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靶向胆固醇稳态可改善实验性视神经炎的恢复。

Targeting Cholesterol Homeostasis Improves Recovery in Experimental Optic Neuritis.

机构信息

Department of Ophthalmology and Visual Sciences, University of Iowa, Iowa City, IA 52242, USA.

Center for the Prevention and Treatment of Visual Loss, Iowa City VA Health Care System, Iowa City, IA 52246, USA.

出版信息

Biomolecules. 2022 Oct 7;12(10):1437. doi: 10.3390/biom12101437.

Abstract

Acute optic neuritis (ON) is a common cause of vision loss and is often associated with multiple sclerosis (MS). Cholesterol recycling has been identified as a key limiting factor in recovery after demyelination events. Thus, the purpose of our study was to determine if the augmentation of cholesterol transport by gentisic acid (GA) benefits retinal ganglion cell (RGC) development and myelination in organoid systems and enables the recovery of the ocular phenotype upon systemic GA treatment in a MOG-induced experimental autoimmune encephalomyelitis (EAE) ON model. The retinal organoids treated with GA demonstrate an accelerated maturation when compared to the conventionally derived organoids, which was evidenced by the improved organization of Brn3a-GFPRGC and increased synaptogenesis. A GA supplementation in brain organoids leads to a 10-fold increase in NG2 and Olig2 expression. Weekly GA injections of EAE mice significantly lessened motor-sensory impairment, protected amplitudes in pattern electroretinogram recordings, and preserved visual acuity over the study period of 56 days. Furthermore, GA-treated EAE mice revealed diminished GCL/IPL complex thinning when compared to the untreated EAE mice. An optic nerve histopathology revealed less severe grades of demyelination in the GA-treated EAE cohort and fewer infiltrating cells were observed. Interventions to improve cholesterol homeostasis may be a viable approach to promoting the rehabilitation of MS patients.

摘要

急性视神经炎(ON)是视力丧失的常见原因,常与多发性硬化症(MS)有关。胆固醇循环已被确定为脱髓鞘事件后恢复的关键限制因素。因此,我们的研究目的是确定 Gentisic 酸(GA)是否可以增强胆固醇转运,从而有益于类器官系统中的视网膜神经节细胞(RGC)发育和髓鞘形成,并在 MOG 诱导的实验性自身免疫性脑脊髓炎(EAE)ON 模型中通过全身 GA 治疗恢复眼部表型。与传统衍生的类器官相比,用 GA 处理的视网膜类器官表现出更快的成熟,这表现在 Brn3a-GFPRGC 的组织改善和突触发生增加。在脑类器官中补充 GA 会导致 NG2 和 Olig2 表达增加 10 倍。每周对 EAE 小鼠进行 GA 注射可显著减轻运动感觉障碍,保护模式视网膜电图记录中的幅度,并在 56 天的研究期间保持视力。此外,与未治疗的 EAE 小鼠相比,GA 治疗的 EAE 小鼠的 GCL/IPL 复合体变薄程度降低。视神经组织病理学显示,GA 治疗的 EAE 队列中的脱髓鞘程度较轻,并且观察到的浸润细胞较少。改善胆固醇动态平衡的干预措施可能是促进 MS 患者康复的可行方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0d0d/9599133/98f7af9d504a/biomolecules-12-01437-g001.jpg

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