角膜机械性内皮损伤和基底膜成分巢蛋白-1 产生引发的后基质细胞凋亡。
Posterior stromal cell apoptosis triggered by mechanical endothelial injury and basement membrane component nidogen-1 production in the cornea.
机构信息
Cole Eye Institute, Cleveland Clinic, Cleveland, OH, USA; University of Sao Paulo, Sao Paulo, Brazil.
Cole Eye Institute, Cleveland Clinic, Cleveland, OH, USA.
出版信息
Exp Eye Res. 2018 Jul;172:30-35. doi: 10.1016/j.exer.2018.03.025. Epub 2018 Mar 27.
This study was performed to determine whether cells in the posterior stroma undergo apoptosis in response to endothelial cell injury and to determine whether basement membrane component nidogen-1 was present in the cornea. New Zealand White rabbits had an olive tip cannula inserted into the anterior chamber to mechanically injure corneal endothelial cells over an 8 mm diameter area of central cornea with minimal injury to Descemet's membrane. At 1 h (6 rabbits) and 4 h (6 rabbits) after injury, three corneas at each time point were cryopreserved in OCT for terminal deoxynucleotidyl transferase dUTP nick end labeling (TUNEL) assay and immunohistochemistry (IHC) for vimentin and nidogen-1, and three corneas at each time point were fixed for transmission electron microscopy (TEM). Uninjured corneas were controls. Stromal cells over approximately the posterior 25% of the stroma overlying to the site of corneal endothelial injury underwent apoptosis detected by the TUNEL assay. Many of these apoptotic cells were vimentin+, suggesting they were likely keratocytes or corneal fibroblasts. Stromal cells peripheral to the site of endothelial injury and more anterior stromal cells overlying the site of endothelial injury did not undergo apoptosis. Stromal cell death was confirmed to be apoptosis by TEM. No apoptosis of stromal cells was detected in control, uninjured corneas. Nidogen-1 was detected in the stroma of unwounded corneas, with higher nidogen-1 in the posterior stroma than the anterior stroma. After endothelial scrape injury, concentrations of nidogen-1 appeared to be in the extracellular matrix of the posterior stroma and, possibly, within apoptotic bodies of stromal cells. Thus, posterior stromal cells, likely including keratocytes, undergo apoptosis in response to corneal endothelial injury, analogous to anterior keratocytes undergoing apoptosis in response to epithelial injury.
本研究旨在确定后弹力层中的细胞是否会在角膜内皮细胞受损时发生凋亡,并确定角膜中是否存在基底膜成分巢蛋白-1。新西兰白兔的前房内插入了一个橄榄尖端套管,以机械方式损伤中央角膜 8mm 直径区域内的角膜内皮细胞,对 Descemet 膜的损伤最小。在损伤后 1 小时(6 只兔子)和 4 小时(6 只兔子),每个时间点的 3 只角膜在 OCT 中冷冻保存,用于末端脱氧核苷酸转移酶 dUTP 缺口末端标记(TUNEL)测定和波形蛋白和巢蛋白-1 的免疫组织化学(IHC),每个时间点的 3 只角膜用于透射电子显微镜(TEM)固定。未受伤的角膜为对照。通过 TUNEL 测定检测到,位于角膜内皮损伤部位上方约后 25%的基质中的基质细胞发生凋亡。这些凋亡细胞中有许多是波形蛋白阳性的,提示它们可能是角膜成纤维细胞或角膜成纤维细胞。内皮损伤部位周围的基质细胞和位于内皮损伤部位上方的更靠前的基质细胞未发生凋亡。TEM 证实基质细胞死亡为凋亡。在对照的未受伤角膜中未检测到基质细胞凋亡。巢蛋白-1在前弹力层未受伤的角膜基质中被检测到,后弹力层中的巢蛋白-1浓度高于前弹力层。内皮刮伤后,巢蛋白-1 的浓度似乎出现在后弹力层的细胞外基质中,并且可能出现在基质细胞的凋亡小体中。因此,后弹力层细胞,可能包括角膜成纤维细胞,在角膜内皮细胞受损时发生凋亡,类似于前角膜成纤维细胞在受到上皮细胞损伤时发生凋亡。
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