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国家自然科学基金(30670853)

作品数:3 被引量:24H指数:2
相关作者:陈立娟沈成兴张晓黎唐耀亮刘乃丰更多>>
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Transplantation of magnetically labeled mesenchymal stem cells improves cardiac function in a swine myocardial infarction model被引量:19
2008年
Background Mesenchymal stem cells (MSCs) transplantation provides a new approach for myocardial repair. However, many important fundamental questions about MSCs transplantation remain unanswered. There is an urgent need to identify MSCs from the beating heart and analyze the efficacy of this new approach. This study aimed to localize the magnetically labeled MSCs (MR-MSCs) and monitor the restorative effects of MR-MSCs with magnetic resonance (MR) imaging. Methods Acute myocardial infarction (AMI) was created in swine by a balloon occlusion of the left anterior descending coronary artery. Cells were delivered via intracoronary infusion after myocardial infarction. Infarct size change and cardiac function were assessed with 3.0T MR scanner. The results were then confirmed by histological and western blot analysis. All statistical procedures were performed with Systat (SPSS version 12.01). Results A total of 26 swine were divided into four groups (sham-operated group, n=6; AMI group with PBS transplantation, n=6; labeled MSCs group, n=7; unlabeled MSCs group, n=7). MSCs, MR-MSCs (10~cells) or PBS were delivered by intracoronary injection after MI and serial cardiac MR imaging studies were performed at 0, 4 and 8 weeks after transplantation. MR imaging demonstrated MI size decreased after MSCs transplantation in labeled and unlabeled groups, however, increases were seen in the AMI group at 8 weeks after MI. The left ventricular ejection fraction (LVEF) was slightly increased in the AMI group ((41.87~2.45)% vs (39.04~2.80)%, P 〉0.05), but significantly improved in the MR-MSCs group ((56.85~1.29)% vs (40.67~2.00)%, P 〈0.05) and unlabeled group ((55.38~1.07)% vs (41.78~2.08)%, P 〈0.05) at 8 weeks after treatment. MR-MSCs were further confirmed by Prussian blue and immunofluorescent staining. Western blot analysis demonstrated that there was an increased expression of cardiomyocyte markers such as myosin heavy chain and troponin T in the MSCs trea
QI Chun-meiMA Gen-shanLIU Nai-fengSHEN Cheng-xingCHEN ZhongLIU Xiao-junHU Yao-pengZHANG Xiao-liTENG Gao-junJU Sheng-hongMA MingTANG Yao-liang
Efficiently tracking of stem cells in vivo using different kinds of superparamagnetic iron oxide in swine with myocardial infarction被引量:3
2011年
Background Superparamagnetic iron oxide (SPIO) particles have shown much promise as a means to visualize labeled cells using molecular magnetic resonance imaging (MRI). Micrometer-sized superparamagnetic iron oxide (MPIO)particles and nanometer-sized ultrasmall superparamagnetic iron oxide (USPIO) are two kinds of SPIO widely used for monitoring stem cells migration. Here we compare the efficiency of two kinds of SPIO during the use of stem cells to treat acute myocardial infarction (AMI).Methods An AMI model in swine was created by 60 minutes of balloon occlusion of the left anterior descending coronary artery. Two kinds of SPIO particles were used to track after intracoronary delivered 107 magnetically labeled mesenchymal stem cells (MR-MSCs). The distribution and migration of the MR-MSCs were assessed with the use of 3.0T MR scanner and then the results were confirmed by histological examination.Results MR-MSCs appeared as a local hypointense signal on T2 -weighted MRI and there was a gradual loss of the signal intensity after intracoronary transplantation. All of the hypointense signals in the USPIO-labeled group were found on T2 -weighted MRI, contrast to noise ratio (CNR) decreased in the MPIO-labeled group (16.07±5.85 vs. 10.96±1.34)and USPIO-labeled group (11.72±1.27 vs. 10.03±0.96) from 4 to 8 weeks after transplantation. However, the hypointense signals were not detected in MPIO-labeled group in two animals. MRI and the results were verified by histological examination.Conclusions We demonstrated that two kinds of SPIO particles in vitro have similar labeling efficiency and viability.USPIO is more suitable for labeling stem cells when they are transplanted via a coronary route.
MA Gen-shanQI Chun-meiLIU Nai-fengSHEN Cheng-xingCHEN ZhongLIU Xiao-junHU Yao-pengZHANG Xiao-liTENG Gao-junJU Sheng-hongMA MingTANG Yao-liang
血红素氧化酶-1基因修饰的自体骨髓间充质干细胞移植治疗猪急性心肌梗死被引量:2
2009年
目的研究骨髓间充质干细胞(MSC)经血红素氧化酶-1(HO-1)基因修饰后移植对急性心肌梗死的治疗作用。方法细胞分为3组,未转染质粒组(MSC组)、转染空载质粒组(LacZ—MSC组)、转染pcDNA3.1-hHO—1组(HO-1-MSC组),体外实验予缺氧诱导观察HO-1基因转染后MSC的抗凋亡情况,同时收集上清液检测血管内皮生长因子(VEGF)的表达。体内实验建立猪的急性心肌梗死模型,梗死1h再灌注1h后分为3组,即生理盐水组、单纯干细胞治疗组(MSC组)及HO-1基因转染干细胞治疗组(HO-1-MSC组)。治疗组分别予MSC及HO-1-MSC移植治疗,对照组则注入等量生理盐水。细胞移植后1周及3个月行磁共振检测。3个月后处死动物,取心脏标本行相关检查。结果(1)体外缺氧诱导实验中HO-1-MSC组凋亡率(30.30±7.64)%低于MSC组(56.93±4.68)%(P〈0.001)和LacZ—MSC组(55.88±4.38)%(P〈0.001)。同时上清液中VEGF的分泌HO-1-MSC组(768.44±78.38)pg/ml高于Msc组(555.27±67.67)pg/ml(P〈0.001)和LacZ-MSC组(522.97±71.45)pg/ml(P〈0.001)。(2)细胞移植3个月后HO-1-MSC组LVEF(53.50±2.09)%明显高于MSC组(49.54±2.74)%(P=0.017)。梗死周边区毛细血管密度(血管数/HPF)HO-1-MSC组14.594-2.39亦大于MSC组11.78±2.48(P=0.033)。结论HO-1基因转染MSC较单纯MSC移植治疗急性心肌梗死疗效明显。
蒋益波陈立娟唐耀亮马根山祈春梅朱琪张晓黎姚玉宇刘乃丰沈成兴
关键词:心肌梗死间质干细胞移植血红素氧化酶-1
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