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Mesenchymal Stem Cell–Derived Small Extracellular Vesicles Promote Neuroprotection in a Genetic DBA/2J Mouse Model of Glaucoma

机译:间充质干细胞衍生的小细胞外囊泡在青光眼的遗传DBA / 2J小鼠模型中促进神经保护。

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Purpose : To determine if bone marrow-derived stem cell (BMSC) small extracellular vesicles (sEV) promote retinal ganglion cell (RGC) neuroprotection in the genetic DBA/2J mouse model of glaucoma for 12 months. Methods : BMSC sEV and control fibroblast-derived sEV were intravitreally injected into 3-month-old DBA/2J mice once a month for 9 months. IOP and positive scotopic threshold responses were measured from 3 months: IOP was measured monthly and positive scotopic threshold responses were measured every 3 months. RGC neuroprotection was determined in wholemounts stained with RNA binding protein with multiple splicing (RBPMS), whereas axonal damage was assessed using paraphenylenediamine staining. Results : As expected, DBA/2J mice developed chronic ocular hypertension beginning at 6 months. The delivery of BMSC sEV, but not fibroblast sEV, provided significant neuroprotective effects for RBPMSsup+/sup RGC while significantly reducing the number of degenerating axons seen in the optic nerve. BMSC sEV significantly preserved RGC function in 6-month-old mice, but provided no benefit at 9 and 12 months. Conclusions : BMSC sEV are an effective neuroprotective treatment in a chronic model of ocular hypertension for 1 year, preserving RGC numbers and protecting against axonal degeneration.
机译:目的:确定在青光眼的遗传DBA / 2J小鼠模型中,骨髓源性干细胞(BMSC)的小细胞外囊泡(sEV)是否能促进视网膜神经节细胞(RGC)的神经保护12个月。方法:每月一次向3个月大的DBA / 2J小鼠玻璃体内注射BMSC sEV和源自成纤维细胞的sEV,共9个月。从3个月开始测量IOP和阳性暗视阈值反应:每月测量IOP,每3个月测量一次暗视阈值反应阳性。 RGC的神经保护作用是通过用RNA结合蛋白进行多次剪接(RBPMS)染色的整体来确定的,而使用对苯二胺染色来评估轴突的损伤。结果:正如预期的那样,DBA / 2J小鼠从6个月开始发展为慢性高眼压。 BMSC sEV而不是成纤维细胞sEV的传递对RBPMS + RGC提供了显着的神经保护作用,同时显着减少了在视神经中看到的变性轴突的数量。 BMSC sEV在6个月大的小鼠中显着保留了RGC功能,但在9个月和12个月时没有提供任何益处。结论:BMSC sEV是一种有效的神经保护性治疗方法,在慢性高眼压高血压模型中维持1年,可以保持RGC数量并防止轴突变性。

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