缺血再灌注条件下内皮祖细胞促进单核/巨噬细胞向M1型极化的研究

doi:10.7655/NYDXBNS20200206

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缺血再灌注条件下内皮祖细胞促进单核/巨噬细胞向M1型极化的研究
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                        10.7655/NYDXBNS20200206
                    
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基金项目:宁夏回族自治区重点研发计划项目（2018EBG02006）

The role and mechanism of endothelial progenitor cells to promote mononuclear/macrophage to type M1 polarization under ischemic reperfusion

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目的：探讨在缺血再灌注条件下内皮祖细胞（endothelial progenitor cell，EPC）促进单核/巨噬细胞向M1型极化的作用及机制。方法：获取健康志愿者的外周血，原代培养EPC和单核/巨噬细胞；体外构建细胞缺血再灌注损伤模型；流式细胞术检测EPC表面细胞间黏附分子-1（intercellular adhesion molecule -1，ICAM-1）、血管细胞黏附分子-1（vascular cell adhesion molecule-1，VCAM-1）和E-选择素的表达；ELISA检测上清中ICAM-1、VCAM-1和E-选择素浓度；采用Transwell小室进行EPC和单核/巨噬细胞共培养，流式细胞术检测M1和M2型单核/巨噬细胞比例。结果：缺血再灌注条件下EPC表面表达及其分泌ICAM-1和VCAM-1均没有显著变化，两组之间差异均没有统计学意义；对照组EPC表面E-选择素平均荧光强度为10.89，缺血再灌注组为33.93（t=3.895，P=0.018）；对照组EPC上清中E-选择素浓度为3.69 ng/mL，缺血再灌注组为18.17 ng/mL（t=4.568，P=0.010）；缺血再灌注条件下EPC能够促进单核/巨噬细胞向M1型极化，对照组M1型单核/巨噬细胞比例为58.83%，缺血再灌注组为81.43%（t=5.394，P=0.006），E-选择素阻断能抑制这种作用（t=5.950，P=0.004）；缺血再灌注条件下EPC抑制单核/巨噬细胞向M2型极化，对照组M2型单核/巨噬细胞比例为60.57%，缺血再灌注组为35.30%（t=6.424，P=0.003），E-选择素阻断能抑制这种作用（t=4.179，P=0.014）。结论：在缺血再灌注损伤条件下，EPC能够通过高表达和分泌E-选择素，促进单核/巨噬细胞向M1型极化，为缺血再灌注损伤的治疗提供了新的靶点。

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Objective：This study aims to explore the role and mechanism of endothelial progenitor cells（EPC） promoting monocyte/macrophage to type M1 polarization under ischemia and reperfusion. Methods：the peripheral blood of healthy volunteers was obtained，the primary EPC and mononuclear/macrophage were cultured. The model of cell ischemia-reperfusion injury was established in vitro，and the expression of intercellular adhesion molecule -1（ICAM-1），vascular cell adhesion molecule -1（VCAM-1）and E- selectin on EPC surface were detected by flow cytometry. ELISA was used to detect the concentration of ICAM-1，VCAM-1 and E- selectin in the supernatant. Co-culture of EPC and mononuclear/macrophages was performed by Transwell chamber，and the ratio of M1 to M2 type monocytes/macrophages was detected by flow cytometry. Results：There was no significant change in the expression and the secretion of ICAM-1 and VCAM-1 of EPC under the ischemic reperfusion condition，and there was no significant difference between the two groups. The average fluorescence intensity of E- selectin on the surface of EPC was 10.89 in the control group and 33.93 in the ischemia reperfusion group（t=3.895，P=0.018）. The concentration of E- selectin in the EPC supernatant was 3.69 ng/mL in the control group and 18.17 ng/mL in the ischemia-reperfusion group（t=4.568，P=0.010）. Under ischemia reperfusion condition，EPC promoted monocyte/macrophage to M1 type polarization. The proportion of monocyte/macrophage type M1 was 58.83% in control group and was 81.43% in ischemia reperfusion group（t=5.394，P=0.006），E- selectin blockage could inhibit this effect（t=5.950，P=0.004）. Under ischemia reperfusion condition，EPC inhibited monocyte/macrophage to M2 type polarization. The ratio of M2 monocyte/macrophage was 60.57% in control group and was 35.30% in ischemia reperfusion group（t=6.424，P=0.003），E- selectin blockage could inhibit this effect（t=4.179，P=0.014）. Conclusion：Under the condition of ischemia-reperfusion injury，EPC can promote the monocyte/macrophage to M1 polarization through the high expression and secretion of E- selectin. Our research provides a new target for the treatment of ischemia-reperfusion injury.

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程华,金梅花,董俭达.缺血再灌注条件下内皮祖细胞促进单核/巨噬细胞向M1型极化的研究[J].南京医科大学学报（自然科学版）,2020,(2):180-184

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收稿日期:2019-07-17
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在线发布日期: 2020-03-14
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