Communication networks discovered between tumuors and surrounding micro-environment
24 Feb 2015
When cancer cells develop in a previously healthy organ, the surrounding area, called the micro-environment, directly influences tumour growth and disease spread. But how this happens was previously unknown.
Now, a research team led by scientists at Weill Cornell Medical College and Houston Methodist Research Institute has identified complex communication networks between the tumours and surrounding complex milieu, which contains blood vessels, immune cells, connective tissue cells and structural cells.
The findings of this research, published on 19 February in Cell Reports, are the first that comprehensively look at crosstalk between a tumour and its micro-environment at this scale, said senior author Dr. Vivek Mittal, an associate professor of cell and developmental biology in cardiothoracic surgery at Weill Cornell Medical College. And the results, he said, could directly impact the way that cancer is treated.
"Current therapy rarely targets the organ cells that aid and abet tumor growth, so treatment of cancer is incomplete," said Dr. Mittal, noting that a tumor wounded by treatment can call on the microenvironment to survive.
"If you know how the microenvironment supports growth, progression and spread of cancer, you can begin to take apart these communications networks to find molecules that are vulnerable," Dr. Mittal says. "You might stop the cancer by disengaging the crosstalk."
In conducting this research, investigators studied a sub-type of non-small cell lung cancer - the 25 per cent that is driven by the Kras gene - because there is no effective treatment, with targeted therapies benefitting only 15 to 20 per cent of non-Kras patients.
There are 220,000 cases of lung cancer diagnosed each year, and it is the leading cause of mortality, accounting for more deaths than the three most common cancers combined, says Dr. Mittal, who is also director of the Neuberger Berman Foundation Lung Cancer Center Laboratory at Weill Cornell.
"Given the serious need for new therapies for lung cancer," he said, "decoding the tumor-micro-environment interplay will be a benefit to lung cancer treatment."
The researchers isolated specific individual cellular compartments directly from the lung tumor micro-environment and deep sequenced RNA of each compartment to accurately measure the activity of every gene. To explain their work, lead author Dr. Hyejin Choi compared lung cancer to a multi-layered city infrastructure.
"The lung tumour is very complex, like New York City," says Dr. Choi, a post-doctoral associate at Weill Cornell. "And in lung cancer, there are individual cell populations, which each have a specialty, like the city has varied specialists - doctors, lawyers, police officers, etc. - who contribute to the development and growth of the larger whole."
Like these specialists within New York City, individual populations of cells within a lung cancer micro-environment contribute to tumour progression and growth. Their research, Dr. Choi said, identified and characterised these cell populations, and figured out what their role is in the larger cancer.
Once they had mapped these cell populations and their contributions, researchers compared their findings to the micro-environment of normal mouse lung tissue and analysed data by developing a new computational program, known as Cell Cell Communication Explorer (CCCExplorer), which decodes how these genes are arranged within networks.
"We found that different populations of cells in the microenvironment talk to tumour cells through different signalling pathways," Dr. Mittal says. "This would not have been possible if we had examined whole tumour tissues and not individual components of the tumour."
"Cancer usually develops due to genetic mutations," he added. "Then its job is to get cell surrounding it involved in its survival and progression - and it does that in an amazing way by educating them and establishing cross-communication pathways. Using knowledge of these pathways and how they work opened up an unexplored area of cancer therapy."
While the pathways are identified, more research is needed to develop new therapeutic approaches, Dr. Choi said. Dr. Mittal agreed.
"So far we have only scratched the surface, and our goal is to identify all the networks and determine how they are modulated as a function of tumour progression," Dr. Mittal adds.
This research will then be used to understand how theses networks mediate responses or resistance to standard of care therapies in the clinic.
Moving forward, Dr. Mittal hopes that more research will continue to decode how this crosstalk works so that new therapies can be developed that are "not just targeted against mutations that cause the cancer," but keep the tumourd from growing with the help of the micro-environment.
Dr. Choi also hopes that this research is applied to other types of cancer, like breast cancer and prostate cancer, which also call on a micro-environment for help.
"With this information on the crosstalk between the tumor and micro-environment," she said, "we could apply a similar approach to other tumour types and target them, too."