穿透性角膜移植术后50年黄斑角膜营养不良复发的研究。

GMS ophthalmology cases Pub Date : 2020-08-06 eCollection Date: 2020-01-01 DOI:10.3205/oc000161
Mona Bischoff-Jung, Elias Flockerzi, Andrea Hasenfus, Arne Viestenz, Pinio Matoula, Ursula Schlötzer-Schrehardt, Berthold Seitz
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引用次数: 1

摘要

目的:报告穿透性角膜移植术(PKP)后50年复发的黄斑角膜基质营养不良。方法:观察性病例报告病例描述:76岁男性患者,1962年发生PKP后50年出现右眼视力障碍(OD)(1968年左眼也发生PKP后44年)。由于双侧角膜混浊,他的视力在外伤前就已经受损。移植角膜的中心厚度分别为584µm(外径)和544µm(外径),而周围宿主厚度(8 mm区)分别为1233µm(外径,颅骨)和1131µm(外径,鼻腔)。双眼原移植角膜直径为6mm,受者角膜混浊,呈灰色。中心测量内皮细胞计数(OD 1162 c/mm2, OS 1320 c/mm2)。视力分别为20/100 (OD)和20/40 (OS)。实验激光辅助重复PKP (8.0/8.1 mm, OD)后,前移植物的组织学分析显示上皮下、界面内、供体间质和内皮中有酸性粘多糖(AMP)沉积,证明移植物周围性黄斑角膜间质营养不良复发。结论:角膜黄斑间质营养不良的复发率较低,但有可能发生在PKP术后数十年。在这个病人中,宿主基质的厚度是移植物基质的两倍。这可能是由于宿主内皮中酸性粘多糖的活性产生和继发性内皮失代偿所致。因此,PKP仍然是治疗黄斑角膜营养不良的长期视力康复的金标准。
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Recurrence of macular corneal dystrophy on the graft 50 years after penetrating keratoplasty.

Purpose: To report the recurrence of a macular corneal stromal dystrophy 50 years after penetrating keratoplasty (PKP). Methods: Observational case report Case description: A 76-year-old male patient presented with visual impairment in the right eye (OD) 50 years after PKP in 1962 (44 years after PKP also in the left eye (OS) in 1968) following explosion injury. His visual acuity had already been impaired before the trauma because of bilateral corneal opacities. The central corneal thickness of the graft measured 584 µm (OD) and 544 µm (OS), whilst the peripheral host thickness (8 mm zone), however, was 1233 µm (OD, cranial) and 1131 µm (OS, nasal). The original graft diameter measured 6 mm in both eyes and the recipient cornea was cloudy and gray. The endothelial cell count was measured centrally (OD 1162 c/mm2, OS 1320 c/mm2). The visual acuity was 20/100 (OD) and 20/40 (OS). After excimerlaser-assisted repeated PKP (8.0/8.1 mm, OD), the histological analysis of the former graft revealed deposits of acid mucopolysaccharides (AMP) subepithelially, within the interface, in the donor stroma, and in the endothelium, which proved the peripheral recurrence of a macular corneal stromal dystrophy on the graft. Conclusion: Recurrence of macular corneal stromal dystrophy is seldom, but it may occur many decades after PKP. In this patient, the host's stroma was twice as thick as that of the graft. This may be caused by the active production of acid mucopolysaccharides in the host endothelium with secondary endothelial decompensation. Thus, PKP remains the gold standard in the cure of macular corneal dystrophy for long-term visual rehabilitation.

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