Lymphomyeloid Contribution of an Immune-Restricted Progenitor Emerging Prior to Definitive Hematopoietic Stem Cells

Böiers, Charlotta; Carrelha, Joana; Lutteropp, Michael; Luc, Sidinh; Green, Joanna C.A.; Azzoni, Emanuele; Woll, Petter S.; Mead, Adam J.; Hultquist, Anne; Swiers, Gemma; Perdiguero, Elisa Gomez; Macaulay, Iain C.; Melchiori, Luca; Luís, Tiago C.; Kharazi, Shabnam; Bouriez-Jones, Tiphaine; Deng, Qiaolin; Pontén, Annica; Atkinson, Deborah; Jensen, Christina T.; Sitnicka, Ewa; Geissmann, Frédéric; Godin, Isabelle; Sandberg, Rickard; Bruijn, Marella F. T. R. de; Jacobsen, Sten Eirik W.

doi:10.1016/j.stem.2013.08.012

Cited by 225 publications

(208 citation statements)

References 53 publications

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“…Next, we assessed whether CSF1R is expressed in the fetal multipotent stem and progenitor cells preceding B-cell lineage commitment. In agreement with previous studies, 15,27 23% and 9% of lymphoid-primed multipotent progenitors (LMPPs; Lin -KIT high SCA-1 high FLT3 high ) expressed CSF1R in E13.5 and E14.5 FL, respectively, whereas 6% of LMPPs in adult BM were CSF1R-positive ( Figure 1D-E). In contrast, there was almost no detectable CSF1R expression on HSCs (Lin…”

Section: Csf1r Is Expressed On Prob Cell Progenitors In the Early Fetsupporting

confidence: 93%

“…12 In adult hematopoiesis, CSF1R has been shown to be highly and selectively expressed on myeloid and dendritic cells, but to be undetectable on lymphocytes, including progenitors and mature cells of the B-cell lineage. 13,14 Recently early lympho-myeloid progenitor cells in the mouse embryo, possessing combined B, T, and myeloid-lineage potential, but not megakaryocyte-erythroid-lineage potential, were found to coexpress CSF1R and IL7 receptor (IL-7R), 15,16 suggesting that CSF1R might not exclusively play a role in myelopoiesis, and a potential role in early embryonic lympho-myeloid development. Thus, although a number of studies have provided support for a strong link between fetal B and myeloid lineage development and the potential existence of a fetal B myeloid-restricted progenitor, such a progenitor has yet to be prospectively identified and characterized.…”

Section: Introductionmentioning

confidence: 99%

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Macrophage colony-stimulating factor receptor marks and regulates a fetal myeloid-primed B-cell progenitor in mice

Zriwil

Böiers

Wittmann

et al. 2016

Blood

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Section: Csf1r Is Expressed On Prob Cell Progenitors In the Early Fetsupporting

confidence: 93%

Section: Introductionmentioning

confidence: 99%

Macrophage colony-stimulating factor receptor marks and regulates a fetal myeloid-primed B-cell progenitor in mice

Zriwil

Böiers

Wittmann

et al. 2016

Blood

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“…We carried out in silico analyses for Trap1a expression. As shown in Figure 5c, RNAseq data 15 showed that Trap1a was not expressed in thymocytes, whereas databases generated by others 18,19 revealed low levels of expression in BM LSK stem/progenitor cells and CLP cells (Figure 5d). Because thymocyte progenitors were identified as part of the LSK population, 21 we used PCR to validate Trap1a expression in LSK cells.…”

Section: Cell-intrinsic Function Of Trap1a In Thymocyte Developmentmentioning

confidence: 95%

“…16 Then, the gene expression level was measured by RPKM and calculated by DEGseq. 17 The expression values of hematopoietic stem cells, LSK and common lymphoid progenitors (CLP) were extracted from the expression result file through GEO Series accession numbers GSE50896 18 and GSE50739. 19 …”

Section: In Silico Data Analysismentioning

confidence: 99%

Trap1a is an X-linked and cell-intrinsic regulator of thymocyte development

Tang

Zhang

et al. 2016

Cell Mol Immunol

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The X-linked Trap1a gene encodes the tumor rejection antigen P1A, which is expressed in fetal tissues and multiple lineages of tumor cells. The function of this gene remains unknown. Using chimeric mice with wild-type (WT) and Trap1a − /y bone marrow, we show that Trap1a − /y donor cells are capable of generating most lineages of hematopoietic cells, with the notable exception of T cells. Deletion of Trap1a selectively arrests T-cell development at double-negative stage 1 (DN1, with a CD4 − CD8 − CD25 − CD44 + phenotype). Because Trap1a is expressed in Lin − Sca-1 + c-Kit + and common lymphoid progenitors but not in immature thymocytes (DN1-DN4), Trap1a mutations affect the differentiation potential of progenitor cells without directly acting on T cells. Despite a similarity in the blockade of DN1 to DN2 transition, the Trap1a − / y DN1 cells have normal expression of c-Kit, in contrast to what was reported in the Notch1 − / − DN1. Complementary DNA profiling of Trap1a − /y and WT embryonic stem cells shows that Trap1a does not regulate the Notch pathway. Our data reveal that Trap1a is an X-linked regulator that affects the differentiation potential of progenitor cells into T cells through a Notch-independent mechanism and identify an important function for the Trap1a gene.

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“…These B cells persist after birth, are mostly resting, and are radio resistant. The precursors of BIa B cells disappear early in life (10). Precursors of later B cell development, generated from pHSCs in bone marrow and used in the clinical setting of bone marrow transplantation to restore hematopoiesis and lymphopoiesis, can no longer develop these long-lived BIa cells.…”

Section: Establishment Of Peripheral Pools Of Mature B Cellsmentioning

confidence: 99%