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NOD mice, susceptible to pancreatic autoimmunity, demonstrate delayed growth of pancreatic cancer. | LitMetric

AI Article Synopsis

  • Pancreatic cancer is a serious type of cancer with a short survival time of about six months and is linked to factors like type 2 diabetes, obesity, pancreatitis, and smoking.
  • Researchers are trying to understand how the body's immune responses could influence the development of pancreatic cancer, as this has been seen in other types of cancer.
  • In a study using special mice, they found that certain genetic traits slowed down the growth of pancreatic tumors, suggesting that boosting the immune system could be a good way to treat this type of cancer.

Article Abstract

Pancreatic cancer is a high mortality form of cancer, with a median survival only six months. There are multiple associated risk factors associated, most importantly type 2 diabetes, obesity, pancreatitis and smoking. The relative rarity of the disease, however, has made it difficult to dissect causative risk factors, especially with related risk factors. A major unanswered question with important therapeutic implications is the effect of immunological responses on pancreatic cancer formation, with data from other cancers suggesting the potential for local immunological responses to either increase cancer development or increase cancer elimination. Due to the rarity and late diagnosis of pancreatic cancer direct epidemiological evidence is lacking, thus necessitating a reliance on animal models. Here we investigated the relationship between pancreatic autoimmunity and cancer by backcrossing the well characterised Ela1-Tag transgenic model of pancreatic cancer onto the pancreatic autoimmune susceptible NOD mouse strain. Through longitudinal magnetic resonance imaging we found that the NOD genetic background delayed the onset of pancreatic tumours and substantially slowed the growth rate of tumours after development. These results suggest that elevated autoimmune surveillance of the pancreas limits tumour formation and growth, identifying pancreatic cancer as a promising target for immune checkpoint blockade therapies that unleash latent autoimmunity.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5655187PMC
http://dx.doi.org/10.18632/oncotarget.21261DOI Listing

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