2022
DOI: 10.3389/fimmu.2022.902947
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Inhibition of Notch Signaling Stimulates Osteoclastogenesis From the Common Trilineage Progenitor Under Inflammatory Conditions

Abstract: Osteoclasts, macrophages and dendritic cells (DCs) can be derived from a common trilineage myeloid progenitor of hematopoietic origin. Progenitor commitment is susceptible to regulation through Notch signaling. Our aim was to determine the effects of Notch modulation on trilineage progenitor commitment and functional properties of differentiated cells under inflammatory conditions. We used the conditional inducible CX3CR1CreERT2 mouse strain to achieve overexpression of the Notch 1 intracellular domain (NICD1)… Show more

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Cited by 2 publications
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“…CIA was induced in male B6 mice by a modified protocol as previously described ( 9 ), and periarticular bone marrow of distal tibia was collected for flow cytometric analysis and cell sorting 33-35 days following immunization ( Figure 1A ). To identify osteoclastogenic cell subsets in the periarticular area, gating strategy was performed as previously described ( 9 , 32 ). Bone marrow OCPs were dissected by delineation of live bone marrow single-cells that were further gated for hematopoietic (CD45 + ) agranulocytes (Ly6G − ), followed by gating of non-lymphoid (CD3 − B220 − NK1.1 − ) cells with low expression of CD11b (CD11b −/lo ) ( Supplementary Figure 1A ).…”
Section: Resultsmentioning
confidence: 99%
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“…CIA was induced in male B6 mice by a modified protocol as previously described ( 9 ), and periarticular bone marrow of distal tibia was collected for flow cytometric analysis and cell sorting 33-35 days following immunization ( Figure 1A ). To identify osteoclastogenic cell subsets in the periarticular area, gating strategy was performed as previously described ( 9 , 32 ). Bone marrow OCPs were dissected by delineation of live bone marrow single-cells that were further gated for hematopoietic (CD45 + ) agranulocytes (Ly6G − ), followed by gating of non-lymphoid (CD3 − B220 − NK1.1 − ) cells with low expression of CD11b (CD11b −/lo ) ( Supplementary Figure 1A ).…”
Section: Resultsmentioning
confidence: 99%
“…Moreover, proportion of OCPs expressing protein level of Kit/CD117 was higher in CCR2 lo than in CCR2 hi subset. CD115 + CD117 + double-positive cells, lacking expression of other mature hematopoietic markers, were shown to exhibit characteristics of monocyte progenitors with the multilineage potency to differentiate into osteoclasts, dendritic cells and macrophages ( 8 , 32 ). Further dissection of the bone marrow using CD115 and CD117 markers showed that, as OCPs mature, they downregulate CD117 but remain CD115 + ( 6 ), which is in line with our observation of lower Kit expression in OCPs stimulated by RANKL and M-CSF in vitro compared to pre-cultured OCPs.…”
Section: Discussionmentioning
confidence: 99%
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