Novel molecular pathway in aggressive breast cancer offers potential therapeutic targets

Novel molecular pathway in aggressive breast cancer offers potential therapeutic targets
Breast cancer cell. Credit: University of Tsukuba

University of Tsukuba-led researchers identified a novel molecular mechanism involved in progression and metastasis in the most aggressive form of breast cancer. The gene MAFK is known to be induced by the TGF-β signaling pathway, which is involved in breast cancer development. The team reported that MAFK protein, in turn, induced cancerous behaviors in cells by switching on the breast cancer-associated gene GPNMB. MAFK thus represents a link between TGF-β signaling and GPNMB-induced breast cancer.

Breast is the most common type of cancer in women. It is divided into different types based on whether certain molecules, including receptors for hormones, are present. Triple-negative (TNBC), which lacks three key receptors, is the most aggressive form. TNBC frequently metastasizes to other organs and has poor prognosis. Understanding the molecular mechanisms underpinning TNBC is key to developing targeted molecular therapies for the condition.

An international research team led by the University of Tsukuba (Japan) has now identified a novel molecular mechanism contributing to progression and metastasis in TNBC. Musculoaponeurotic fibrosarcoma (MAF) oncogene family protein K (MAFK) is a protein involved in switching on specific target . The team previously identified MAFK as a gene that is itself switched on by a protein called TGF-β, which is known to be involved in TNBC development. The researchers confirmed MAFK as a functional link between TGF-β and TNBC. The findings were published in Science Signaling.

"The TGF-β signaling pathway is involved in TNBC progression and metastasis," corresponding author Mitsuyasu Kato says. "However, it's also involved in beneficial processes in healthy cells, and actually helps to suppress the early stages of tumor development. Identifying molecular processes downstream of the TGF-β pathway could offer specific targets for TNBC therapy to combat progression and metastasis without interfering with the beneficial effects of TGF-β signaling."

The team found higher levels of MAFK in TNBC cells than in other cancer cell types. A survey of patient data revealed that patients with higher MAFK gene activity had poorer prognosis. Moreover, when the team interfered with the production of MAFK in , the tumors the cells formed were smaller and metastasized to a lesser degree. Conversely, genetically engineering non-cancerous breast cells to make them produce MAFK caused them to behave like cancer cells.

There was already some evidence of MAFK promoting tumor development in other cancer types, but the underlying mechanism remained a mystery. By screening DNA, the team identified a gene, GPNMB, which is switched on by MAFK.

"We found that induction by MAFK of cancer-like behaviors in breast is dependent on GPNMB," lead author Yukari Okita says. "GPNMB is already known to be present at high levels in the most aggressive and lethal TNBC and to contribute to cancer development; our study identifies induction by MAFK as a missing link between the TGF-β pathway and GPNMB." Shedding light on this pathway therefore offers potential new therapeutic targets for patients with TNBC.

More information: Yukari Okita et al. The transcription factor MAFK induces EMT and malignant progression of triple-negative breast cancer cells through its target GPNMB, Science Signaling (2017). DOI: 10.1126/scisignal.aak9397

Journal information: Science Signaling
Citation: Novel molecular pathway in aggressive breast cancer offers potential therapeutic targets (2017, April 21) retrieved 28 March 2024 from https://medicalxpress.com/news/2017-04-molecular-pathway-aggressive-breast-cancer.html
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