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Nanoparticle-delivered 'suicide' genes slowed ovarian tumour growth

31 Jul 2009

Potential late-stage ovarian cancer therapy; currently none available - Diphtheria-encoding genes delivered to tumour site by nanoparticles - Laboratory research; possible human trials about 18 months away - Multimedia materials available below

Nanoparticle delivery of diphtheria toxin-encoding DNA selectively expressed in ovarian cancer cells reduced the burden of ovarian tumours in mice, and researchers expect this therapy could be tested in humans within 18 to 24 months, according to a report in Cancer Research, a journal of the American Association for Cancer Research.

Although early stage ovarian cancer can be treated with a combination of surgery followed by chemotherapy, there are currently no effective treatments for advanced ovarian cancer that has recurred after surgery and primary chemotherapy. Therefore, the majority of treated early stage cancers will relapse.

“This report is definitely a reason to hope. We now have a potential new therapy for the treatment of advanced ovarian cancer that has promise for targeting tumour cells and leaving healthy cells healthy,” said lead researcher Janet Sawicki, Ph.D., a professor at the Lankenau Institute for Medical Research.

Sawicki and colleagues at the Massachusetts Institute of Technology evaluated the therapeutic efficacy of a cationic biodegradable beta-amino ester polymer as a vector for the nanoparticle delivery of a DNA encoding diphtheria toxin suicide gene. These nanoparticles were injected into mice with primary or metastatic ovarian tumours.

To test the efficacy of this technique, the researchers measured tumour volume before and after treatment. They found that while treated tumours increased 2-fold, this was significantly less than the between 4.1-fold and 6-fold increase in control mice.

Furthermore, four of the treated tumours failed to grow at all, while all control tumours increased in size. Administration of nanoparticles to three different ovarian cancer mouse models prolonged lifespan by nearly four weeks and suppressed tumour growth more effectively, and with minimal non-specific cytotoxicity, than in mice treated with clinically relevant doses of cisplatin and paclitaxel.

Edward Sausville, M.D., Ph.D., an associate editor of Cancer Research and associate director for clinical research at the Greenebaum Cancer Center at the University of Maryland, said this report illustrates significant progress in targeted therapy.

“In oncology we have been studying ways to kill tumours for a long time, but much of this has run up against the real estate principle of location, location, location,” he said. “In other words, an effective therapy is not effective if it cannot get to the target.”

Sausville said a major accomplishment of this research is the multiple ways it can target ovarian cancer cells, as scientists were able to deliver diphtheria toxin genes, using a nanoparticle, to the actual tumour site (peritoneum) with a basis for selective activity in the cancer cells (how the toxin genes were regulated once inside the cells).

“A real plus of a cancer therapy like this is not just the functionality of the nanoparticle construct molecule, but the ability to deliver the toxin to the tumour cells,” said Sausville, who agrees that inception of clinical trials could be just 18 months away.