The Fungal Mycobiome Promotes Pancreatic Oncogenesis Via Activation of MBL

Overview

Journal Nature

Specialty Science

Date 2019 Oct 4

PMID 31578522

Citations 400

Authors

Berk Aykut

Smruti Pushalkar

Ruonan Chen

Qianhao Li

Raquel Abengozar

Jacqueline I Kim

Sorin A Shadaloey

Dongling Wu

Pamela Preiss

Narendra Verma

Yuqi Guo

Anjana Saxena

Mridula Vardhan

Brian Diskin

Wei Wang

Joshua Leinwand

Emma Kurz

Juan A Kochen Rossi

Mautin Hundeyin

Constantinos Zambrinis

Xin Li

Deepak Saxena

George Miller

Affiliations

Soon will be listed here.

Abstract

Bacterial dysbiosis accompanies carcinogenesis in malignancies such as colon and liver cancer, and has recently been implicated in the pathogenesis of pancreatic ductal adenocarcinoma (PDA). However, the mycobiome has not been clearly implicated in tumorigenesis. Here we show that fungi migrate from the gut lumen to the pancreas, and that this is implicated in the pathogenesis of PDA. PDA tumours in humans and mouse models of this cancer displayed an increase in fungi of about 3,000-fold compared to normal pancreatic tissue. The composition of the mycobiome of PDA tumours was distinct from that of the gut or normal pancreas on the basis of alpha- and beta-diversity indices. Specifically, the fungal community that infiltrated PDA tumours was markedly enriched for Malassezia spp. in both mice and humans. Ablation of the mycobiome was protective against tumour growth in slowly progressive and invasive models of PDA, and repopulation with a Malassezia species-but not species in the genera Candida, Saccharomyces or Aspergillus-accelerated oncogenesis. We also discovered that ligation of mannose-binding lectin (MBL), which binds to glycans of the fungal wall to activate the complement cascade, was required for oncogenic progression, whereas deletion of MBL or C3 in the extratumoral compartment-or knockdown of C3aR in tumour cells-were both protective against tumour growth. In addition, reprogramming of the mycobiome did not alter the progression of PDA in Mbl- (also known as Mbl2) or C3-deficient mice. Collectively, our work shows that pathogenic fungi promote PDA by driving the complement cascade through the activation of MBL.

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