Restricted dendritic cell and monocyte progenitors in human cord blood and bone marrow

Lee, Jaeyop; Breton, Gaëlle; Oliveira, Thiago Y.; Zhou, Yu; Aljoufi, Arafat; Puhr, Sarah; Cameron, Mark J.; Sékaly, Rafick‐Pierre; Nussenzweig, Michel C.; Liu, Kang

doi:10.1084/jem.20141442

Cited by 231 publications

(296 citation statements)

References 60 publications

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“…We recently described the human (h)MODP 15 and noted that its cell surface phenotype was similar to that of the hCDP that was described shortly before that 28 ( Figure 7H). Both progenitor populations are very rare, representing about 0.2% of total BM ( Figure 7I).…”

Section: Comparison Of Cdp and Mdp With Modp And Mop: Differentiationmentioning

confidence: 58%

“…These data, together with gene expression profiling, confirmed without bias the existence of the MODP and MOP and their developmental relationship. They also revealed that the mouse 23,24 and human 28 CDP populations are similar, respectively identical to the MODP, and that the mouse MDP population 22 is partially overlapping with the MOP and indeed devoid of DC potential.…”

Section: C-fmsmentioning

confidence: 93%

“…Human CDPs 28 were sorted and cultured at 1000 cells per well in 96-well plates (BD Falcon) under OC or MF differentiation conditions, as has been previously described. 15 For OC differentiation, cells were cultured in a-MEM with 10% FCS, 25 ng/mL recombinant human (rh) M-CSF, and 40 ng/mL rh RANKL.…”

Section: In Vitro Differentiation Of Human Progenitors Into Ocs or Mfsmentioning

confidence: 99%

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Macrophages and osteoclasts stem from a bipotent progenitor downstream of a macrophage/osteoclast/dendritic cell progenitor

Xiao¹,

Palomero²,

Grabowska³

et al. 2017

Blood Advances

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Key Points• Under homeostatic conditions, MFs, OCs, and DCs develop from a tripotent progenitor, the MODP.• (CDP) has been described as committed to plasmacytoid and conventional DC development.However, the human CDP proved identical to the MODP population, whereas the mouse CDP largely overlapped with the MODP population and was accordingly oligopotent for MF, OC, and DC development. The CX 3 CR1 1 MF/DC progenitor (MDP) population described in the mouse generated MFs and OCs but not DCs. Thus, monocytes/MFs, OCs, and DCs share a common progenitor that gives rise to a bipotent MF/OC progenitor, but a dedicated DC progenitor is currently undefined. The definition of these progenitor populations may serve diagnostics and interventions in diseases with pathogenic activity of MFs, OCs, or DCs.

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Section: Comparison Of Cdp and Mdp With Modp And Mop: Differentiationmentioning

confidence: 58%

Section: C-fmsmentioning

confidence: 93%

Section: In Vitro Differentiation Of Human Progenitors Into Ocs or Mfsmentioning

confidence: 99%

See 1 more Smart Citation

Macrophages and osteoclasts stem from a bipotent progenitor downstream of a macrophage/osteoclast/dendritic cell progenitor

Xiao¹,

Palomero²,

Grabowska³

et al. 2017

Blood Advances

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show abstract

“…34,35 This population was detected in the BM of BRGSF mice (supplemental Figure 2B), and its frequency and total numbers increased following Flt3L treatment (supplemental Figure 2C). These data suggest that the increased frequency and absolute numbers of myeloid cells in Flt3L-treated BRGSF HIS mice may result from an increase in the CD34…”

Section: Resultsmentioning

confidence: 99%

A functional DC cross talk promotes human ILC homeostasis in humanized mice

et al. 2017

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“…Protocols to differentiate moDC use purification of CD14 + blood cells, and most likely omit dedicated DC precursors, which circulate in human peripheral blood in low numbers. These blood‐borne pre‐DC can be induced to differentiate into bona fide DC ex vivo 60, 61. For future DC‐based immunotherapy, it will be of interest to compare the tolerogenic potential of preDC‐derived DC and monocyte‐derived DC generated ex vivo with or without VD3.…”

Section: Vd3‐programmed DC For Immune Therapymentioning

confidence: 99%

Vitamin D immunoregulation through dendritic cells

2016

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SummaryVitamin D (VD3) has been linked to immunological processes, and its supplementation may have a role in treatment or prevention of diseases with underlying autoimmune or pro‐inflammatory states. As initiators of the immune responses, dendritic cells (DC) are a potential target of VD3 to dampen autoimmunity and inflammation, but the role of DC in VD3‐mediated immunomodulation in vivo is not understood. In addition to being targets of VD3, DC can provide a local source of bioactive VD3 for regulation of T‐cell responses. Here we review existing studies that describe the tolerogenic potential of VD3 on DC, and discuss them in the context of current understanding of DC development and function. We speculate on mechanisms that might account for the potent but poorly understood tolerogenic activities of VD3 and the role of DC as both targets and sources of this hormone.

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Restricted dendritic cell and monocyte progenitors in human cord blood and bone marrow

Cited by 231 publications

References 60 publications

Macrophages and osteoclasts stem from a bipotent progenitor downstream of a macrophage/osteoclast/dendritic cell progenitor

Macrophages and osteoclasts stem from a bipotent progenitor downstream of a macrophage/osteoclast/dendritic cell progenitor

A functional DC cross talk promotes human ILC homeostasis in humanized mice

Vitamin D immunoregulation through dendritic cells

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