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Engineered T lymphocytes eliminate lung metastases in models of pancreatic cancer. | LitMetric

AI Article Synopsis

  • Pancreatic cancer is extremely lethal, particularly in advanced stages where patients often have distant metastasis and poor outcomes, highlighting the need for better treatments.
  • Mesothelin, a protein overexpressed in pancreatic cancer, presents a potential target for immunotherapy using engineered T cells known as meso-CART cells.
  • This study demonstrates that meso-CART cells can effectively combat mesothelin-positive tumors, slowing tumor growth and eliminating lung metastases in a mouse model, suggesting they may offer a viable treatment for pancreatic cancer patients.

Article Abstract

Pancreatic cancer is known as one of the most lethal cancers in the world. A majority of advanced stage pancreatic cancer patients are diagnosed with distant metastasis and given poor prognoses, calling for a better therapeutic option. Mesothelin, which is overexpressed in pancreatic cancer and other solid tumors, is a potential target for pancreatic cancer immunotherapy. Adoptive transfer of T cells engineered with chimeric antigen receptors (CART cells) was effective for treating CD19-positive leukemia, but it is more difficult for CART cells to eliminate solid tumors. Because distal metastasis is an important malignant behavior of solid tumors, we investigated whether meso-CART cells exert anti-tumor effects against distant metastases. After expressing meso-CAR in human primary T lymphocytes, the resultant meso-CART cells released cytokines in response to and exhibited cytolytic effects on mesothelin-positive tumor cells . Injection of meso-CART cells into tumor-bearing mice moderately delayed subcutaneous tumor growth and eliminated lung metastases. This is the first study to show that meso-CART cells are effective against lung metastases induced by intravenous injection of pancreatic tumor cells. Our results suggest that meso-CART cells may be an effective clinical treatment for mesothelin-positive primary and metastatic tumors in pancreatic cancer patients.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5862608PMC
http://dx.doi.org/10.18632/oncotarget.24122DOI Listing

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