[ Back to EurekAlert! ]

PUBLIC RELEASE DATE:
7-Aug-2014

[ | E-mail ] Share Share

Contact: Stephanie Xenos
sxenos@umn.edu
612-624-8723
University of Minnesota
www.twitter.com/UMNews

University of Minnesota research finds key piece to cancer cell survival puzzle

An international team led by Eric A. Hendrickson of the University of Minnesota and Duncan Baird of Cardiff University has solved a key mystery in cancer research: What allows some malignant cells to circumvent the normal process of cell death that occurs when chromosomes get too old to maintain themselves properly?

Researchers have long known that chromosomal defects that occur as cells repeatedly divide over time are linked to the onset of cancer. Now, Hendrickson, Baird and colleagues have identified a specific gene that human cells require in order to survive these types of defects.

"We have identified a gene that, as cells age, seems to regulate whether the cells become cancerous or not," Hendrickson said. "This gene has never been identified before in this role, so this makes it a potentially very important therapeutic target."

As cells divide their telomeres the DNA "caps" that protect the ends of chromosomes from damage shorten, leaving the chromosomes vulnerable to sticking to each other. In normal cells, this chromosome stickiness is a death knell a signal to defective-cell cleanup crews to move in and finish them off. Malignant cells, however, are somehow able to elude the cleanup crews.

The current research, published in the August 7 issue of the journal Cell Reports, identifies an essential component that allows older cells to evade death. Using sophisticated gene-targeting techniques to disable particular genes in human cells and then studying the impact on telomere fusion, the researchers found that cells escaped death only when the gene Ligase 3 was active but not when its action, which appears to promote fusion within like chromosomes rather than between different chromosomes, was blocked.

"Telomere dysfunction has been identified in many human cancers, and as we have shown previously, short telomeres can predict the outcome of patients with [chronic lymphocytic leukemia] and probably many other tumor types," said Baird. "Thus, the discovery that Ligase 3 is required for this process is fundamentally important."

Interestingly, the research was made possible by a chance meeting between Hendrickson, who is an expert in using gene targeting to create cells missing key components (such as Ligase 3), and Baird, who is a leading expert in analyzing telomeres. When the two discovered at a scientific conference that they were both looking at the role of Ligase 3 in cancer, they decided to collaborate.

"The collaboration paid off as we were able to uncover something that neither one of us could have done on our own," Hendrickson says.

Importantly, additional studies are already underway. In particular, the reliance on Ligase 3 appears, in turn, to be dependent upon the activity of another key DNA repair gene, p53.

"Since p53 is the most commonly mutated gene in human cancer, it now behooves us to discover how these two genes are interacting and to see if we can't use that information to develop synergistic treatment modalities," says Hendrickson.

###



[ Back to EurekAlert! ] [ | E-mail Share Share ]

 


AAAS and EurekAlert! are not responsible for the accuracy of news releases posted to EurekAlert! by contributing institutions or for the use of any information through the EurekAlert! system.