Scientific Reports (Apr 2018)

IL23 and TGF-ß diminish macrophage associated metastasis in pancreatic carcinoma

  • S. Mazher Hussain,
  • Leighton F. Reed,
  • Bradley A. Krasnick,
  • Gustavo Miranda-Carboni,
  • Ryan C. Fields,
  • Ye Bi,
  • Abul Elahi,
  • Abidemi Ajidahun,
  • Paxton V. Dickson,
  • Jeremiah L. Deneve,
  • William G. Hawkins,
  • David Shibata,
  • Evan S. Glazer

DOI
https://doi.org/10.1038/s41598-018-24194-5
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 9

Abstract

Read online

Abstract The precise role of tumor associated macrophages remains unclear in pancreatic ductal adenocarcinoma (PDAC) while TGF-ß has an unclear role in metastases formation. In order to understand the role of IL23, an interleukin associated with macrophage polarization, we investigated IL23 in the context of TGF-ß expression in PDAC. We hypothesized that IL23 expression is associated with metastatic development and survival in PDAC. We investigated IL23 and TGF-ß protein expression on resected PDAC patient tumor sections who were divided into short-term (30 months) survivors. Panc-1 cells treated with IL23, TGF-ß, macrophages, or combinations thereof, were orthotopically implanted into NSG mice. Patients in the long-term survivor group had higher IL23 protein expression (P = 0.01). IL23 expression was linearly correlated with TGF-ß expression in patients in the short-term survivor group (P = 0.038). Macrophages induce a higher rate of PDAC metastasis in the mouse model (P = 0.02), which is abrogated by IL23 and TGF-ß treatment (P < 0.001). Macrophages serve a critical role in PDAC tumor growth and metastasis. TGF-ß contributes to a less tumorigenic TME through regulation of macrophages. Macrophages increases PDAC primary tumor growth and metastases formation while combined IL23 and TGF-ß pre-treatment diminishes these processes.