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视神经损伤后 BM88 的下调。

Downregulation of BM88 after optic nerve injury.

机构信息

MiNDS Graduate Program in Neuroscience, McMaster University, Hamilton, Ontario, Canada.

出版信息

Invest Ophthalmol Vis Sci. 2014 Mar 28;55(3):1919-29. doi: 10.1167/iovs.13-12986.

Abstract

PURPOSE

BM88 is a cell-cycle exit and neuronal differentiation protein that has been used as a marker of surviving retinal ganglion cells (RGCs) after optic nerve injury. Thy1.1 has also been used as a marker for RGC loss, but after optic nerve crush (ONC) a decrease in Thy1.1 expression precedes the loss of RGCs. The purpose of this study was to determine if BM88 expression was correlated with RGC loss after ONC and optic nerve transection (ONT) injuries.

METHODS

Rats were injected with Fluorogold (FG) into the superior colliculus to label RGCs and received ONC or ONT 7 days later. Eyes were collected 2 to 28 days after injury. Retinas were labeled with BM88 and intensity of the BM88 cell labeling was measured.

RESULTS

In control retinas, 98.9% of RGCs were immunoreactive (-IR) for BM88. There was a significant downregulation of BM88 by 52% to 80% of RGCs 7 days after ONC or ONT. The staining intensity of the remaining labeled cells was reduced to 41% to 51% of the control after 28 days of optic nerve injury. However, early in the injury there was a significant increase in the staining intensity of BM88.

CONCLUSIONS

Nearly all BM88-IR RGCs colocalized with FG-labeled RGCs in control retinas. However, both the number of BM88-IR RGCs and their intensity decreased gradually between 4 and 28 days, preceding the loss of FG-labeled cells. These findings indicate that BM88 is not a good marker of surviving RGCs but may indicate abnormal RGC functioning, which precedes cell death.

摘要

目的

BM88 是一种细胞周期退出和神经元分化蛋白,已被用作视神经损伤后存活的视网膜神经节细胞(RGC)的标志物。Thy1.1 也被用作 RGC 丢失的标志物,但在视神经挤压(ONC)后,Thy1.1 表达的减少先于 RGC 的丢失。本研究的目的是确定 BM88 表达是否与 ONC 和视神经横断(ONT)损伤后 RGC 丢失相关。

方法

将荧光金(FG)注射到上丘以标记 RGC,并在 7 天后接受 ONC 或 ONT。在损伤后 2 至 28 天收集眼睛。用 BM88 标记视网膜,并测量 BM88 细胞标记的强度。

结果

在对照视网膜中,98.9%的 RGC 对 BM88 呈免疫反应性(-IR)。在 ONC 或 ONT 后 7 天,有 52%至 80%的 RGC 对 BM88 表达显著下调。在视神经损伤 28 天后,剩余标记细胞的染色强度降低至对照的 41%至 51%。然而,在损伤早期,BM88 的染色强度显著增加。

结论

在对照视网膜中,几乎所有的 BM88-IR RGC 与 FG 标记的 RGC 共定位。然而,在 4 至 28 天之间,BM88-IR RGC 的数量及其强度逐渐下降,先于 FG 标记细胞的丢失。这些发现表明 BM88 不是存活的 RGC 的良好标志物,但可能表明异常的 RGC 功能,这先于细胞死亡。

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