首页> 美国卫生研究院文献>other >COMBINATION TREATMENT OF STROKE WITH SUB-THERAPEUTIC DOSES OF SIMVASTATIN AND HUMAN UMBILICAL CORD BLOOD CELLS ENHANCES VASCULAR REMODELING AND IMPROVES FUNCTIONAL OUTCOME
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COMBINATION TREATMENT OF STROKE WITH SUB-THERAPEUTIC DOSES OF SIMVASTATIN AND HUMAN UMBILICAL CORD BLOOD CELLS ENHANCES VASCULAR REMODELING AND IMPROVES FUNCTIONAL OUTCOME

机译:血管脱落素和人脐脐带血细胞患者中风的组合治疗提高了血管重塑并改善了功能结果

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摘要

Human umbilical cord blood cells (HUCBCs) have been employed as a restorative treatment for experimental stroke. In this study, we investigated whether transplantation of sub-therapeutic doses of HUCBCs and Simvastatin enhances cerebral vascular remodeling after stroke. Adult male Wistar rats (n=34) were subjected to transient middle cerebral artery occlusion (MCAo) and treated with: phosphate buffered solution (PBS, gavaged daily for 7 days); Simvastatin (0.5mg/kg, gavaged daily for 7 days); HUCBCs (1x106, injected once via tail vein); and combination Simvasatin with HUCBCs, starting at 24 h after MCAo. There was no significant difference between Simvastatin- or HUCBC-monotherapy and MCAo-alone group. Combination treatment 24 h post-stroke significantly increased the perimeter of von Willebrand factor (vWF)-positive vessels, the diameter and density of alpha smooth muscle actin ( SMA)-positive arteries, and the percentage of BrdU-positive endothelial cells (ECs) in the ischemic boundary zone (IBZ) compared with MCAo-alone or HUCBC-monotherapy 14 days after MCAo (p<0.05, n=8/group); Combination treatment significantly increased the densities of vWF-vessels and SMA-arteries as well as the densities of BrdU-ECs and BrdU-positive smooth muscle cells (SMCs) in vascular walls in the IBZ compared with Simvastatin-monotherapy. Moreover, the increased BrdU-ECs and BrdU-SMCs were significantly correlated with neurological functional outcome 14 days after MCAo. Combination treatment also significantly increased the expression of Angiopoietin-1 (Ang1), Tie2 and Occludin in the IBZ (p<0.05, n=8/group). The in vitro experiments showed that combination treatment and Ang1 significantly increased capillary-like tube formation and arterial cell migration; anti-Ang1 significantly reduced combination treatment induced tube-formation and artery cell migration (p<0.05, n=6/group). These findings indicated that combination of sub-therapeutic doses of Simvastatin and HUCBCs treatment of stroke increases Ang1/Tie2 and Occludin expression in the ischemic brain, amplifies endogenous angiogenesis and arteriogenesis, and enhances vascular remodeling which in concert may contribute to functional outcome after stroke.
机译:人脐带血细胞(HUCBC)已被用作实验性中风的修复性治疗。在这项研究中,我们调查了亚治疗剂量的HUCBCs和辛伐他汀的移植是否可增强中风后的脑血管重构。对成年雄性Wistar大鼠(n = 34)进行短暂的大脑中动脉闭塞(MCAo),并用磷酸盐缓冲液(PBS,每天灌胃7天)进行处理;辛伐他汀(0.5mg / kg,每天灌胃7天); HUCBC(1x106,通过尾静脉注射一次);并在MCAo后24小时开始将Simvasatin与HUCBCs合并使用。辛伐他汀或HUCBC单一疗法与单独MCAo组之间没有显着差异。卒中后24小时的联合治疗显着增加了von Willebrand因子(vWF)阳性血管的周长,α平滑肌肌动蛋白(SMA)阳性动脉的直径和密度以及BrdU阳性内皮细胞(ECs)的百分比与单纯MCAo或HUCBC单药治疗相比,MCAo 14天后缺血边界区(IBZ)发生率更高(p <0.05,n = 8 /组);与辛伐他汀单一疗法相比,联合治疗显着增加了IBZ血管壁中vWF血管和SMA动脉的密度以及BrdU-EC和BrdU阳性平滑肌细胞(SMC)的密度。此外,MCAo后14天,BrdU-ECs和BrdU-SMCs的增加与神经功能预后显着相关。联合治疗还显着增加了IBZ中Angiopoietin-1(Ang1),Tie2和Occludin的表达(p <0.05,n = 8 /组)。体外实验显示,联合治疗和Ang1可以显着增加毛细血管样管的形成和动脉细胞的迁移。抗Ang1显着降低了联合治疗引起的管形成和动脉细胞迁移(p <0.05,n = 6 /组)。这些发现表明,亚治疗剂量的辛伐他汀和HUCBCs联合治疗中风会增加缺血性脑中Ang1 / Tie2和Occludin的表达,放大内源性血管生成和动脉生成,并增强血管重塑,共同可能有助于中风后的功能预后。

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