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Researchers Determine Epigenetic Origin of Docetaxel-Resistant Breast Cancer

Researchers Determine Epigenetic Origin of Docetaxel-Resistant Breast Cancer

Researchers at the Bellvitge Biomedical Research Institute (IDIBELL) have published a study in Molecular Cancer Research in which they identify methylation patterns associated with different subtypes of breast cancer, and a subclassification of the group of "triple negatives," a breast cancer type typically associated with poor prognosis. In addition, they identified changes in DNA methylation associated with the response to docetaxel, a common therapy. The research was led by Dr. Eva González-Suárez, head of the IDIBELL Transformation and Metastasis research group.

Patient-derived xenografts (PDXs) are based on the implantation of tumor cells from a patient in an animal model (mice). This yields a much more representative model for drug preclinical studies compared to conventional cell cultures.

Methylation is an epigenetic process of regulating gene expression, which is based on the binding of molecules called methyl groups into DNA. These molecules bind to DNA following certain methylation profiles and activate or silence gene expression without altering the genetic sequence.

The authors of the study have reported for the first time that the methylation patterns of tumor samples from the two main breast cancer subtypes (with and without hormone receptors) in PDXs are the same as those observed in patients. This validates the use of these models in preclinical studies of methylation and drug resistance.

In addition, authors have also observed that in triple negative breast cancer, a very heterogeneous and vaguely classifiable cancer group, there are methylation patternsthat would allow subclassification. This classification in subgroups could allow researchers to find more specific treatments.

Another factor that the researchers asked was whether methylation in tumor cells played an important role in the acquisition of resistance to drugs such as docetaxel, one of the most widespread drugs in chemotherapy. "Even no changes in the global methylation profiles were found, we have identified changes in the methylation of specific genes that can improve the classification of patient samples, thus helping us know whether they will respond to docetaxel treatment or not," Dr. González-Suárez says. "The differentially methylated genes identified can help us find treatments associated with the new subgroups."

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