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首页> 外文期刊>Basic Research in Cardiology: Official Journal of the German Association of Cardiovascular Research >HO-1 gene overexpression enhances the beneficial effects of superparamagnetic iron oxide labeled bone marrow stromal cells transplantation in swine hearts underwent ischemia/reperfusion: an MRI study.
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HO-1 gene overexpression enhances the beneficial effects of superparamagnetic iron oxide labeled bone marrow stromal cells transplantation in swine hearts underwent ischemia/reperfusion: an MRI study.

机译:MRI研究表明,HO-1基因的过表达增强了超顺磁性氧化铁标记的骨髓基质细胞在猪心脏缺血/再灌注中的有益作用。

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摘要

To determine the effect of intracoronary transfer of superparamagnetic iron oxide (SPIO) labeled heme oxygenase-1 (HO-1) overexpressed bone marrow stromal cells (BMSCs) in a porcine myocardial ischemia/reperfusion model. Cell apoptosis was assayed and supernatant cytokine concentrations were measured in BMSCs that underwent hypoxia/reoxygen in vitro. Female mini-swines that underwent 1 h LAD occlusion followed by 1 h reperfusion were randomly allocated to receive intracoronary saline (control), 1 x 10(7) SPIO-labeled BMSCs transfected with pcDNA3.1-Lacz plasmid (Lacz-BMSCs), pcDNA3.1-human HO-1 (HO-1-BMSCs), pcDNA3.1-hHO-1 pretreated with a HO inhibitor, tin protoporphyrin (SnPP, n = 10 each). MRI and postmortem histological analysis were made at 1 week or 3 months thereafter. Post hypoxia/reoxygen in vitro, apoptosis was significantly reduced, supernatant VEGF significantly increased while TNF-alpha and IL-6 significantly reduced in HO-1-BMSCs group compared with Lacz-BMSCs group (all p < 0.05). Myocardial expression of VEGF was significantly higher in HO-1-BMSCs than in Lacz-BMSCs group at 1 week post transplantation (all p < 0.05). Signal voids induced by the SPIO were detected in the peri-infarction region in all BMSC groups at 1 week but not at 3 months post transplantation and the extent of the hypointense signal was the highest in HO-1-BMSCs group, and histological analysis showed that signal voids represented cardiac macrophages that engulfed the SPIO-labeled BMSCs. Pretreatment with SnPP significantly attenuated the beneficial effects of HO-1-BMSCs. Transplantation of HO-1-overexpressed BMSCs significantly enhanced the beneficial effects of BMSCs on improving cardiac function in this model.
机译:为了确定在猪心肌缺血/再灌注模型中超顺磁性氧化铁(SPIO)标记的血红素加氧酶-1(HO-1)的冠状动脉内转移对骨髓基质细胞(BMSCs)过度表达的影响。在体外进行了缺氧/复氧的BMSCs中,检测细胞凋亡并测量上清细胞因子浓度。将接受1小时LAD闭塞再灌注1小时的雌性小天鹅随机分配以接受冠状动脉生理盐水(对照),转染了pcDNA3.1-Lacz质粒(Lacz-BMSCs)的1 x 10(7)SPIO标记的BMSC,用HO抑制剂锡原卟啉预处理的pcDNA3.1-人HO-1(HO-1-BMSCs),pcDNA3.1-hHO-1(SnPP,n = 10)。此后1周或3个月进行MRI和验尸组织学分析。与Lacz-BMSCs组相比,HO-1-BMSCs组在体外缺氧/复氧后,凋亡明显减少,上清液VEGF显着增加,而TNF-α和IL-6显着降低(所有p <0.05)。移植后1周,HO-1-BMSCs的心肌VEGF表达明显高于Lacz-BMSCs组(所有p <0.05)。在移植后1周而非3个月时,在所有BMSC组的梗死周围区域均检测到由SPIO诱导的信号空洞,并且HO-1-BMSCs组中低信号信号的程度最高,并且组织学分析表明信号空隙代表吞噬了SPIO标记的BMSC的心脏巨噬细胞。 SnPP预处理显着减弱了HO-1-BMSC的有益作用。 HO-1过表达的BMSCs的移植显着增强了该模型中BMSCs对改善心脏功能的有益作用。

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