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In vivo confocal microscopy of patients with corneal recurrent erosion syndrome or epithelial basement membrane dystrophy.

机译:患有角膜复发性侵蚀综合征或上皮基底膜营养不良的患者的体内共聚焦显微镜检查。

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OBJECTIVE: To characterize morphologic changes in corneas of patients with recurrent erosion syndrome or epithelial basement membrane dystrophy using in vivo confocal microscopy. DESIGN: Observational case series PARTICIPANTS: Fourteen eyes of eight patients with diagnosed epithelial basement membrane dystrophy and 13 eyes of seven patients with recurrent erosion syndrome were examined. METHODS: Slit-lamp examination and in vivo confocal microscopy. The pathologic findings are presented as digitized images obtained from video tape recorded during the confocal microscopy. MAIN OUTCOME MEASURES: The morphology of corneal surface epithelial cells, basal epithelial cells, subbasal nerve plexus, Bowman's layer, stromal keratocytes, and endothelium was analyzed. RESULTS: The surface epithelium was intact in all but two eyes. One cornea (a basement membrane disorder with clinically visible dots) had multinucleate surface epithelial cells, and one eye with recurrent corneal erosions showed a freely floating surface epithelium sheet in the tear fluid. Patients in both groups showed islets of highly reflective cells with presumed intracellular deposits surrounded by normal cells in the basal epithelial cell layer. The basal epithelial cell area also showed other pathologic changes, including drop-shaped configurations, streaks, or ridges. Folding of the Bowman's layer was also observed in both groups. Anterior keratocytes showed signs of activation (highly reflective nuclei with visible processes) in some of the patients regardless of the clinical diagnosis, and in recurrent erosions even increased deposition of abnormal extracellular matrix in the anterior stroma was suspected. Posterior corneal keratocytes and endothelium appeared normal when examined. The subbasal nerve plexus showed various pathologic changes, such as short or strangely shaped nerve fiber bundles, decreased numbers of long nerve fiber bundles, only faintly visible long nerve fiber bundles (instead of the normally observed long parallel running interconnected bundles), or increased amounts of Langerhans cells, but only one patient (with recurrent erosion syndrome) lacked the subbasal nerve plexus. CONCLUSIONS: In vivo confocal microscopy of corneas with recurrent erosions or epithelial basement membrane dystrophy showed deposits in basal epithelial cells, subbasal microfolds and streaks, damaged subbasal nerves, or altered morphology of the anterior stroma. Confocal microscopy cannot replace biomicroscopy in making a specific diagnosis, but it sometimes helps the diagnosis in corneas that appear normal under a biomicroscope.
机译:目的:利用体内共聚焦显微镜对复发性侵蚀综合征或上皮基底膜营养不良患者的角膜形态学特征进行表征。设计:观察病例系列研究对象:检查了八名被诊断为上皮基底膜营养不良的患者的十四只眼和七名复发性侵蚀综合征的十三只眼。方法:裂隙灯检查和体内共聚焦显微镜检查。病理结果显示为从共聚焦显微镜下录制的录像带获得的数字化图像。主要观察指标:分析角膜表面上皮细胞,基底上皮细胞,基底下神经丛,鲍曼层,基质角膜细胞和内皮的形态。结果:除两只眼睛外,所有其他动物的表面上皮均完好无损。一只角膜(具有临床上可见的点的基底膜疾病)具有多核表面上皮细胞,而一只眼角膜反复侵蚀的眼睛在泪液中显示出自由漂浮的表面上皮片。两组患者均显示出高反射性细胞的胰岛,推测其细胞内沉积物被基底上皮细胞层中的正常细胞所包围。基底上皮细胞区域还显示出其他病理变化,包括滴状构型,条纹或隆起。在两组中也观察到鲍曼层的折叠。不论临床诊断如何,某些患者的前角膜细胞均显示出活化迹象(具有可见过程的高度反射核),在复发性糜烂中,甚至怀疑前基质中异常细胞外基质的沉积增加。检查时,角膜后角膜细胞和内皮细胞看起来正常。基底下神经丛表现出各种病理变化,例如神经纤维束短或形状异常,神经纤维束的数量减少,仅神经纤维束的可见性较弱(而不是通常观察到的长平行运行的互连束)或数量增加的朗格汉斯细胞,但只有一名患者(复发性糜烂综合征)缺乏基底下神经丛。结论:体内共聚焦显微镜下的角膜反复糜烂或上皮基底膜营养不良,显示在基底上皮细胞中沉积,基底下微褶和条纹,基底下神经受损或前基质的形态改变。共聚焦显微镜不能代替生物显微镜进行特定的诊断,但有时可以帮助在生物显微镜下看起来正常的角膜进行诊断。

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