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感染性结晶状角膜炎。

Infectious crystalline keratopathy.

机构信息

City Eye Centre, Brisbane, Queensland, Australia.

City Eye Centre, Brisbane, Queensland, Australia; University of Queensland, Brisbane, Queensland, Australia; Mater Health Services, Brisbane, Queensland, Australia.

出版信息

Surv Ophthalmol. 2018 Jul-Aug;63(4):480-499. doi: 10.1016/j.survophthal.2017.10.008. Epub 2017 Oct 31.

Abstract

Infectious crystalline keratopathy was first reported by Gorovoy and colleagues in 1983 when they identified bacteria colonizing a cornea after a penetrating keratoplasty. Subsequent cases have elaborated on the organisms responsible and the management outcomes. Patients present with a white or gray branching opacity originating from an epithelial defect, commonly after a penetrating keratoplasty. Local immunosuppression contributes to the quiescent nature and the limited inflammatory response associated with infectious crystalline keratopathy. Diagnosis of the infective pathogens may be difficult, with a corneal scraping often being too superficial to obtain an adequate specimen. A biofilm is present that advantages microorganism survival, reduces antibiotic bioavailability, and inhibits diagnostic microbial detection. Treatment begins with topical antimicrobials, initially broad spectrum and then targeted to microorganism sensitivity. Adjunctive therapies to enhance the efficacy of treatment include disruption of the microorganism biofilm by laser, intrastromal antibiotics, and keratectomy. In recalcitrant cases, or where corneal scarring ensues, corneal transplantation is required.

摘要

感染性结晶状角膜炎于 1983 年由 Gorovoy 及其同事首次报道,当时他们在穿透性角膜移植术后发现细菌定植于角膜。随后的病例进一步阐述了致病生物体和治疗结果。患者表现为源自上皮缺损的白色或灰色分支状混浊,常见于穿透性角膜移植术后。局部免疫抑制导致感染性结晶状角膜炎的静止性质和有限的炎症反应。感染病原体的诊断可能具有挑战性,因为角膜刮片往往太浅,无法获得足够的标本。生物膜的存在有利于微生物的存活,降低抗生素的生物利用度,并抑制微生物检测。治疗始于局部使用抗生素,最初是广谱的,然后针对微生物敏感性进行靶向治疗。增强治疗效果的辅助治疗包括激光破坏微生物生物膜、间质内抗生素和角膜切除术。在难治性病例或出现角膜瘢痕的情况下,需要进行角膜移植。

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