<img height="1" width="1" style="display:none" src="https://www.facebook.com/tr?id=799546403794687&amp;ev=PageView&amp;noscript=1">
placeholder

Weekes shares clinical trail results

Default sub title

minute read

Written by Danielle Zieg on August 11, 2014

Colin Weekes, MD, PhD, CU Cancer Center investigator and assistant professor in the Division of Oncology at the CU School of Medicine, discussed recent researching findings this spring at the 50th Annual Meeting of the American Society for Clinical Oncology (ASCO).

He described the results of a phase I clinical trial of the investigational agent DMOT4039A against pancreatic and ovarian cancers. In this early clinical trial with the goal of identifying possible risks and defining likely dosages, the drug was well tolerated and, in some patients, showed initial evidence of anti-cancer activity.

The drug is a combination of a chemotherapeutic agent with an antibody, technically called an antibody-drug conjugate (ADC). Just as cells of the immune system use antibodies to recognize pathogens, researchers in this study designed antibodies to recognize a protein over-expressed by these cancer cells, namely the protein mesothelin. The engineered antibodies attach to mesothelin on the cells, and thus bring along their chemotherapeutic cargo directly to the mesothelin-rich cancer cells.

“The deal is that the cell has to express the protein. The more it’s expressed only on cancer cells, the more targeted the therapy becomes,” said Weekes.

A similar antibody-drug conjugate approach is used by the breast cancer agent T-DM1, which attaches chemotherapy to an antibody that seeks the HER2 protein in HER2+ breast cancers.

The current phase I clinical trial, sponsored by the agent’s manufacturer, Genentech, was carried out at the University of Colorado Cancer Center, in the Netherlands, and at three Mayo Clinic locations in Scottsdale, Ariz., Jacksonville, Fla. and Rochester, Minn. The study enrolled 71 patients, with no dose-limiting toxicities seen at maximum study dosage.

“For tumors that overexpress a specific protein ADCs may make sense,” Weekes said. “But for other tumors with specific genetic abnormality that doesn’t result in overexpression of a protein, it won’t make sense.”

Additionally, Weekes explained, the creation of antibody-drug conjugates requires technically sophisticated procedures to create “linker constructs” between drug and antibody. “You can’t just put any drug on these things,” Weekes said.

But in tumors that overexpress certain proteins, or perhaps in tumors that can be made to overexpress certain proteins, the strategy of targeting cancers with antibody-drug conjugates remains promising. The agent DMOT4039A is now being evaluated for further human trials.

Related Stories