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Targeted Suppression of Human IBD-associated Gut Microbiota Commensals by Phage Consortia for Treatment of Intestinal Inflammation

Overview
Journal Cell
Publisher Cell Press
Specialty Cell Biology
Date 2022 Aug 5
PMID 35931020
Authors
Sara Federici
Sharon Kredo-Russo
Rafael Valdes-Mas
Denise Kviatcovsky
Eyal Weinstock
Yulia Matiuhin
Yael Silberberg
Koji Atarashi
Munehiro Furuichi
Akihiko Oka
Bo Liu
Morine Fibelman
Iddo Nadav Weiner
Efrat Khabra
Nyssa Cullin
Noa Ben-Yishai
Dana Inbar
Hava Ben-David
Julian Nicenboim
Noga Kowalsman
Wolfgang Lieb
Edith Kario
Tal Cohen
Yael Friedman Geffen
Lior Zelcbuch
Ariel Cohen
Urania Rappo
Inbar Gahali-Sass
Myriam Golembo
Vered Lev
Mally Dori-Bachash
Hagit Shapiro
Claudia Moresi
Amanda Cuevas-Sierra
Gayatree Mohapatra
Lara Kern
Danping Zheng
Samuel Philip Nobs
Jotham Suez
Noa Stettner
Alon Harmelin
Naomi Zak
Sailaja Puttagunta
Merav Bassan
Kenya Honda
Harry Sokol
Corinna Bang
Andre Franke
Christoph Schramm
Nitsan Maharshak
Ryan Balfour Sartor
Rotem Sorek
Eran Elinav
Affiliations
Soon will be listed here.
Abstract

Human gut commensals are increasingly suggested to impact non-communicable diseases, such as inflammatory bowel diseases (IBD), yet their targeted suppression remains a daunting unmet challenge. In four geographically distinct IBD cohorts (n = 537), we identify a clade of Klebsiella pneumoniae (Kp) strains, featuring a unique antibiotics resistance and mobilome signature, to be strongly associated with disease exacerbation and severity. Transfer of clinical IBD-associated Kp strains into colitis-prone, germ-free, and colonized mice enhances intestinal inflammation. Stepwise generation of a lytic five-phage combination, targeting sensitive and resistant IBD-associated Kp clade members through distinct mechanisms, enables effective Kp suppression in colitis-prone mice, driving an attenuated inflammation and disease severity. Proof-of-concept assessment of Kp-targeting phages in an artificial human gut and in healthy volunteers demonstrates gastric acid-dependent phage resilience, safety, and viability in the lower gut. Collectively, we demonstrate the feasibility of orally administered combination phage therapy in avoiding resistance, while effectively inhibiting non-communicable disease-contributing pathobionts.

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