Just 1% of drugs investigated ever make it through the gamut of testing and approval to market. 

Technology that accommodates better precision in drug discovery and treatment is now being pursued.

Nemours Biomedical Research and the University of Delaware (UD) Department of Materials Science and Engineering have developed a patent-pending process to make 3D models work in HTS labs, allowing drug discovery to move into more meaningful screening systems.

Their progress is published in Analytical Biochemistry.

A traditional two-dimensional (2D) culture is a flat monolayer grown in a plastic dish, which, while containing tumour cells, does not necessarily mimic the three-dimensional nature of a tumour.

In other words, 2D doesn't reflect the human body.

Think of a sheet of tissue versus a ball of tissue.

The ball more accurately represents the tumour's composition and in vivo conditions.

One of the problems with applying 3D cell cultures to drug discovery has been the incompatibility of 3D models with high throughput screening (HTS) techniques in place in drug discovery labs.

Research in bridging this gap is hot as scientists, engineers and physicians work together to develop ways to connect 3D models and HTS to lead to more meaningful drug discovery.

The advantage of the new process is that it allows greater predictability of the effectiveness and toxicity of certain drug therapies before the drugs move into clinical trials which, in turn, is expected to lower the attrition rate of new medicines under development.

Because the 3D models offer a more in vivo-like context, researchers will be able to re-visit drug therapies that may have been ruled out or overlooked in the past using 2D models.

Dr. Sigrid Langhans, Head of the HTS Lab at Nemours, says the new process can mimic the physical properties of tumours and signalling pathways, which vary greatly between 2D and 3D models. 

Many drugs never make it to market because labs are not using appropriate models.

The process is a simple one with broad applicability and no need for additional specialised equipment.

Her focus at Nemours is on paediatric brain tumours - specifically medulloblastoma - but she says many labs will be able to duplicate the process to look into other types of pediatric and adult cancers.

"The technology is simple and can be tuned and adapted so that it's broadly applicable in other labs," she said.

Glioblastoma, the form of brain cancer that Sen. John McCain has, is aggressive and hard to treat in adults.

It is also one of those tumours where 3D culture technologies hold great promise.

There is potential, Langhans said, for the Nemours/UD process to further research and treatment if investigators are able to generate more models for glioblastoma and thus speed the discovery of more drug therapy options.

Source: Nemours Children's Health System