In our bodies, we all have genes working hard to prevent cancer. If they don’t do their job properly, rogue cells can mutate and develop into the life-threatening disease.
The malfunction of one so-called “super tumour suppressor gene” known as p53 causes at least half of all cancers. When it works, p53 regulates how a cell reacts to various stresses and can instruct a rogue cell to die or stop multiplying.
The researchers found particular genes are critical in p53’s role in preventing cancer development. Picture: Getty Images
Researchers have known about the significance of p53 in protecting us from cancer for about 30 years, but until now no one has explained how it prevents cancer development.
In a world-first, Melbourne scientists have found that a special group of genes that function in the body’s normal DNA repair process are critical to p53’s effectiveness in preventing the development of cancer.
The team discovered that the DNA repair gene MLH1 and as well as other related genes are critical to p53’s ability to prevent the development of B-cell lymphomas.
This new information could help doctors better identify patients with an increased risk of certain cancers. It could also lead to safer, more effective treatments.
Walter and Eliza Hall Institute (WEHI) researchers with honorary University of Melbourne appointments - Dr Ana Janic, Associate Professor Marco Herold and Professor Andreas Strasser - led the study, published in Nature Medicine.
Dr Janic says that while the results will take several years to translate into clinical practice, the discovery is ground-breaking.
She says it paves the way for researchers to investigate whether the DNA repair process is as important in cancers other than lymphoma, like pancreatic and colon cancer.
“It is defects (mutations) in this gene that’s actually causing 50 per cent of human cancers,” Dr Janic says. “It’s really exciting because we’ve kind of opened the window for many new discoveries in this area.”
Dr Janic says that knowing MLH1 (and related DNA repair factors) functions as a powerful weapon for p53 should eventually help doctors diagnose patients earlier and prescribe safer, more targeted cancer treatments.
Knowing that MLH1 functions as a powerful weapon for p53 should eventually help doctors diagnose patients earlier. Picture: Shutterstock
“For instance, if a patient has lymphoma with a mutation that disables the DNA repair mechanism, doctors will now know to avoid certain DNA-damaging treatments, like chemotherapy, that may only make the cancer more aggressive,” she says.
The discovery could help many people with cancer but particularly those with a condition called Li-Fraumeni Syndrome, a familial predisposition to a range of cancers that is caused by inherited mutations in – you guessed it – p53.
According to Dr Janic, p53 is mutated in close to 70 per cent of colon and pancreatic cancers, so this discovery could also have a significant impact on understanding and treating these diseases.
“We are keen to test whether genes involved in the DNA repair process might also play a role in helping p53 to prevent the development of these highly prevalent and, in the case of pancreatic cancer, highly deadly cancers,” she says.
The next step is to investigate how human cells react to cancer inducing stresses in tissue culture and eventually develop more personalised treatments for individual patients.
Professor Strasser says understanding how p53 works is a “holy grail” for cancer researchers.
“We are planning to continue our studies into the genes that are regulated by p53, digging deeper into understanding other potential processes that might impact its function,” he says.
Dr Herold says their findings stemmed from a screen of more than 300 genes directly regulated by p53 to identify which ones were critical for its tumour-suppressing function, demonstrating the importance of detailed functional analyses.
“It was amazing to find that the loss of the DNA repair gene MLH1 prevented p53 from functioning properly, causing the development of lymphoma,” he says. “And when MLH1 was put back into the equation, tumour development was significantly stalled.
This research opens up the potential for further exploration of how DNA repair genes help p53 prevent cancer development. Picture: Shutterstock
“This led us to explore other DNA repair genes and it has become clear just how important the whole DNA repair machinery is to p53’s ability to prevent cancer development.”
Like many discoveries at this level, Dr Janic says the results were a surprise as researchers had no idea that p53 worked in this way. But, it also means there’s a lot of potential for further exploration.
“We actually found that the DNA repair (MLH1) is one of the most critical processes for this,” she says. “This was an absolutely novel discovery for us and for the field. The field is very excited about our work and where this will lead in the near future.”
This work was supported by the Australian National Health and Medical Research Council, Cancer Council Victoria, Australian Phenomics Network, Cancer Australia, the Leukemia & Lymphoma Society of America, Marie Curie Actions and Beatriu de Pinos, and the Lady Tata Memorial Trust.
SethRogen-Not on June 12nd, 2018 at 02:32 UTC »
Hey, I have Li-Fraumeni Syndrome! Don’t see that in the news everyday!
huwmo on June 12nd, 2018 at 02:05 UTC »
All these people going on about clickbait because they learned that p53 was tumour suppressor back in their undergrad didn't read the article. The scientists aren't claiming the discovery of the role of p53, they discovered the mechanism. Clicking the article and reading it beyond the headline will make that pretty clear. Also, take note that this article is written for a more generalised audience, so don't expect too much detail.
This is the paper's abstract: "It has long been assumed that p53 suppresses tumor development through induction of apoptosis, possibly with contributions by cell cycle arrest and cell senescence1,2. However, combined deficiency in these three processes does not result in spontaneous tumor formation as observed upon loss of p53, suggesting the existence of additional mechanisms that are critical mediators of p53-dependent tumor suppression function3,4,5. To define such mechanisms, we performed in vivo shRNA screens targeting p53-regulated genes in sensitized genetic backgrounds. We found that knockdown of Zmat3, Ctsf and Cav1, promoted lymphoma/leukemia development only when PUMA and p21, the critical effectors of p53-driven apoptosis, cell cycle arrest and senescence, were also absent. Notably, loss of the DNA repair gene Mlh1 caused lymphoma in a wild-type background, and its enforced expression was able to delay tumor development driven by loss of p53. Further examination of direct p53 target genes implicated in DNA repair showed that knockdown of Mlh1, Msh2, Rnf144b, Cav1 and Ddit4 accelerated MYC-driven lymphoma development to a similar extent as knockdown of p53. Collectively, these findings demonstrate that extensive functional overlap of several p53-regulated processes safeguards against cancer and that coordination of DNA repair appears to be an important process by which p53 suppresses tumor development."
idaholives on June 11st, 2018 at 23:12 UTC »
My mom and grandfather both had lymphoma. One at stage 0, the other at stage 4 with metastases in the lungs, brain, and liver. Both were completely cured by Rituximab.
I will sing the praises of modern medicine and it's ability to cure with greater efficiency and certainty. But I'd prefer to not get this shit in the first place. Maybe with gene therapy that will be possible. Thanks, Melbourne.