New Straits Times

Clues on breast cancer recurrence

The findings are important to identify women at risk of developing it again

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FOR breast cancer survivors, the risk of tumours returning casts a long shadow, with recurrence possible up to two decades after a diagnosis. But new research can help identify and treat those most in danger. Doctors have traditiona­lly relied on factors such as the size and grade of a tumour during diagnosis, the involvemen­t of lymph nodes and a patient’s age when determinin­g the risk of relapse. But the rate at which breast cancer recurs, and why it does so, remains “poorly understood”, according to the study published recently in the journal Nature.

In a bid to change that, the researcher­s turned to data from over 3,000 breast cancer patients diagnosed in the United Kingdom and Canada between 1977 and 2005. Nearly 2,000 of the cases included molecular data about the cancers that provided the researcher­s with detailed informatio­n about the tumours.

The data was used to develop a computer model that identified four subgroups with “exceedingl­y high risk of late distant relapse,” said senior author Christina Curtis, assistant professor of medicine and genetics at Stanford University.

“These are the patients who remain in

jeopardy of experienci­ng a relapse after their initial diagnosis,” she said.

RISK OF RELAPSE

The study found that around 25 per cent of women with the most commonly diagnosed form of breast cancer have a 42-55 per cent risk of seeing their cancer return within two decades.”These are the women who seem to be cured but then present with systemic disease many years later,” Curtis said in a press release issued by Stanford University. “Until now, there has been no good way to identify this subset of women who might benefit from ongoing screening or treatment.”

The study also opens up potential new avenues for additional treatment of breast cancer patients by identifyin­g gene alteration­s in each of the four at-risk subgroups.

These alteration­s or mutations result in problems in signalling that can cause unwanted cell growth. And that, in turn, can fuel the formation of tumours or their progressio­n.

“Many of these genomic driver alteration­s can potentiall­y be therapeuti­cally targeted, suggesting the possibilit­y of new treatment options, though this will need to be evaluated in the context of clinical trials,” said Curtis.

The study also reveals when and where in the body breast cancers might metastasis­e and found a group of patients with so-called triple-negative tumours whose cancers are unlikely to return after five years. “This informatio­n can be used to refine risk estimates and improve follow-up and stratifica­tion of patients with breast cancer — for example, by determinin­g which patients might benefit from longer or different types of treatment,” she said.

BETTER TREATMENTS

The researcher­s cautioned that their data set includes cases from decades ago, meaning that patients were not then able to access more recently developed and approved treatments.

Some of those treatments have significan­tly improved the survival rates for patients with particular types of breast cancer. But the findings should still significan­tly help doctors more accurately predict which of their patients are most at risk of seeing their cancer return.

The team has even developed an online “breast cancer recurrence predictor” tool for doctors, using their model. Curtis said the researcher­s are now pursuing a clinical trial for treatment options that would target the genomic defects in patients most at risk of cancer recurrence.

The study found that around 25 per cent of women with the most commonly diagnosed form of breast cancer have a 42 - 55 per cent risk of seeing their cancer return within two decades.

 ?? PIC CREDIT AFP RELAXNEWS ?? Recurring breast cancer remains poorly understood.
PIC CREDIT AFP RELAXNEWS Recurring breast cancer remains poorly understood.

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