Chemokine (C-C Motif) Receptor 2 Mediates Dendritic Cell Recruitment to the Human Colon but Is Not Responsible for Differences Observed in Dendritic Cell Subsets, Phenotype, and Function Between the Proximal and Distal Colon

BACKGROUND & AIMS: Most knowledge about gastrointestinal (GI)-tract dendritic cells (DC) relies on murine studies where CD103(+) DC specialize in generating immune tolerance with the functionality of CD11b(+/−) subsets being unclear. Information about human GI-DC is scarce, especially regarding...

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Detalles Bibliográficos
Autores principales: Bernardo, David, Durant, Lydia, Mann, Elizabeth R., Bassity, Elizabeth, Montalvillo, Enrique, Man, Ripple, Vora, Rakesh, Reddi, Durga, Bayiroglu, Fahri, Fernández-Salazar, Luis, English, Nick R., Peake, Simon T.C., Landy, Jon, Lee, Gui H., Malietzis, George, Siaw, Yi Harn, Murugananthan, Aravinth U., Hendy, Phil, Sánchez-Recio, Eva, Phillips, Robin K.S., Garrote, Jose A., Scott, Paul, Parkhill, Julian, Paulsen, Malte, Hart, Ailsa L., Al-Hassi, Hafid O., Arranz, Eduardo, Walker, Alan W., Carding, Simon R., Knight, Stella C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2015
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4705905/
https://www.ncbi.nlm.nih.gov/pubmed/26866054
http://dx.doi.org/10.1016/j.jcmgh.2015.08.006
Descripción
Sumario:BACKGROUND & AIMS: Most knowledge about gastrointestinal (GI)-tract dendritic cells (DC) relies on murine studies where CD103(+) DC specialize in generating immune tolerance with the functionality of CD11b(+/−) subsets being unclear. Information about human GI-DC is scarce, especially regarding regional specifications. Here, we characterized human DC properties throughout the human colon. METHODS: Paired proximal (right/ascending) and distal (left/descending) human colonic biopsies from 95 healthy subjects were taken; DC were assessed by flow cytometry and microbiota composition assessed by 16S rRNA gene sequencing. RESULTS: Colonic DC identified were myeloid (mDC, CD11c(+)CD123(−)) and further divided based on CD103 and SIRPα (human analog of murine CD11b) expression. CD103(-)SIRPα(+) DC were the major population and with CD103(+)SIRPα(+) DC were CD1c(+)ILT3(+)CCR2(+) (although CCR2 was not expressed on all CD103(+)SIRPα(+) DC). CD103(+)SIRPα(-) DC constituted a minor subset that were CD141(+)ILT3(−)CCR2(−). Proximal colon samples had higher total DC counts and fewer CD103(+)SIRPα(+) cells. Proximal colon DC were more mature than distal DC with higher stimulatory capacity for CD4(+)CD45RA(+) T-cells. However, DC and DC-invoked T-cell expression of mucosal homing markers (β7, CCR9) was lower for proximal DC. CCR2 was expressed on circulating CD1c(+), but not CD141(+) mDC, and mediated DC recruitment by colonic culture supernatants in transwell assays. Proximal colon DC produced higher levels of cytokines. Mucosal microbiota profiling showed a lower microbiota load in the proximal colon, but with no differences in microbiota composition between compartments. CONCLUSIONS: Proximal colonic DC subsets differ from those in distal colon and are more mature. Targeted immunotherapy using DC in T-cell mediated GI tract inflammation may therefore need to reflect this immune compartmentalization.

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