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Researchers discover new high throughput screening technique using spheroids to stop cancer cells from multiplying

ANI May 15, 2018

Researchers have found a new way to stop cancer cells from multiplying out of control, thereby blocking the growth and spread of tumours.

 


According to a study conducted by the Scripps Research Institute, there is an innovative new method to screen for potential cancer drugs. The technique makes use of tiny, three-dimensional ball-like aggregates of cells called spheroids. These structures can be used to interrogate hundreds or even thousands of compounds rapidly using a technique called high throughput screening. In fact, by using this approach, the team has already identified one potential drug for an important cancer gene.

"What's important about this research is that we're able to do studies using a form of cancer cells that is more physiologically relevant and better recapitulates how these cells appear in the body," said Timothy Spicer, one of the study's corresponding authors. "Until now, most of the research to screen for cancer drugs has used cells that are growing flat on a plate," added Louis Scampavia, one of the study's co-authors. "With these 3-D spheroids, we emulate much more closely what's found in living tissues."

The spheroids are 100 to 600 microns in diameter-equivalent to the thickness of a few sheets of paper. In contrast to single layers of cells normally used to screen for drugs, which tend to all grow at the same rate because they get the same exposure to oxygen and nutrients, the spheroids mimic what might happen in a tumor: Some cells are on the outside and some are on the inside.

The researchers focused on a cancer-driving protein called KRAS. The KRAS gene and other members of the related RAS gene family are found to be mutated in nearly one-third of all cancers. They are common in lung cancer, colorectal cancer, and especially pancreatic cancer. In fact, up to 90 percent of pancreatic cancers are driven by KRAS mutations, and the investigators used pancreatic cancer cell lines for the current study.

"In the past, KRAS has been a very tricky protein to target. People have spent several decades trying, but so far there has been little success," said Joseph Kissil, the other co-corresponding author. "The KRAS protein is relatively small, and that's made it hard to attack it directly. But the method of screening that we used in this study allowed us to come at the question in a different way."

The investigators performed what is called a phenotypic screen, which means they were looking for drugs that had an effect on cell growth but didn't have a preconceived idea about how they might work. "We came at this in an unbiased way," Kissil explained. "We were not trying to design something to attack a specific part of the KRAS protein. We were just looking for something that acted on some part of the pathway that's driving cell growth."

The investigators reported that they have already identified one compound that was previously not known to affect KRAS, called Proscillaridin A. The compound is similar to a class of drugs used to treat some heart conditions. Although the team says this particular drug is unlikely to be developed as a cancer treatment, it validates the approach of conducting drug screenings using spheroids. "It's unlikely we would have discovered this connection using standard 2-D methods," Scampavia said.

"From our perspective, this is a proof-of-principle study," Kissel added. "It shows you can look at libraries of drugs that have already been approved for other diseases, and find drugs that may also work for cancer. In theory, you could use this screening method for any line of cancer cells, and any mutation you want."

"We would love to use this research to create a pipeline for new oncology drugs," Spicer concluded. "Many of the most promising compounds may be overlooked with 2-D screening. This study provides direct evidence that screening for drugs using 3-D structures of cancer cells may be more appropriate." The study appears in the journal Oncogene.

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