TLR3–Responsive, XCR1+, CD141(BDCA-3)+/CD8α+-Equivalent Dendritic Cells Uncovered in Healthy and Simian Immunodeficiency Virus–Infected Rhesus Macaques

Dutertre, Charles–Antoine; Jourdain, Jean-Pierre; Rancez, Magali; Amraoui, Sonia; Fossum, Even; Bogen, Bjarne; Sanchez, Carole; Couëdel-Courteille, Anne; Richard, Yolande; Dalod, Marc; Feuillet, Vincent; Cheynier, Rémi

doi:10.4049/jimmunol.1302448

Cited by 38 publications

(43 citation statements)

References 68 publications

(108 reference statements)

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“…XCR1 + CD34-DC expressed the molecular signature characteristic of XCR1 + bDC, including the chemokine receptor XCR1, which likely promotes physical interactions with CD8 + T cells (8,13), the endocytic receptor CLEC9A, which promotes crosspresentation of Ag derived from dying cells (43), the adhesion receptor CADM1, which may promote the induction of CTL responses (44), and the pattern recognition receptor TLR3, which allows sensing of dsRNA including responsiveness to the synthetic adjuvant PolyI:C. CD1c and CD141 are not reliable markers of human DC subsets, because they were expressed on all the three in vitro-derived DC subsets studied in this work, consistent with similar observations reported for ex vivo-isolated human DC subsets (7,11,42). Hence, flow cytometry assessment of cell surface expression of the discriminative markers XCR1 or CLEC9A and CADM1, or gene expression profiling, are critical to ensure the identity of HLA-DR + CD141 + cells in humans (7,8,11,36).…”

Section: Discussionsupporting

confidence: 74%

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Human XCR1+ Dendritic Cells Derived In Vitro from CD34+ Progenitors Closely Resemble Blood Dendritic Cells, Including Their Adjuvant Responsiveness, Contrary to Monocyte-Derived Dendritic Cells

Balan

Ollion

Colletti

et al. 2014

The Journal of Immunology

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113

154

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Human monocyte-derived dendritic cell (MoDC) have been used in the clinic with moderately encouraging results. Mouse XCR1+ DC excel at cross-presentation, can be targeted in vivo to induce protective immunity, and share characteristics with XCR1+ human DC. Assessment of the immunoactivation potential of XCR1+ human DC is hindered by their paucity in vivo and by their lack of a well-defined in vitro counterpart. We report in this study a protocol generating both XCR1+ and XCR1− human DC in CD34+ progenitor cultures (CD34-DC). Gene expression profiling, phenotypic characterization, and functional studies demonstrated that XCR1− CD34-DC are similar to canonical MoDC, whereas XCR1+ CD34-DC resemble XCR1+ blood DC (bDC). XCR1+ DC were strongly activated by polyinosinic-polycytidylic acid but not LPS, and conversely for MoDC. XCR1+ DC and MoDC expressed strikingly different patterns of molecules involved in inflammation and in cross-talk with NK or T cells. XCR1+ CD34-DC but not MoDC efficiently cross-presented a cell-associated Ag upon stimulation by polyinosinic-polycytidylic acid or R848, likewise to what was reported for XCR1+ bDC. Hence, it is feasible to generate high numbers of bona fide XCR1+ human DC in vitro as a model to decipher the functions of XCR1+ bDC and as a potential source of XCR1+ DC for clinical use.

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Section: Discussionsupporting

confidence: 74%

“…Human XCR1 was stained with a fluorescently coupled recombinant human chemokine ligand vaccibody (rhXCL1-mCherry) (36). FS36 and FS3T cultures were sorted into .97% pure DC subsets with a FACSAria cytometer (BD Biosciences), based on viability (negativity for Sytox blue; Invitrogen) and expression of CD141 and CD11c.…”

Section: In Vitro Generation Of Xcr1mentioning

confidence: 99%

Human XCR1+ Dendritic Cells Derived In Vitro from CD34+ Progenitors Closely Resemble Blood Dendritic Cells, Including Their Adjuvant Responsiveness, Contrary to Monocyte-Derived Dendritic Cells

Balan

Ollion

Colletti

et al. 2014

The Journal of Immunology

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113

154

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“…In pig and macaques, cDC1 were the only cells to strongly express CADM1. In macaques, cDC1 were also XCR1 positive and expressed CLEC9A and BATF3 at the RNA level; similar to human cDC1, they also strongly expressed CD205 and CD162 and were responsive to TLR3 triggering [75,76]. cDC that closely resemble cDC1 in terms of FLT3, CADM1, CD205, TLR3 and XCR1 expression, were also identified for the first time in a non-mammalian species, the chicken [77].…”

Section: Xcr1 + Cadm1 + Cdc1 Across Speciesmentioning

confidence: 77%

“…These recent studies confirmed that BATF3, XCR1, CADM1, TLR3 and, to a lesser extent, CLEC9A are conserved markers of cDC1 across species. CLEC9A was detected only at the RNA level both in macaque [75] and sheep [77], but surface protein expression was only detectable on CADM1 + XCR1 + cDC1 in 2 of the 27 macaques tested [75]. Among leukocytes, cDC1 also have the highest expression level of other molecules including CD205 (DEC-205) in mouse, human, macaque and sheep [61,75,78], CD162 in human and macaque [51,75], and CD26 in mouse, human and sheep [46,61,79].…”

Section: Xcr1 + Cadm1 + Cdc1 Across Speciesmentioning

confidence: 82%

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Aligning bona fide dendritic cell populations across species

Dutertre

Wang

Ginhoux

2014

Cellular Immunology

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Comprehensive Phenotyping of Human Dendritic Cells and Monocytes

Mair

Liechti

2020

Cytometry Pt A

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Professional antigen‐presenting cells (APCs), which include dendritic cells (DCs) and monocytes are essential for inducing and steering adaptive T‐cell responses. Recent technological developments in single‐cell analysis have significantly advanced our understanding of APC subset heterogeneity. To accurately resolve this functional diversity and to account for tissue‐specific adaptation, novel phenotyping markers have been described more recently. While some of these largely overlap with traditionally used markers, more fine‐grained phenotyping might be essential during inflammatory settings, where the traditional distinction between monocytes and dendritic cells has become blurred. Within this phenotype report, we provide a concise overview of traditional and recently described markers for the phenotyping of DCs and monocytes in the human system.

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TLR3–Responsive, XCR1+, CD141(BDCA-3)+/CD8α+-Equivalent Dendritic Cells Uncovered in Healthy and Simian Immunodeficiency Virus–Infected Rhesus Macaques

Cited by 38 publications

References 68 publications

Human XCR1+ Dendritic Cells Derived In Vitro from CD34+ Progenitors Closely Resemble Blood Dendritic Cells, Including Their Adjuvant Responsiveness, Contrary to Monocyte-Derived Dendritic Cells

Human XCR1+ Dendritic Cells Derived In Vitro from CD34+ Progenitors Closely Resemble Blood Dendritic Cells, Including Their Adjuvant Responsiveness, Contrary to Monocyte-Derived Dendritic Cells

Aligning bona fide dendritic cell populations across species

Comprehensive Phenotyping of Human Dendritic Cells and Monocytes

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