. The technology
could be used in genomic research, clinical diagnosis,
drug testing, environmental monitoring and monitoring
for biological terrorism, they suggest.
Further
details on "tree-shaped" DNA appear in a
paper in Nature Materials (Vol. 3, Pg. 38-42, 2004).
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This
story has been adapted from a news release -
Diese Meldung basiert auf einer Pressemitteilung -
Deze
tekst is gebaseerd op een nieuwsbericht - |
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