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August 15, 2005

Hybrid Nanostructure Programmed to Fluoresce in Presence of Enzyme Activity

Combining brightly fluorescent quantum dots with gold nanoparticles using a linker that can allow the two nanomaterials to go their separate ways, researchers at Rice University's Center for Biological and Environmental Nanotechnology have developed a "smart" beacon that is programmed to light up only when activated by specific enzymes known as proteases. Altered expression of particular proteases is a common hallmark of cancer, atherosclerosis, and many other diseases.

Nanoparticles allow cells on the floor of a mouse brain ventricle to express the gene for green fluorescent protein.

Illustration of "smart" probe concept. Quantum dot surrounded by gold nanoparticles connected via degradable peptides (left). Cleavage of peptide separates gold nanoparticles (middle) enabling quantum dots to glow brightly (right).

Courtesy: Rebekah Drezek, Ph.D., Rice University

Writing in the journal Biochemical and Biophysical Research Communications, a team led by Jennifer West, Ph.D., and Rebekah Drezek, Ph.D., describe the development of a new nanoprobe for visualization of proteolytic activity in vivo. "The idea is to develop a ‘smart’ nanostructure that is dark in its original state but lights up very brightly in the presence of enzymatic activity associated with a particular disease process," says West. "Other groups have used targeted nanostructures including quantum dots for molecular imaging, but they have never been able to adequately solve the problem of clearly distinguishing between the ‘cancer is here’ signal and the background light which arises from nanostructures not specifically bound to their molecular targets."

West and Drezek’s team technology solved this longstanding problem by using quantum dots that give off light in the near-infrared region of the optical spectrum, a rare portion of the spectrum that has no background component in biomedical imaging. Near-infrared light also passes harmlessly through skin, muscle and cartilage, so the new probes could alert doctors to tumors and other disease sites deep in the body without the need for a biopsy or invasive surgery.

Nanoparticles allow cells on the floor of a mouse brain ventricle to express the gene for green fluorescent protein.

Quantum dots (red color in image above) glowing after targeting to cancer cells.

Courtesy: Rebekah Drezek, Ph.D.
Rice University

The probe's design makes use of a technique called "quenching" that involves tethering a gold nanoparticle to the quantum dot to inhibit luminescence. The tether, a peptide sequence measuring only a few nanometers in length, holds the gold close enough to prevent the quantum dot from giving off its light.

In their test system, the Rice team used a peptide tether that is cleaved by the enzyme collagenase. The researchers first showed that luminescence of the quantum dots was cut by more than 70 percent when they were attached to the gold particles. They remained dark until the nanostructures were exposed to collagenase after which the luminescence steadily returned.

"There is currently a critical need for methods to simultaneously image the activity of multiple proteases in vivo," said Drezek. "This is important not only for early detection of several diseases, but perhaps more significantly, in understanding and monitoring the efficacy of therapeutic interventions, including the growing class of drugs that act as protease inhibitors. What is particularly powerful about the protease imaging probes described in this study is the combination of the contrast enhancement achievable through an activateable probe with the imaging advantages provided by the brightness, photostability, and tunability of quantum dots."

This work is detailed in a paper titled, "Protease-activated quantum dot probes." An abstract is available through PubMed.
View abstract.


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