Study describes a molecular strategy that helps prevent development of tumors in mice

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Study describes a molecular strategy that helps prevent development of tumors in mice

The body's process for manufacturing fatty acids is regulated by the enzyme FASN. In normal cells, this is not a very active process - except occasionally in the liver and adipose tissue - since most of the fatty acids we need for cell maintenance are obtained from the diet.

However, it is known that FASN is overexpressed in many types of cancer, such as prostate, breast, thyroid, colorectal, bladder, lung, and pancreatic cancer. Therefore, even though its relationship with the disease is still poorly understood, scientists from around the world are studying FASN as a potential target for cancer treatment.

Now, a team of researchers led by Miguel Quintela-Fandino, Head of the Breast Cancer Clinical Research Unit of the Spanish National Cancer Research Centre (CNIO), has discovered the link between FASN and cancer and has shown that therapies that inhibit FASN are highly effective in early stages of cancer to prevent the development of tumors in mice and cell cultures, but not to treat tumors once they have already appeared. The results are published in Nature Communications.

One of the main findings of the study is that the importance of FASN for the development of cancer is not related to its ability to generate fatty acids. Until now, it was thought that tumor cells over-activate FASN to generate energy, build their cell membranes, etc.

In this work, however, we show that cancer continues to capture these fatty acids from circulating blood. Therefore, FASN's function of synthesizing fatty acids is not necessary for cancer cells."
Miguel Quintela-Fandino, leader of the study

Cancer does need FASN to help it arise. The researchers discovered that FASN is essential for one of the key processes - known as the hallmarks of cancer - in the transformation of a normal cell into a cancer cell: anchorage-independent growth - that is, being able to grow without being attached to a solid surface, a capacity that a normal cell does not have.

"Together with other signs - such as the ability to invade and resistance to programmed cell death -, a key feature that defines that a cell is transforming into a malignant cell is that it can grow autonomously and separate itself from the tissue to which it is anchored," explains study leader Quintela. "As soon as they separate, normal cells enter a process called anoikis and die, while tumor cells can continue growing."

Without FASN there is no tumor


The team confirmed these results in cultures of normal mouse cells in which they overexpressed known oncogenes - such as KRAS (involved in lung cancer) or PyMT and HER2 (involved in breast cancer) - to induce the transformation of normal cells into malignant cells. By eliminating the expression of FASN, normal cells did not transform into cancer cells, even though the oncogenes were overexpressed.

Researchers around the world are studying the potential of FASN to treat certain types of cancer. However, the results of the CNIO team suggest that its effectiveness is preventive, not therapeutic. "In our mouse model, which develops a highly penetrant form of breast cancer, areas where FASN was present developed cancer, whereas tumors did not develop in areas where we blocked FASN, and survival increased by 68%," says Quintela. "But when we tried to inhibit FASN in already established tumors, there was a small transient effect that hardly affected tumor progression."

In the following steps of the investigation, the team will try to study the implications of these findings for metastasis and the immune system's response to tumors. In the future, the potential of these findings for application in risk populations could also be analyzed.

Centro Nacional de Investigaciones Oncológicas (CNIO)

Journal reference:
Bueno., M.J. et al. (2019) Essentiality of fatty acid synthase in the 2D to anchorage-independent growth transition in transforming cells. Nature Communications. doi.org/10.1038/s41467-019-13028-1.

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