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CCR2 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

机译：CCR2介导树突状细胞向人结肠募集，但对于树突状细胞亚群，近端和远端结肠之间的表型和功能观察到的差异不起作用

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© 2016 The Authors.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.

机译：©2016作者。背景与目的：关于胃肠道（GI）的树突状细胞（DC）的大多数知识依赖于鼠类研究，其中CD103 + DC专门用于产生免疫耐受，而CD11b +/-亚组的功能尚不清楚。关于人类GI-DC的信息很少，尤其是有关地区规范的信息。在这里，我们表征了整个人类结肠的人类DC特性。方法：对来自95名健康受试者的近端（右/升）和远端（左/降）人结肠活检进行配对；通过流式细胞术评估DC，并通过16S rRNA基因测序评估菌群组成。结果：鉴定出的结肠DC是骨髓（mDC，CD11c + CD123-），并根据CD103和SIRPα（鼠CD11b的人类类似物）表达进一步划分。 CD103-SIRPα+ DC是主要人群，而CD103 +SIRPα+ DC是CD1c + ILT3 + CCR2 +（尽管并非在所有CD103 +SIRPα+ DC上都表达了CCR2）。 CD103 +SIRPα-DC构成了CD141 + ILT3-CCR2-的次要子集。近端结肠样品具有更高的总DC计数和更少的CD103 +SIRPα+细胞。近端DC比远端DC更成熟，对CD4 + CD45RA + T细胞的刺激能力更高。然而，对于近端DC，DC和粘膜归巢标记（β7，CCR9）的DC调用的T细胞表达较低。 CCR2在循环CD1c +上表达，但在CD141 + mDC上不表达，并在Transwell分析中由结肠培养上清液介导DC募集。近端结肠DC产生更高水平的细胞因子。黏膜微生物群分析显示近端结肠中的微生物群负荷较低，但各隔室之间的微生物群组成没有差异。结论：近端结肠DC亚群不同于远端结肠DC亚群，并且更加成熟。因此，在DC介导的GI道炎症中使用DC进行靶向免疫治疗可能需要反映这种免疫区室化。

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Bernardo D; Mann ER; Montalvillo E; Bassity E; Bayiroglu F; Man R; Fernández-Salazar L; English NR; Peake STC; Landy J; Lee GH; Malietzis G; Siaw YH; Vora R; Murugananthan A; Sánchez-Recio E; Phillips RKS; Garrote JA; Scott P; Parkhill J; Hart AL; Omar HO; Arranz E; Walker AW; Carding SR; Knight SC;
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6. 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 [O] . David Bernardo, Lydia Durant, Elizabeth R. Mann, 2016

机译：趋化因子（C-C母题）受体2介导树突状细胞向人结肠的募集但对树突状细胞亚群表型以及近端和远端结肠之间的功能差异不负责任
7. 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 [O] . Bernardo, David, Mann, Elizabeth R., Montalvillo, Enrique, 2017

机译：趋化因子（C-C基序）受体2介导树突状细胞向人结肠的募集，但并不负责树突状细胞亚群，表型和近端与远端结肠之间功能的差异

CCR2 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

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