The Pancreatic Cancer Microbiome Promotes Oncogenesis by Induction of Innate and Adaptive Immune Suppression

Smruti Pushalkar , Mautin Hundeyin , Donnele Daley , Smruti Pushalkar , Mautin Hundeyin , Donnele Daley , Constantinos P. Zambirinis , Emma Kurz , Ankita Mishra , Navyatha Mohan , Berk Aykut , Mykhaylo Usyk , Luisana E. Torres , Gregor Werba , Kevin Zhang , Yuqi Guo , Qianhao Li , Neha Akkad , Sarah Lall , Benjamin Wadowski , Johana Gutierrez , Juan Andres Kochen Rossi , Jeremy Herzog , Brian Diskin , Alejandro Torres‐Hernandez , Josh Leinwand , Wei Chuan K. Wang , Pardeep S. Taunk , Shivraj Savadkar , Malvin N. Janal , Anjana Saxena , Xin Li , Deirdre Jill Cohen , R. Balfour Sartor , Deepak Saxena , George Miller
2018 Cancer Discovery 1,239 citations

Abstract

Abstract We found that the cancerous pancreas harbors a markedly more abundant microbiome compared with normal pancreas in both mice and humans, and select bacteria are differentially increased in the tumorous pancreas compared with gut. Ablation of the microbiome protects against preinvasive and invasive pancreatic ductal adenocarcinoma (PDA), whereas transfer of bacteria from PDA-bearing hosts, but not controls, reverses tumor protection. Bacterial ablation was associated with immunogenic reprogramming of the PDA tumor microenvironment, including a reduction in myeloid-derived suppressor cells and an increase in M1 macrophage differentiation, promoting TH1 differentiation of CD4+ T cells and CD8+ T-cell activation. Bacterial ablation also enabled efficacy for checkpoint-targeted immunotherapy by upregulating PD-1 expression. Mechanistically, the PDA microbiome generated a tolerogenic immune program by differentially activating select Toll-like receptors in monocytic cells. These data suggest that endogenous microbiota promote the crippling immune-suppression characteristic of PDA and that the microbiome has potential as a therapeutic target in the modulation of disease progression. Significance: We found that a distinct and abundant microbiome drives suppressive monocytic cellular differentiation in pancreatic cancer via selective Toll-like receptor ligation leading to T-cell anergy. Targeting the microbiome protects against oncogenesis, reverses intratumoral immune tolerance, and enables efficacy for checkpoint-based immunotherapy. These data have implications for understanding immune suppression in pancreatic cancer and its reversal in the clinic. Cancer Discov; 8(4); 403–16. ©2018 AACR. See related commentary by Riquelme et al., p. 386. This article is highlighted in the In This Issue feature, p. 371

Keywords

Innate immune systemMicrobiomeImmune systemCarcinogenesisBiologyPancreatic cancerCancerAcquired immune systemImmunologyBioinformaticsGenetics

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Year
2018
Type
article
Volume
8
Issue
4
Pages
403-416
Citations
1239
Access
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Smruti Pushalkar, Mautin Hundeyin, Donnele Daley et al. (2018). The Pancreatic Cancer Microbiome Promotes Oncogenesis by Induction of Innate and Adaptive Immune Suppression. Cancer Discovery , 8 (4) , 403-416. https://doi.org/10.1158/2159-8290.cd-17-1134

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DOI
10.1158/2159-8290.cd-17-1134