HCA Data Explorer

Distinct microbial and immune niches of the human colon

Updated November 15, 2021

Gastrointestinal microbiota and immune cells interact closely and display regional specificity, but little is known about how these communities differ with location. Here, we simultaneously assess microbiota and single immune cells across the healthy, adult human colon, with paired characterisation of immune cells in the mesenteric lymph nodes, to delineate colonic immune niches at steady-state. We describe distinct T helper 1 cell activation and migration profiles along the colon and characterise the transcriptional adaptation trajectory of T regulatory cells between lymphoid tissue and colon. Finally, we show increasing B cell accumulation, clonal expansion and mutational frequency from caecum to sigmoid colon, and link this to the increasing number of reactive bacterial species

Kylie JamesWellcome Sanger Institutekj7@sanger.ac.uk
Sarah TeichmannWellcome Sanger Institutest9@sanger.ac.uk
Kylie James (Experimental Scientist)1
Kerstin B Meyer (Experimental Scientist)1
Rasa Elmentaite (Experimental Scientist)1
Tomas Pires de Carvalho Gomes (Computational Scientist)1
Velislava Petrova (Computational Scientist)1
Nitin Kumar (Computational Scientist)1
Krzysztof Polanski (Computational Scientist)1
Trevor Lawley (Principal Investigator)1
Mark Stares (Experimental Scientist)1
Emily Gulliver (Computational Scientist)2
Menna Clatworthy (Principal Investigator)3
John Ferdinand (Experimental Scientist)3
Beth Bareham (Experimental Scientist)3
Sam Forster (Experimental Scientist)2
Sarah Howlett (Experimental Scientist)3
Lorna Jarvis (Experimental Scientist)3
Hamish King (Computational Scientist)4
Kourosh Saeb-Parsy (Clinician)3
Ondej Suchanek (Clinician)3
Louisa James (Computational Scientist)4
Joanne Jones (Principal Investigator)3
Sarah Teichmann (Principal Investigator)1
1Wellcome Sanger Institute
2Monash University
3University of Cambridge
4Queen Mary University of London
Marion F Shadbolt

To reference this project, please use the following link:

https://explore.data.humancellatlas.org/projects/83f5188e-3bf7-4956-9544-cea4f8997756

Supplementary links are provided by contributors and represent items such as additional data which can’t be hosted here; code that was used to analyze this data; or tools and visualizations associated with this specific dataset.

1.https://www.gutcellatlas.org/
Array Express Accessions:
E-MTAB-8007, E-MTAB-8474, E-MTAB-8476, E-MTAB-8484, E-MTAB-8486
INSDC Project Accessions:
ERP115651, ERP118125, ERP118315, ERP118165, ERP118273
INSDC Study Accessions:
PRJEB32912, PRJEB35119, PRJEB35284, PRJEB35153, PRJEB35244

Downloaded and exported data is governed by the HCA Data Release Policy and licensed under the Creative Commons Attribution 4.0 International License (CC BY 4.0). For more information please see our Data Use Agreement.

Analysis Portals

CZ CELLxGENECZ CELLxGENE
UCSC Cell BrowserUCSC Cell Browser

Project Label

ColonImmune10XSS2VDJ

Species

Homo sapiens

Sample Type

specimens

Anatomical Entity

2 anatomical entities

Organ Part

4 organ parts

Selected Cell Types

8 cell types

Disease Status (Specimen)

normal

Disease Status (Donor)

normal

Development Stage

human adult stage

Library Construction Method

5 library construction methods

Nucleic Acid Source

single cell

Paired End

false, true

Analysis Protocol

MultiSampleSmartSeq2_v2.2.6, SmartSeq2SingleSample_v5.1.5, optimus_post_processing_v1.0.0, optimus_v4.2.2

File Format

6 file formats

Cell Count Estimate

1.5k

Donor Count

6
bai1,534 file(s)bam1,558 file(s)fastq.gz3,216 file(s)h5ad1 file(s)loom28 file(s)rds1 file(s)