A faecal microbiota signature with high specificity for pancreatic cancer

Author:

Kartal EceORCID,Schmidt Thomas S BORCID,Molina-Montes EstherORCID,Rodríguez-Perales SandraORCID,Wirbel JakobORCID,Maistrenko Oleksandr MORCID,Akanni Wasiu AORCID,Alashkar Alhamwe BilalORCID,Alves Renato JORCID,Carrato AlfredoORCID,Erasmus Hans-Peter,Estudillo LidiaORCID,Finkelmeier Fabian,Fullam AnthonyORCID,Glazek Anna M,Gómez-Rubio Paulina,Hercog Rajna,Jung FerrisORCID,Kandels StefanieORCID,Kersting StephanORCID,Langheinrich MelanieORCID,Márquez Mirari,Molero Xavier,Orakov AskarbekORCID,Van Rossum TheaORCID,Torres-Ruiz RaulORCID,Telzerow AnjaORCID,Zych KonradORCID,Benes VladimirORCID,Zeller GeorgORCID,Trebicka JonelORCID,Real Francisco XORCID,Malats NuriaORCID,Bork PeerORCID, ,

Abstract

BackgroundRecent evidence suggests a role for the microbiome in pancreatic ductal adenocarcinoma (PDAC) aetiology and progression.ObjectiveTo explore the faecal and salivary microbiota as potential diagnostic biomarkers.MethodsWe applied shotgun metagenomic and 16S rRNA amplicon sequencing to samples from a Spanish case–control study (n=136), including 57 cases, 50 controls, and 29 patients with chronic pancreatitis in the discovery phase, and from a German case–control study (n=76), in the validation phase.ResultsFaecal metagenomic classifiers performed much better than saliva-based classifiers and identified patients with PDAC with an accuracy of up to 0.84 area under the receiver operating characteristic curve (AUROC) based on a set of 27 microbial species, with consistent accuracy across early and late disease stages. Performance further improved to up to 0.94 AUROC when we combined our microbiome-based predictions with serum levels of carbohydrate antigen (CA) 19–9, the only current non-invasive, Food and Drug Administration approved, low specificity PDAC diagnostic biomarker. Furthermore, a microbiota-based classification model confined to PDAC-enriched species was highly disease-specific when validated against 25 publicly available metagenomic study populations for various health conditions (n=5792). Both microbiome-based models had a high prediction accuracy on a German validation population (n=76). Several faecal PDAC marker species were detectable in pancreatic tumour and non-tumour tissue using 16S rRNA sequencing and fluorescence in situ hybridisation.ConclusionTaken together, our results indicate that non-invasive, robust and specific faecal microbiota-based screening for the early detection of PDAC is feasible.

Funder

Red Temática de Investigación Cooperativa en Cáncer

BMBF-funded Heidelberg Center for Human Bioinformatics (HD-HuB) within the German Network for Bioinformatics Infrastructure

Instituto de Salud Carlos III-FEDER

EU-6FP Integrated Project

H2020 European Research Council

World Cancer Research Fund

EU-FP7-HEALTH

Publisher

BMJ

Subject

Gastroenterology

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