窪蹋勛圖厙

Skip to main content
MRI

MRI contrast agent locates and distinguishes aggressive from slow-growing breast cancer

FEATURED | September 25, 2017
STORY BY: EDITORIAL STAFF

窪蹋勛圖厙 researchers target tumor protein

A new magnetic resonance imaging (MRI) contrast agent being tested by researchers at 窪蹋勛圖厙 not only pinpoints breast cancers at early stages but differentiates between aggressive and slow-growing types. Doing both will help doctors find the right treatment, said Zheng-Rong Lu, the M. Frank Rudy and Margaret Domiter Rudy Professor of Biomedical Engineering at 窪蹋勛圖厙 and leader of the research. Theres no such technology available now that we know of. The gadolinium-based agent is also more efficient and safer than traditional agents, requiring a gadolinium dose 20-times smaller, easily flushing from the body and leaving no accumulation in tissues, the researchers found in tests with mouse models. The figure shows the different expressions of the biomarker (EDB-FN) and probe binding (ZD2) in slow-growing ER-positive breast cancer (not much yellow and red color representing low expression of the biomarker and low binding), and in triple- negative breast cancer (TNBC, high expression and high binding). As a result, the targeted contrast agent produced weak signal enhancement (brightness) in the former and strong signal (brightness) in the latter as referenced by the arrow. The figure shows the different expressions of the biomarker (EDB-FN) and probe binding (ZD2) in slow-growing ER-positive breast cancer (not much yellow and red color representing low expression of the biomarker and low binding), and in triple- negative breast cancer (TNBC, high expression and high binding). As a result, the targeted contrast agent produced weak signal enhancement (brightness) in the former and strong signal (brightness) in the latter as referenced by the arrow. At the low dosage, the agent lights up cancer biomarkers during scans, overcoming the low sensitivity of MRIs for imaging the markers. The research was published today (Sept. 25) in Nature Communications. To make the agent, Lu and colleagues at 窪蹋勛圖厙 combined commercially available tri-gadolinium nitride metallofullerene (Gd3N@C80), a highly efficient contrast agent, with a peptide labeled ZD2, which was developed in Lus lab. Compared to the gadolinium used in traditional agents, Gd3N@C80s structure is differentthe gadolinium ions are encaged in a hollow molecule of fullerene that looks like a soccer ball, Lu said. The cage prevents direct contact between the gadolinium and tissue, and the gadolinium will not be released, which prevents any kind of interaction with tissue. But the key technology for our targeted contrast agent is the peptide attached, Lu said. The lab applies ZD2 to the surface of the soccer ball. The peptide specifically targets the cancer protein extradomain-B fibronectin (EDB-FN). EDB-FN, which is associated with tumor invasion, metastasis and drug resistance, is highly expressed in the matrix around cancerous cells in many aggressive forms of human cancers. The illustration represents the concept of the work. The targeted contrast agent, ZD2-Gd3N@C80, binds to aggressive tumor and produces strong signal enhancement, but not in a slow-growing tumor, which allows detection and risk-stratification of breast cancer. The illustration represents the concept of the work. The targeted contrast agent, ZD2-Gd3N@C80, binds to aggressive tumor and produces strong signal enhancement, but not in a slow-growing tumor, which allows detection and risk-stratification of breast cancer. In testing on six mouse models, MRIs detected breast cancers in all cases. But the signal created by the accumulation of contrast molecules on three aggressive triple-negative breast cancers (MDA-MB-231, Hs578T and BT549) were significantly brighter. Because slow-moving ER-positive breast cancers (MCF-7, ZR-75-1 and T47D) produce less EDB-FN, fewer molecules attached. While detectable, the signal was muted. Coauthors of the study are biomedical engineering PhD students Zheng Han and Xiaohui Wu, research assistant Sarah Roelle and undergraduate student Chuheng Chen; and William Schiemann, the Goodman-Blum Professor of Cancer Research at the Case Comprehensive Cancer Center. Lus lab is now investigating ways to reduce the cost of producing the agent to make it more attractive for clinical use.
For more information, contact Bill Lubinger at william.lubinger@case.edu.