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‘Genome Archeologists’ at University and UHN activate immune response against cancer

Researchers at University Health Network and the University of Toronto have identified silent and ancient DNA elements buried in our genomes that, when reactivated, can initiate a powerful immune response to kill colorectal cancer cells.

The researchers also discovered a key enzyme that human cancer cells use to prevent that immune response. Inhibiting this enzyme makes cancer cells more sensitive to new drug therapies that induce viral mimicry in mice, the study shows.Viral mimicry causes cancer cells to behave as though they have been infected, thereby activating the immune system to fight cancer like an infection.

The findings were recently .

“Humans acquired a series of ‘silent’ repetitive elements in our DNA over millions of years of evolution, but it has been unclear why or what purpose they serve,” says Daniel De Carvalho, an associate professor of medical biophysics in the Temerty Faculty of Medicine and a senior scientist at Princess Margaret Cancer Centre.

“As ‘genome archeologists,’ we set out to identify the function of these DNA relics and have found that under the right conditions they can be reactivated and stimulate our immune system.”

Daniel De Carvalho is an associate professor of medical biophysics in U of T’s Temerty Faculty of Medicine and a senior scientist at Princess Margaret Cancer Centre (photo by Perry King)

The first authors on the study are post-doctoral researchers Parinaz Mehdipour and Sajid Marhon, as well as Ilias Ettayebi, formerly a research technician in De Carvalho’s lab and now a medical student at U of T.

The enzyme that some cancer cells use to signal the immune system and undermine its response is called ADAR1. The discovery of ADAR1 explains how some cancer cells mount a defence and protect themselves from the immune response.

“These findings open up a new field of cancer therapies,” says De Carvalho. “They give us the opportunity to take advantage of these ancient repetitive DNA elements to fight cancer.”

Modulation of the immune response against tumour cells is one of the most rapidly changing and exciting areas in clinical oncology.

Researchers have made several key discoveries about the immune system’s interaction with cancer that have led to novel immunotherapy drugs, but a large proportion of cancer patients still do not respond to immunotherapy alone.

Illias Ettayabi

Ilias Ettayebi, a medical student at U of T, is one of the first authors of the study (photo courtesy PMCC)

In De Carvalho’s earlier discovery of viral mimicry, epigenetic drugs were shown to reactivate repetitive DNA elements and lead to production of double-stranded RNA, a molecular pattern that is also observed following viral infection. This leads to an antiviral response directed specifically against cancer cells.

In the current paper, the researchers identified the specific ancient repetitive DNA elements as SINEs (Short Interspersed Nuclear Elements). These SINEs usually lie quiet in our genome, having little known effect.

However, if activated by new epigenetic drugs, these SINES produce double-stranded RNA – a marker for infection – and can ultimately trigger an innate immune response. De Carvalho likens this response to an ancient dagger that can be used against cancer.

But cancer cells are wily and have evolved to evade detection by the immune system – even when the ancient DNA sequences are activated.

Carvalho and his team discovered that cancer cells strike back by making more of the ADAR1 enzyme, which disrupts the double-stranded RNA produced by the ancient DNA. This prevents the cancer cells from activating the immune system.

The researchers went on to demonstrate that deleting ADAR1 from cancer cells makes them vulnerable to epigenetic drugs that induce the antiviral response.

“Since the ADAR1 activity is enzymatic, our work provides an exciting new target for drug development efforts for a completely new class of drugs that could exploit these ancient weapons in our genome,” says De Carvalho.

The work was funded by the Canadian Institutes of Health Research, the Princess Margaret Cancer Foundation and the Ontario Institute for Cancer Research, with additional support from the Princess Margaret Cancer Centre Genomics.

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