5:["$","div",null,{"className":"fixed inset-0 z-[200]","children":["$","$L13",null,{"pii":"103653","figures":[{"id":"f1","label":"Figure 1","title":"$undefined","caption":"$14"},{"id":"f2","label":"Figure 2","title":"$undefined","caption":"miR-21 secreted from ovarian cancer cells facilitates the secretion of IL-6 from M2 macrophages and this crosstalk elevates the expression of PD-L1 in both cell lines. (A) EVs uptake capacity of M2 macrophage visualized by CFSE-labeled EVs. (B) knock down efficiency of miR-21 assessed by RT-qPCR. (C) effect of miR-21 in EVs on the expression of IL-6 in M2 macrophage determined by Western blotting and RT-qPCR. (D) secretion of IL-6 by M2 macrophages was determined by ELISA assay. (E, F) expression of PD-L1 in M2 macrophage and SKOV3 determined by Western blotting analysis and RT-qPCR. (G) proliferation of CFSE-labeled T cells was assessed by flow cytometry. * p < 0.05 vs. control or co-M2. # p< 0,05 vs. EVs-NC. Statistical comparisons were performed using unpaired t test when only two groups were compared or by Tukey’s test-corrected one-way ANOVA with when more than two groups were compared.
"},{"id":"f3","label":"Figure 3","title":"$undefined","caption":"Overexpressed IL-6R in SKOV3 response to miR-21/IL-6 crosstalk elevates expression of PD-L1. (A, B) The expression of IL-6R and PD-L1 in ovarian cancer biopsy specimens analyzed by IHC. (C) correlation between IL-6R and PD-L1. (D) knock down efficiency of IL-6R assessed by western blotting. (E) expression of miR-21 after depletion of IL-6R determined by RT-qPCR. (F) change of PD-L1 after IL-6R silencing assessed by Western blotting analysis. (G) proliferation of T cells after inhibition of IL-6R analyzed by flow cytometry. * p < 0.05 vs. control or normal. Statistical comparisons were performed using unpaired t test when only two groups were compared or by Tukey’s test-corrected one-way ANOVA with when more than two groups were compared.
"},{"id":"f4","label":"Figure 4","title":"$undefined","caption":"SNHG12 facilitates the expression of IL-6R by NF-κB1. (A) Transcription factor for upregulation of IL-6R by SNHG12 predicted by the LNCmap database. (B) sub-localization of SNHG12 predicted by the LNCmap database. (C) sub-localization of SNHG12 visualized by FISH (D) expression of SNHG12 detected by RT- qPCR. (E) the binding of SNHG12 and NF-κB1 determined by RIP. (F) effects of SNHG12 and NF-κB1 on IL-6R promoter activity assessed by dual luciferase assay. (G) The binding of NF-κB1 to IL-6R promoter determined by ChIP. (H) the expression of IL-6R after silencing or overexpressing SNHG12 determined by Western blotting analysis. * p < 0.05 vs. control or IL-6R-WT + NC. # p < 0.05 vs. IgG. Statistical comparisons were performed using unpaired t test when only two groups were compared or by Tukey’s test-corrected one-way ANOVA with when more than two groups were compared.
"},{"id":"f5","label":"Figure 5","title":"$undefined","caption":"SNHG12 suppresses T cell proliferation by upregulation of PD-L1. (A) The expression of miR-21 determined by RT- qPCR. (B) protein levels of PD-L1 after SNHG12 depleted SKOV3 co-cultured with M2 macrophage determined by Western blotting analysis. (C) effect of SNHG12 depletion or IL-6R overexpression in SKOV3 co-cultured with M2 macrophages, on T cells proliferation determined by flow cytometry. * p < 0.05 vs. si-NC. Statistical comparisons were performed using unpaired t test when only two groups were compared or by Tukey’s test-corrected one-way ANOVA with when more than two groups were compared.
"},{"id":"f6","label":"Figure 6","title":"$undefined","caption":"SNHG12 depletion suppresses immune escape in vivo. (A) Weight of mice recorded every 3 d. (B) Growth curve of transplanted tumor recorded every 5 d. (C) image of transplanted tumors (Scale = 1 mm). (D) CD3⁺ cells in transplanted tumors determined by IHC. (E) the rate of IFN-γ positive cells in transplanted tumors determined by flow cytometry. * p < 0.05 vs. SKOV3 + T cells. Statistical comparisons were performed using unpaired t test when only two groups were compared or by Tukey’s test-corrected one-way ANOVA with when more than two groups were compared. Variables were analyzed at different time points using Bonferroni-corrected repeated measures ANOVA.
"},{"id":"f7","label":"Figure 7","title":"$undefined","caption":"SNHG12 is highly expressed in clinical ovarian cancer patients and positively correlates with IL-6R. (A) the expression of SNHG12 in clinical ovarian cancer samples determined by RT-qPCR. (B) correlation between SNHG12 and IL-6 according to its ranks in related IHC results. (C) correlation of IL-6 and PD-L1 analyzed by IHC. Statistical comparisons were performed using unpaired t test. * p < 0.05 vs. normal tissue.
"},{"id":"f8","label":"Figure 8","title":"$undefined","caption":"Model for ovarian cancer immune escape mechanism: SNHG12 promotes IL-6/miR-21 crosstalk between ovarian cancer cells and M2 macrophages, through elevation of IL-6R via NF-κB1.
"}],"initialId":"f8","articleInfo":{"pii":"103653","title":"Long non-coding RNA SNHG12 promotes immune escape of ovarian cancer cells through their crosstalk with M2 macrophages","articleTypeName":"Research Paper","volume":12,"issue":"17","pageStart":17122,"pageEnd":17136},"backHref":"/article/103653/text#f8"}]}]