Author
Listed:
- Amanda J. Oliver
(Wellcome Genome Campus)
- Ni Huang
(Wellcome Genome Campus)
- Raquel Bartolome-Casado
(Wellcome Genome Campus
University of Oslo and Oslo University Hospital–Rikshospitalet)
- Ruoyan Li
(Wellcome Genome Campus
The University of Texas MD Anderson Cancer Center)
- Simon Koplev
(Wellcome Genome Campus)
- Hogne R. Nilsen
(University of Oslo and Oslo University Hospital–Rikshospitalet)
- Madelyn Moy
(Wellcome Genome Campus)
- Batuhan Cakir
(Wellcome Genome Campus)
- Krzysztof Polanski
(Wellcome Genome Campus)
- Victoria Gudiño
(Hospital Clínic
Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD))
- Elisa Melón-Ardanaz
(Hospital Clínic
Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD))
- Dinithi Sumanaweera
(Wellcome Genome Campus)
- Daniel Dimitrov
(Bioquant)
- Lisa Marie Milchsack
(Wellcome Genome Campus)
- Michael E. B. FitzPatrick
(University of Oxford)
- Nicholas M. Provine
(University of Oxford)
- Jacqueline M. Boccacino
(Wellcome Genome Campus)
- Emma Dann
(Wellcome Genome Campus)
- Alexander V. Predeus
(Wellcome Genome Campus)
- Ken To
(Wellcome Genome Campus)
- Martin Prete
(Wellcome Genome Campus)
- Jonathan A. Chapman
(Newcastle University)
- Andrea C. Masi
(Newcastle University)
- Emily Stephenson
(Wellcome Genome Campus
Newcastle University)
- Justin Engelbert
(Wellcome Genome Campus
Newcastle University)
- Sebastian Lobentanzer
(Bioquant)
- Shani Perera
(Wellcome Genome Campus)
- Laura Richardson
(Wellcome Genome Campus)
- Rakeshlal Kapuge
(Wellcome Genome Campus)
- Anna Wilbrey-Clark
(Wellcome Genome Campus)
- Claudia I. Semprich
(Wellcome Genome Campus)
- Sophie Ellams
(Wellcome Genome Campus)
- Catherine Tudor
(Wellcome Genome Campus)
- Philomeena Joseph
(Wellcome Genome Campus)
- Alba Garrido-Trigo
(Hospital Clínic
Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD))
- Ana M. Corraliza
(Hospital Clínic
Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD))
- Thomas R. W. Oliver
(Cambridge University Hospitals)
- C. Elizabeth Hook
(University of Cambridge)
- Kylie R. James
(Translational Genomics, Garvan Institute of Medical Research
University of New South Wales)
- Krishnaa T. Mahbubani
(University of Cambridge
Cambridge NIHR Biomedical Research Centre
Cambridge Stem Cell Institute)
- Kourosh Saeb-Parsy
(University of Cambridge
Cambridge NIHR Biomedical Research Centre)
- Matthias Zilbauer
(University of Cambridge
University of Cambridge
Cambridge University Hospitals)
- Julio Saez-Rodriguez
(Bioquant)
- Marte Lie Høivik
(Oslo University Hospital
University of Oslo)
- Espen S. Bækkevold
(University of Oslo and Oslo University Hospital–Rikshospitalet)
- Christopher J. Stewart
(Newcastle University)
- Janet E. Berrington
(Newcastle University)
- Kerstin B. Meyer
(Wellcome Genome Campus)
- Paul Klenerman
(University of Oxford
University of Oxford
Oxford University Hospitals NHS Foundation Trust)
- Azucena Salas
(Hospital Clínic
Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD))
- Muzlifah Haniffa
(Wellcome Genome Campus
Newcastle University
Newcastle upon Tyne Hospitals NHS Foundation Trust)
- Frode L. Jahnsen
(University of Oslo and Oslo University Hospital–Rikshospitalet)
- Rasa Elmentaite
(Wellcome Genome Campus
Wellcome Genome Campus)
- Sarah A. Teichmann
(Wellcome Genome Campus
University of Cambridge
Wellcome Genome Campus
University of Cambridge)
Abstract
The gastrointestinal tract is a multi-organ system crucial for efficient nutrient uptake and barrier immunity. Advances in genomics and a surge in gastrointestinal diseases1,2 has fuelled efforts to catalogue cells constituting gastrointestinal tissues in health and disease3. Here we present systematic integration of 25 single-cell RNA sequencing datasets spanning the entire healthy gastrointestinal tract in development and in adulthood. We uniformly processed 385 samples from 189 healthy controls using a newly developed automated quality control approach (scAutoQC), leading to a healthy reference atlas with approximately 1.1 million cells and 136 fine-grained cell states. We anchor 12 gastrointestinal disease datasets spanning gastrointestinal cancers, coeliac disease, ulcerative colitis and Crohn’s disease to this reference. Utilizing this 1.6 million cell resource (gutcellatlas.org), we discover epithelial cell metaplasia originating from stem cells in intestinal inflammatory diseases with transcriptional similarity to cells found in pyloric and Brunner’s glands. Although previously linked to mucosal healing4, we now implicate pyloric gland metaplastic cells in inflammation through recruitment of immune cells including T cells and neutrophils. Overall, we describe inflammation-induced changes in stem cells that alter mucosal tissue architecture and promote further inflammation, a concept applicable to other tissues and diseases.
Suggested Citation
Amanda J. Oliver & Ni Huang & Raquel Bartolome-Casado & Ruoyan Li & Simon Koplev & Hogne R. Nilsen & Madelyn Moy & Batuhan Cakir & Krzysztof Polanski & Victoria Gudiño & Elisa Melón-Ardanaz & Dinithi , 2024.
"Single-cell integration reveals metaplasia in inflammatory gut diseases,"
Nature, Nature, vol. 635(8039), pages 699-707, November.
Handle:
RePEc:nat:nature:v:635:y:2024:i:8039:d:10.1038_s41586-024-07571-1
DOI: 10.1038/s41586-024-07571-1
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