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经鼻中隔途径的强化水凝胶包封 hMSC 治疗脑损伤。

Reinforced-hydrogel encapsulated hMSCs towards brain injury treatment by trans-septal approach.

机构信息

Nano-Bio Regenerative Medical Institute, College of Medicine, Hallym University, 1 Hallymdaehak-gil, Chuncheon, Gangwon-do, 24252, Republic of Korea.

Department of Physiology, Hallym University College of Medicine, Chuncheon, 24252, Republic of Korea.

出版信息

Biomaterials. 2021 Jan;266:120413. doi: 10.1016/j.biomaterials.2020.120413. Epub 2020 Sep 30.

Abstract

Encapsulated stem cells in various biomaterials have become a potentially promising cell transplantation strategy in the treatment of various neurologic disorders. However, there is no ideal cell delivery material and method for clinical application in brain diseases. Here we show silk fibroin (SF)-based hydrogel encapsulated engineered human mesenchymal stem cells (hMSCs) to overproduce brain-derived neurotrophic factor (BDNF) (BDNF-hMSC) is an effective approach to treat brain injury through trans-septal cell transplantation in the rat model. In this study, we observed SF induced sustained BDNF production by BDNF-hMSC both in 2D (9.367 ± 1.969 ng/ml) and 3D (7.319 ± 0.1025 ng/ml) culture conditions for 3 days. Through immunohistochemistry using α-tubulin, BDNF-hMSCs showed a significant increased average neurite length of co-cultured neuro 2a (N2a) cells, suggested that BDNF-hMSCs induced neurogenesis in vitro. Encapsulated BDNF-hMSC, pre-labeled with the red fluorescent dye PKH-26, exhibited intense fluorescence up to 14 days trans-septal transplantation, indicated excellent viability of the transplanted cells. Compared to the vehicle-treated, encapsulated BDNF- hMSC demonstrated significantly increased BDNF level both in the sham-operated and injured hippocampus (Hip) through immunoblot analysis after 7 days implantation. Transplantation of the encapsulated BDNF-hMSC promoted neurological functional recovery via significantly reduced neuronal death in the Hip 7 days post-injury. Using magnetic resonance imaging (MRI) analysis, we demonstrated that encapsulated BDNF-hMSC reduced lesion area significantly at 14 and 21 days in the damaged brain following trans-septal implantation. This stem cell transplantation approach represents a critical set up towards brain injury treatment for clinical application.

摘要

各种生物材料包封的干细胞已成为治疗各种神经疾病的潜在有前途的细胞移植策略。然而,在脑疾病的临床应用中,还没有理想的细胞输送材料和方法。在这里,我们展示了丝素蛋白(SF)基水凝胶包封的工程人间充质干细胞(hMSC)过表达脑源性神经营养因子(BDNF)(BDNF-hMSC),通过在大鼠模型中的经隔细胞移植是治疗脑损伤的有效方法。在这项研究中,我们观察到 SF 在 2D(9.367±1.969ng/ml)和 3D(7.319±0.1025ng/ml)培养条件下诱导 BDNF-hMSC 持续产生 BDNF 3 天,分别为 9.367±1.969ng/ml 和 7.319±0.1025ng/ml。通过使用α-微管蛋白的免疫组织化学,BDNF-hMSC 显示出共培养的神经 2a(N2a)细胞的平均神经突长度显着增加,表明 BDNF-hMSC 在体外诱导了神经发生。用红色荧光染料 PKH-26 预先标记的包封的 BDNF-hMSC 表现出强烈的荧光,直到 14 天经隔移植,表明移植细胞具有极好的活力。与载体处理相比,包封的 BDNF-hMSC 在植入后 7 天通过免疫印迹分析在假手术和受伤的海马体(Hip)中均显示出 BDNF 水平显着增加。包封的 BDNF-hMSC 的移植通过在受伤后 7 天减少 Hip 中的神经元死亡,促进了神经功能的恢复。使用磁共振成像(MRI)分析,我们证明了在经隔植入后 14 和 21 天,包封的 BDNF-hMSC 在受损大脑中显着减少了病变面积。这种干细胞移植方法代表了向临床应用中的脑损伤治疗迈出的关键一步。

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