General Information
Overview
Data ID:
SAID195
GSE:
HRA000166
GSM:
HRR060115
Species:
Human
Condition:
lymphoma
Disease:
Tissue:
Subcutaneous Tissue
Position:
not mentioned
Cells:
2804
Age:
35
Sex:
male
Characteristics
tissue: skin strain: BALB/c cell type: monocytes and macrophages genotype: WT cell subtype: Classical mono
Experiment Information
Title:
Bulk RNA-sequence of four monocyte-macrophage subpopulations isolated from the IgE-dependent skin allergic inflammation (IgE-CAI) skin lesion
Summary:
Basophils play critical roles in the development of mouse delayed-onset skin allergic inflammation (IgE-CAI model). Importantly, they also contribute to the resolution of allergic inflammation by promoting the generation of pro-resolving macrophages. However, it remains unclear how pro-resolving macrophages suppress excess inflammation. To address this, we conducted single-cell RNA-seq (scRNA-seq) analysis of the IgE-CAI skin lesion at days 3 and 5 post-challenge of allergens. scRNA-seq analysis identified four distinct monocyte-macrophage subpopulations, namely classical monoytes, early CMDMs, late CMDMs and resident-like macrophages. Based on the gene expression profiles, classical monoytes, early CMDMs, late CMDMs and resident-like macrophages corresponded to Ly6ChiPD-L2lo, Ly6ChiPD-L2hi, Ly6CloPD-L2hi, and Ly6CloPD-L2lo, respectively.
Overall Design:
IgE-CAI model was elicited to BALB/c WT mice. Cells isolated from IgE-CAI skin lesions of WT mice on day 5 post-antigen challenge were subjected to cell sorting. Four monocyte-macrophage subpopulations, namely Ly6ChiPD-L2lo, Ly6ChiPD-L2hi, Ly6CloPD-L2hi, and Ly6CloPD-L2lo were isolated from the IgE-CAI skin lesion and subjected to bulk RNA-seq analysis.
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