作者
Samarth Hegde, Varintra E Krisnawan, Brett H Herzog, Chong Zuo, Marcus A Breden, Brett L Knolhoff, Graham D Hogg, Jack P Tang, John M Baer, Cedric Mpoy, Kyung Bae Lee, Katherine A Alexander, Buck E Rogers, Kenneth M Murphy, William G Hawkins, Ryan C Fields, Carl J DeSelm, Julie K Schwarz, David G DeNardo
发表日期
2020/3/16
期刊
Cancer cell
卷号
37
期号
3
页码范围
289-307. e9
出版商
Elsevier
简介
Here, we utilized spontaneous models of pancreatic and lung cancer to examine how neoantigenicity shapes tumor immunity and progression. As expected, neoantigen expression during lung adenocarcinoma development leads to T cell-mediated immunity and disease restraint. By contrast, neoantigen expression in pancreatic ductal adenocarcinoma (PDAC) results in exacerbation of a fibro-inflammatory microenvironment that drives disease progression and metastasis. Pathogenic TH17 responses are responsible for this neoantigen-induced tumor progression in PDAC. Underlying these divergent T cell responses in pancreas and lung cancer are differences in infiltrating conventional dendritic cells (cDCs). Overcoming cDC deficiency in early-stage PDAC leads to disease restraint, while restoration of cDC function in advanced PDAC restores tumor-restraining immunity and enhances responsiveness to …
学术搜索中的文章
S Hegde, VE Krisnawan, BH Herzog, C Zuo… - Cancer cell, 2020