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Data from CD73-Dependent Adenosine Signaling through Adora2b Drives Immunosuppression in Ductal Pancreatic Cancer

Authors :
Jennifer M. Bailey-Lundberg
Florencia McAllister
Holger K. Eltzschig
Tingting Mills
Powel H. Brown
Zhongming Zhao
Altaf Mohammed
Shizuko Sei
Michelle I. Savage
Lana A. Vornik
Kyle L. Poulsen
Dafna Bar-Sagi
Curtis J. Wray
John S. Bynon
Nirav C. Thosani
George Van Buren
Trent Clark
Melissa Pruski
Amanda N. Warner
Emily Vucic
Le Li
Lincoln N. Strickland
Baylee J. O'Brien
Ismet Sahin
Yulin Dai
Olivereen Le Roux
Vidhi Chandra
Kanchan Singh
Erika Y. Faraoni
Publication Year :
2023
Publisher :
American Association for Cancer Research (AACR), 2023.

Abstract

The microenvironment that surrounds pancreatic ductal adenocarcinoma (PDAC) is profoundly desmoplastic and immunosuppressive. Understanding triggers of immunosuppression during the process of pancreatic tumorigenesis would aid in establishing targets for effective prevention and therapy. Here, we interrogated differential molecular mechanisms dependent on cell of origin and subtype that promote immunosuppression during PDAC initiation and in established tumors. Transcriptomic analysis of cell-of-origin–dependent epithelial gene signatures revealed that Nt5e/CD73, a cell-surface enzyme required for extracellular adenosine generation, is one of the top 10% of genes overexpressed in murine tumors arising from the ductal pancreatic epithelium as opposed to those rising from acinar cells. These findings were confirmed by IHC and high-performance liquid chromatography. Analysis in human PDAC subtypes indicated that high Nt5e in murine ductal PDAC models overlaps with high NT5E in human PDAC squamous and basal subtypes, considered to have the highest immunosuppression and worst prognosis. Multiplex immunofluorescent analysis showed that activated CD8+ T cells in the PDAC tumor microenvironment express high levels of CD73, indicating an opportunity for immunotherapeutic targeting. Delivery of CD73 small-molecule inhibitors through various delivery routes reduced tumor development and growth in genetically engineered and syngeneic mouse models. In addition, the adenosine receptor Adora2b was a determinant of adenosine-mediated immunosuppression in PDAC. These findings highlight a molecular trigger of the immunosuppressive PDAC microenvironment elevated in the ductal cell of origin, linking biology with subtype classification, critical components for PDAC immunoprevention and personalized approaches for immunotherapeutic intervention.Significance:Ductal-derived pancreatic tumors have elevated epithelial and CD8+GZM+ T-cell CD73 expression that confers sensitivity to small-molecule inhibition of CD73 or Adora2b to promote CD8+ T-cell–mediated tumor regression.See related commentary by DelGiorno, p. 977

Details

ISSN :
00085472
Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....cad72cac19ab5d47976812827ffaa09a
Full Text :
https://doi.org/10.1158/0008-5472.c.6487377