A new Brazilian study has revealed the key role of the protein periostin and stellate pancreatic cells in allowing pancreatic cancer to infiltrate nerves and spread early, increasing the risk of metastasis. The research demonstrates how the tumor reprograms part of the surrounding healthy tissue to acquire a high capacity for invasion. This mechanism is associated with the aggressiveness of the disease and the difficulty of treatment. It also points to possible targets for more precise therapies and personalized treatments.
The findings are published in the journal Molecular and Cellular Endocrinology.
The most common type of pancreatic cancer is adenocarcinoma, which originates in the glandular tissue that produces pancreatic juice. It accounts for 90% of diagnosed cases. Although it is not among the most frequent types of cancer, it is considered an aggressive and highly lethal tumor, with a mortality rate almost equivalent to its incidence rate. Globally, there are approximately 510,000 new cases and nearly the same number of deaths each year.
