The protein p53-psi, a variant of the well-known anti-cancer guardian protein p53, can reprogram cells to “switch sides” and acquire pro-metastatic features. Pro-metastatic cells naturally expressing p53-psi are seen in LEFT panel. On RIGHT, when p53-psi is silenced, these cells reacquire the characteristics of non-metastatic cells. Credit: Sordella lab, Cold Spring Harbor Laboratory
Researchers at Cold Spring Harbor Laboratory (CSHL) have discovered a new function of the body’s most important tumor-suppressing protein. Called p53, this protein has been called “the guardian of the genome.” It normally comes to the fore when healthy cells sense damage to their DNA caused by stress, such as exposure to toxic chemicals or intense exposure to the sun’s UV rays. If the damage is severe, p53 can cause a cell to commit preprogrammed cell-death, or apoptosis. Mutant versions of p53 that no longer perform this vital function, on the other hand, are enablers of many different cancers.
Cancer researcher Dr. Raffaella Sordella, a CSHL Associate Professor, and colleagues, today report in Proceedings of the National Academy of Sciences the discovery of a p53 cousin they call p53-psi (the Greek letter “psi”). It is a previously unknown variant of the p53 protein, generated by the same gene, called TP53 in humans, that gives rise to other forms of p53.
Sordella and colleagues observed that p53-psi, when expressed, reduces the expression of a molecular glue called E-cadherin, which normally keeps cells in contact within epithelial tissue, the tissue that forms the lining of the lung and many other body organs. This is accompanied by expression of key cellular markers associated with tumor invasiveness and metastatic potential. (These are markers of EMT, or epithelial-to-mesenchymal transition.) Consistently, Sordella and her team found levels of p53-psi to be elevated in early-stage lung tumors with poor prognosis.
Careful investigation revealed that p53-psi generates pro-growth effects by interacting with a protein called cyclophillin D (CypD), at the membrane of the cell’s energy factories, the mitochondria, and by spurring the generation of oxidizing molecules called reactive oxygen species (ROS).
p53-psi was found by the team to be inherently expressed in tumors but also in injured tissue. “This is intriguing,” Sordella says, “because generation of cells bearing characteristics of those seen in wound healing has been seen previously, in tumors.”
The protein p53-psi, a variant of the well-known anti-cancer guardian protein p53, can reprogram cells to “switch sides” and acquire pro-metastatic features. Two types of cells that don’t naturally express p53-psi (LEFT panel) exhibit changes in shape (RIGHT panel) characteristic of the transition to metastasis when they are made to express p53-psi. Credit: Sordella lab, Cold Spring Harbor Laboratory
It is possible, Sordella says, that more familiar p53 mutants associated with tumor growth and metastasis may have “hijacked” those abilities from the program used by p53-psi; to promote healing during tissue injury. A cellular program, in other words, that evolved over eons to heal may have been hijacked by mutant p53 to enable cancers to spread out of control.
The team is currently investigating p53-psi in wound healing to help clarify its role. Confirmation would lend support to the theory that mutant p53 hijacks that function to help advance pro-metastatic processes in cancer.
Provided by Cold Spring Harbor Laboratory