Washington: A drug used to treat blood cancers may also stop the spread of invasive breast cancer, scientists have found.
Researchers at Mayo Clinic in Florida have discovered that in the lab and in animals, the drug decitabine turns on a gene coding for protein kinase D1 (PRKD1) that halts the ability of cancer cells to separate from a tumour and spread to distant organs.
"Treatment with low doses of decitabine in an animal model of breast cancer restored PRKD1 expression, reduced tumour size, and blocked metastasis to the lung," said the study`s senior investigator, Peter Storz, a biochemist and molecular biologist at Mayo Clinic.
"The outcome of patients with invasive breast cancer is less than optimal despite many attempts to improve treatment, including advanced chemotherapy and hormonal therapy," said Storz.
"We hope this study offers a new avenue to prevent breast cancer from becoming aggressive and untreatable," he said.
The research team, which included first author Sahra Borges, a postdoctoral researcher in Storz`s lab, found that the gene coding for PRKD1 was silenced in all but one subtype of invasive breast cancer, including aggressive triple negative breast cancer. That subtype is invasive lobular carcinoma.
Borges also developed an assay that can be used to measure the amount of PRKD1 that is silenced in patients` breast tumours.
"Because we found that PRKD1 is increasingly silenced as breast cancer becomes aggressive and spreads, the hope is that this test can be further developed and used to predict which patients are at risk for cancer metastasis, and thus may benefit from decitabine," Borges said.
Decitabine, approved by the US Food and Drug Administration for use in some blood cancers, is a demethylating agent, meaning that it can switch on beneficial genes such as PRKD1 that cancer has silenced in order to grow.
Treating genes that are silenced is much easier than trying to restore function of a mutated gene, Storz said.
The normal function of PRKD1, which is expressed in cells of the mammary gland, is to maintain normal function by preventing cells from morphing into a state where they can dislodge and spread, he said.
The study was published in journal Breast Cancer Research.