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小鼠创伤性脑损伤后的急性玻璃体视网膜创伤与炎症

Acute vitreoretinal trauma and inflammation after traumatic brain injury in mice.

作者信息

Evans Lucy P, Newell Elizabeth A, Mahajan MaryAnn, Tsang Stephen H, Ferguson Polly J, Mahoney Jolonda, Hue Christopher D, Vogel Edward W, Morrison Barclay, Arancio Ottavio, Nichols Russell, Bassuk Alexander G, Mahajan Vinit B

机构信息

Medical Scientist Training Program University of Iowa Iowa City Iowa.

Department of Pediatrics University of Iowa Iowa City Iowa.

出版信息

Ann Clin Transl Neurol. 2018 Feb 26;5(3):240-251. doi: 10.1002/acn3.523. eCollection 2018 Mar.

Abstract

OBJECTIVE

Limited attention has been given to ocular injuries associated with traumatic brain injury (TBI). The retina is an extension of the central nervous system and evaluation of ocular damage may offer a less-invasive approach to gauge TBI severity and response to treatment. We aim to characterize acute changes in the mouse eye after exposure to two different models of TBI to assess the utility of eye damage as a surrogate to brain injury.

METHODS

A model of blast TBI (bTBI) using a shock tube was compared to a lateral fluid percussion injury model (LFPI) using fluid pressure applied directly to the brain. Whole eyes were collected from mice 3 days post LFPI and 24 days post bTBI and were evaluated histologically using a hematoxylin and eosin stain.

RESULTS

bTBI mice showed evidence of vitreous detachment in the posterior chamber in addition to vitreous hemorrhage with inflammatory cells. Subretinal hemorrhage, photoreceptor degeneration, and decreased cellularity in the retinal ganglion cell layer was also seen in bTBI mice. In contrast, eyes of LFPI mice showed evidence of anterior uveitis and subcapsular cataracts.

INTERPRETATION

We demonstrated that variations in the type of TBI can result in drastically different phenotypic changes within the eye. As such, molecular and phenotypic changes in the eye following TBI may provide valuable information regarding the mechanism, severity, and ongoing pathophysiology of brain injury. Because vitreous samples are easily obtained, molecular changes within the eye could be utilized as biomarkers of TBI in human patients.

摘要

目的

与创伤性脑损伤(TBI)相关的眼部损伤受到的关注有限。视网膜是中枢神经系统的延伸,评估眼部损伤可能提供一种侵入性较小的方法来衡量TBI的严重程度和对治疗的反应。我们旨在描述小鼠眼睛在暴露于两种不同的TBI模型后的急性变化,以评估眼部损伤作为脑损伤替代指标的效用。

方法

将使用冲击管的爆炸型TBI(bTBI)模型与直接向脑部施加流体压力的侧方流体冲击伤模型(LFPI)进行比较。在LFPI后3天和bTBI后24天从小鼠收集全眼,并使用苏木精和伊红染色进行组织学评估。

结果

bTBI小鼠除了有伴有炎性细胞的玻璃体积血外,还在后房出现玻璃体脱离的迹象。在bTBI小鼠中还可见视网膜下出血、光感受器退变以及视网膜神经节细胞层细胞数量减少。相比之下,LFPI小鼠的眼睛出现前葡萄膜炎和囊下白内障的迹象。

解读

我们证明了TBI类型的差异可导致眼内截然不同的表型变化。因此,TBI后眼睛的分子和表型变化可能提供有关脑损伤的机制、严重程度和持续病理生理学的有价值信息。由于玻璃体样本易于获取,眼内的分子变化可作为人类患者TBI的生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4cb7/5846452/87e576b9f434/ACN3-5-240-g001.jpg

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