Altered immunity to microbiota, B cell activation and depleted γδ/resident memory T cells in colorectal cancer

被引:0
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作者
Alistair Noble
Edward T. Pring
Lydia Durant
Ripple Man
Stella M. Dilke
Lesley Hoyles
Steve A. James
Simon R. Carding
John T. Jenkins
Stella C. Knight
机构
[1] Gut Microbes and Health Program,Antigen Presentation Research Group
[2] Quadram Institute Bioscience,St. Mark’s Hospital
[3] Imperial College London,Department of Biosciences
[4] London North West University Healthcare NHS Trust,Norwich Medical School
[5] Nottingham Trent University,undefined
[6] University of East Anglia,undefined
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关键词
Colorectal cancer; Microbiota; Resident memory T cell; Gamma delta T cell; B cell;
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摘要
The role of microbiota:immune system dysregulation in the etiology of colorectal cancer (CRC) is poorly understood. CRC develops in gut epithelium, accompanied by low level inflammatory signaling, intestinal microbial dysbiosis and immune dysfunction. We examined populations of intraepithelial lymphocytes in non-affected colonic mucosa of CRC and healthy donors and circulating immune memory to commensal bacterial species and yeasts. γδ T cells and resident memory T cells, populations with a regulatory CD39-expressing phenotype, were found at lower frequencies in the colonic tissue of CRC donors compared to healthy controls. Patterns of T cell proliferative responses to a panel of commensal bacteria were distinct in CRC, while B cell memory responses to several bacteria/yeast were significantly increased, accompanied by increased proportions of effector memory B cells, transitional B cells and plasmablasts in blood. IgA responses to mucosal microbes were unchanged. Our data describe a novel immune signature with similarities to and differences from that of inflammatory bowel disease. They implicate B cell dysregulation as a potential contributor to parainflammation and identify pathways of weakened barrier function and tumor surveillance in CRC-susceptible individuals.
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页码:2619 / 2629
页数:10
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