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Image Search Results
Journal: Nephrology Dialysis Transplantation
Article Title: Plasmacytoid dendritic cells modulate the production of mucosal IgA in IgA nephropathy
doi: 10.1093/ndt/gfaf216
Figure Lengend Snippet: Frequency of tonsillar pDCs positively correlates with the expression of mRNAs encoding APRIL, BAFF and TLR9 in tonsillar MNCs from patients with IgAN. Correlation analysis was performed between the frequency of tonsillar pDCs and gene expression in tonsillar MNCs from patients with IgAN ( n = 10, red dots) and CT ( n = 9, black dots). ( A ) Correlation between the percentage of tonsillar pDCs and the expression of TLR9 in tonsillar MNCs from patients with IgAN and CT. ( B ) Correlation between the percentage of tonsillar pDCs and the expression of IL-6 in tonsillar MNCs from patients with IgAN and CT. ( C ) Correlation between the percentage of tonsillar pDCs and the expression of BAFF in tonsillar MNCs from patients with IgAN and CT. ( D ) Correlation between the percentage of tonsillar pDCs and the expression of APRIL in tonsillar MNCs from patients with IgAN and CT. Spearman’s correlation coefficients (r) and P -values are shown in each panel. * P ≤ .05.
Article Snippet: The
Techniques: Expressing, Gene Expression
Journal: Nephrology Dialysis Transplantation
Article Title: Plasmacytoid dendritic cells modulate the production of mucosal IgA in IgA nephropathy
doi: 10.1093/ndt/gfaf216
Figure Lengend Snippet: Ratio of Gd-IgA1/IgA levels in culture supernatants of tonsillar MNCs from patients with IgAN correlates with the percentage of pDCs and the expression of APRIL in tonsillar MNCs. Association between Gd-IgA1/IgA levels and tonsillar pDC frequency or gene expression in MNCs from patients with IgAN ( n = 7, red dots) and CT ( n = 8, black dots). ( A ) The ratios of Gd-IgA1/IgA in culture supernatants of tonsillar MNCs from patients with IgAN or CT. ( B ) Correlation between the Gd-IgA1/IgA ratio and the percentage of tonsillar pDCs in MNCs from patients with IgAN and CT. ( C ) Correlation between the Gd-IgA1/IgA ratio and the expression of APRIL in MNCs from patients with IgAN and CT. ( D ) Correlation between the Gd-IgA1/IgA ratio and the expression of BAFF in MNCs from patients with IgAN and CT. ( E ) Association between the APRIL and TLR9 expression levels in tonsillar MNCs from patients with IgAN and CT. Correlations were assessed using Spearman’s correlation coefficients (r) with P -values shown in each panel. ns, not significant; * P ≤ .05.
Article Snippet: The
Techniques: Expressing, Gene Expression
Journal: Life Science Alliance
Article Title: Histone methyltransferase DOT1L differentially affects the development of dendritic cell subsets
doi: 10.26508/lsa.202603624
Figure Lengend Snippet: (A) Cre-ER T2 Dot1l wt/wt and Cre-ER T2 Dot1l fl/fl mice were injected three times with tamoxifen. Subsequently, BM was cultured with SCF and FLT3L. Seven days after the start of the culture, DC and precursor subset composition was evaluated. (B) Comparison of myeloid and lymphoid precursor percentages of Live Lineage neg AF neg cells in Dot1l- WT (Cre-ER T2 Dot1l wt/wt ) and Dot1l -KO (Cre-ER T2 Dot1l fl/fl ) conditions. CMPs, MDPs, and CDPs were gated from MHC class II neg CD11c neg CD135 pos cells and defined as CD117 hi CD115 neg CMPs, CD117 int CD115 hi MDPs, and CD117 neg CD115 hi CDPs. CLPs were defined as MHC class II neg CD11c neg CD135 neg CD127 pos . Pre-pDCs were gated as CD117 neg CD135 pos CD11c pos Siglec-H pos Ly-6D pos , pDCs as B220 pos Siglec-H pos BST2 pos , and cDC1s and cDC2s as B220 neg MHC class II hi CD11c hi Sirpα neg/pos . (C) On day 7 after the start of the culture, BM cells were stimulated with class A CpGs (ODN1585) overnight. IFNα levels were determined using ELISA. (D) After class A CpG stimulation, cells were stained for maturation markers. Conditions are shown with and without the addition of CpGs. The individual dots represent individual mice with a total of three independent experiments performed. Error bars indicate the mean ± SD. * P < 0.05, ** P < 0.01, *** P < 0.001, **** P < 0.0001.
Article Snippet: Where indicated, BM cells and/or splenocytes were stimulated with
Techniques: Injection, Cell Culture, Comparison, Enzyme-linked Immunosorbent Assay, Staining
Journal: Life Science Alliance
Article Title: Histone methyltransferase DOT1L differentially affects the development of dendritic cell subsets
doi: 10.26508/lsa.202603624
Figure Lengend Snippet: (A) Schematic overview of the setup of the 7-d BM culture. Total BM of WT C57BL/6 mice was cultured with SCF and FLT3L to facilitate the development of DCs. DOT1L inhibitor SGC-0946 (1 μM) was added at days 0, 3, and 5 to ensure constant inhibition of DOT1L during DC development. DMSO (0.1%) was used as a vehicle control. (B) Comparison of myeloid and lymphoid precursor percentages of Live Lineage neg AF neg cells in cultures with and without DOT1L inhibitor. CMPs, MDPs, and CDPs were gated from MHC class II neg CD11c neg CD135 pos cells and defined as CD117 hi CD115 neg CMPs, CD117 int CD115 hi MDPs, and CD117 neg CD115 hi CDPs. CLPs were defined as MHC class II neg CD11c neg CD135 neg CD127 pos . Pre-pDCs were gated as CD117 neg CD135 pos CD11c pos Siglec-H pos Ly-6D pos , pDCs as B220 pos Siglec-H pos BST2 pos , and cDC1s and cDC2s as B220 neg MHC class II hi CD11c hi Sirpα neg/pos . (C) On day 7, BM cells were stimulated with class A CpGs (ODN1585) overnight. IFNα levels were determined in the supernatant using ELISA, and maturation markers were evaluated by flow cytometry. Conditions are shown with and without the addition of CpGs. The individual dots represent the average of technical replicates in one independent experiment, with a total of three independent experiments performed. Error bars indicate the mean ± SD. * P < 0.05, ** P < 0.01, *** P < 0.001, **** P < 0.0001.
Article Snippet: Where indicated, BM cells and/or splenocytes were stimulated with
Techniques: Cell Culture, Inhibition, Control, Comparison, Enzyme-linked Immunosorbent Assay, Flow Cytometry
Journal: Life Science Alliance
Article Title: Histone methyltransferase DOT1L differentially affects the development of dendritic cell subsets
doi: 10.26508/lsa.202603624
Figure Lengend Snippet: (A) Schematic overview of the experimental setup. Cre-ER T2 Dot1l wt/wt and Cre-ER T2 Dot1l fl/fl mice were injected with tamoxifen on three subsequent days to induce KO of Dot1l . On day 12, BM was harvested and analyzed. (B) Comparison of myeloid and lymphoid precursor percentages of Live Lineage neg AF neg cells in Dot1l -WT (Cre-ER T2 Dot1l wt/wt ) and Dot1l -KO (Cre-ER T2 Dot1l fl/fl ) conditions. CMPs, MDPs, and CDPs were gated from MHC class II neg CD11c neg CD135 pos cells and defined as CD117 hi CD115 neg CMPs, CD117 int CD115 hi MDPs, and CD117 neg CD115 hi CDPs. CLPs were defined as MHC class II neg CD11c neg CD135 neg CD127 pos . Pre-pDCs were gated as CD117 neg CD135 pos CD11c pos Siglec-H pos Ly-6D pos , pDCs as B220 pos Siglec-H pos BST2 pos , and cDC2s as B220 neg MHC class II hi CD11c hi Sirpα pos . (C) Comparisons of specific markers on pDCs and DC2s that were differentially expressed between Dot1l -WT and Dot1l -KO conditions based on the MFI of (N = 10) biological replicates. (D) On day 12, BM cells were stimulated with class A CpGs (ODN1585). IFNα levels were determined in the supernatant using ELISA. In addition, cells were stained intracellularly for IFNαβ. After overnight stimulation, cells were also stained for maturation markers. Conditions are shown with and without the addition of CpGs. The individual dots represent individual mice with a total of two independent experiments performed. (E) Pie charts highlighting the number of up- and down-regulated genes in Dot1l-KO DC populations compared with Dot1l-WT as determined by RNAseq (based on Log 2 FC < −0.5 and >0.5 for the leftmost plot and <−1.0 and >1.0 for all others). (F) GO enrichment of genes that were down-regulated in KO pDCs (Log 2 FC < −1.0). (G) Heatmap of selected transcription factors showing the H3K79me2 signal near the transcriptional start site (TSS; N = 2, green gradient) and expression differences between Dot1l KO and WT (N-1, blue-red gradient) in the sorted DC subsets. (H) GO enrichment of genes that were up-regulated in expression in all sorted subsets (Log 2 FC > 0.5). For (F, H), pathways were ranked by fold enrichment and visualized using ShinyGO . (I) Heatmap correlating the H3K79me2 TSS signal to expression differences for genes from pathways enriched in all KO subsets (as visualized in (H)). Error bars indicate the mean ± SD. * P < 0.05, ** P < 0.01, *** P < 0.001, **** P < 0.0001.
Article Snippet: Where indicated, BM cells and/or splenocytes were stimulated with
Techniques: Injection, Comparison, Enzyme-linked Immunosorbent Assay, Staining, RNA sequencing, Expressing
Journal: Life Science Alliance
Article Title: Histone methyltransferase DOT1L differentially affects the development of dendritic cell subsets
doi: 10.26508/lsa.202603624
Figure Lengend Snippet: (A) Cre-ER T2 Dot1l wt/wt and Cre-ER T2 Dot1l fl/fl mice were injected with tamoxifen on three subsequent days to induce KO of Dot1l . On day 12, organs were harvested, and several (functional) experiments were performed on the splenocytes and BM cells. The region surrounding exon 2 of Dot1L was amplified, and the frequency of Dot1l ∆ alleles was quantified as described previously (BM, bone marrow). (B) Histograms of H3K79me2 in representative Dot1l WT and KO samples derived from either spleen (left) or BM (right). For the KO samples, cells overlapping with the WT peak were classified as H3K79me2 high, and the remainder as H3K79me2 low. (C) Quantification of the H3K79me2 low fractions from S5B (N = 10 for spleen, N = 2 (pooled replicates) for BM). (D) Splenic DC subset percentages of Live Lineage neg AF neg cells in Dot1l WT (Cre-ER T2 Dot1l wt/wt ) and Dot1l -KO (Cre-ER T2 Dot1l fl/fl ) conditions. pDCs were gated as BST2 pos Siglec-H pos , cDC2s as CD11c pos MHC class II pos Sirpα pos , and cDC1s as CD11c pos MHC class II pos XCR1 pos . (E) Mean fluorescence intensity (MFI) of proliferation marker Ki67 on several cell subsets in the BM (left) and spleen (right) in Dot1l WT versus KO conditions on day 12 after the start of tamoxifen injections. The individual dots represent individual mice with a total of two independent experiments performed. (F) Quantification of specific markers on pDCs and cDCs that were differentially expressed between Dot1l WT and Dot1l -KO conditions based on the MFI of (N = 10) biological replicates. (G) On day 12, splenocytes were stimulated with class A CpGs (ODN1585). IFNα levels were determined in the supernatant using ELISA. In addition, cells were stained intracellularly for IFNαβ. After overnight stimulation, cells were also stained for maturation markers. Conditions are shown with and without the addition of CpGs. (H) Principal component analysis of pooled and sorted DC subsets (N = 1) from both WT and Dot1l-KO mice. (I) Pie chart (left) highlighting the number of down- and up-regulated genes in all KO populations (based on Log 2 FC < −0.5 and >0.5, respectively); (right) GO enrichment of genes that were down-regulated in expression (Log 2 < −0.5) in all sorted subsets, ranked by fold enrichment and visualized using ShinyGO. (J) Representative H3K79me2 ChIPseq tracks for Ciita and Fbxo11 exported from IGV. Data scales were standardized to visualize quantitative differences both between genes and between DC subsets. (K) Heatmap of selected epigenetic modifiers showing the H3K79me2 signal near the TSS (N = 2, green gradient) and expression differences between Dot1l KO and WT (N = 1, blue-red gradient) in the sorted DC subsets. Error bars indicate the mean ± SD. * P < 0.05, ** P < 0.01, *** P < 0.001, **** P < 0.0001. Error bars indicate the mean ± SD. * P < 0.05, ** P < 0.01, *** P < 0.001, **** P < 0.0001.
Article Snippet: Where indicated, BM cells and/or splenocytes were stimulated with
Techniques: Injection, Functional Assay, Amplification, Derivative Assay, Fluorescence, Marker, Enzyme-linked Immunosorbent Assay, Staining, Expressing