School of Optometry, University of California, Berkeley, California 94720-2020, USA.
Invest Ophthalmol Vis Sci. 2010 Jun;51(6):3100-6. doi: 10.1167/iovs.09-4593. Epub 2010 Feb 3.
PURPOSE: Contact lens wear predisposes to Pseudomonas aeruginosa keratitis, but the mechanisms involved remain unclear. An in vivo model was used to study lens inoculation conditions enabling disease. METHODS: Custom-made hydrogel contact lenses were fitted to rats after incubation in P. aeruginosa approximately 10(11) cfu/mL (3 hours) or approximately 10(3) cfu/mL (24 hours). Another group was inadvertently inoculated with a suction pen previously used with high inocula, but rinsed in ethanol and stored dry (6 months). Some corneas were tissue paper-blotted to cause fluorescein staining before lens fitting. Contralateral eyes were untreated. Twenty-four hours after disease detection, lenses were transferred to naive rats or examined by confocal microscopy before homogenization to quantify viable bacteria. After lens removal, corneas were washed to collect nonadherent bacteria and were analyzed by immunohistochemistry. RESULTS: All eyes challenged with unworn contaminated lenses developed keratitis after approximately 7 to 10 days. Disease delay and severity were unaffected by inoculum parameters or tissue blotting but occurred sooner with lenses transferred from infected eyes ( approximately 2 days). Worn lenses and corneal washes contained infecting bacteria. Posterior, not anterior, lens surfaces harbored P. aeruginosa biofilms that penetrated the lens matrix. Diseased corneas showed an infiltration of phagocytes and T-lymphocytes. CONCLUSIONS: P. aeruginosa induces keratitis in this lens-wearing model after a single inoculation. Delayed disease onset was interesting considering the greater keratitis risk during extended wear. Infection did not require the disruption of corneal barrier function before lens wear and occurred without exposure to lens care solutions. The data suggest that keratitis involves biofilm formation or other bacterial adaptations in vivo.
目的:隐形眼镜的佩戴会导致绿脓杆菌角膜炎,但其中涉及的机制尚不清楚。本研究使用体内模型来研究导致疾病的隐形眼镜接种条件。
方法:将经过大约 10(11)cfu/mL(3 小时)或大约 10(3)cfu/mL(24 小时)的绿脓杆菌孵育的定制水凝胶隐形眼镜佩戴在大鼠上。另一组大鼠则意外地接种了之前用于高接种量的吸管,但在乙醇中冲洗并干燥储存(6 个月)。一些角膜在佩戴隐形眼镜之前用纸巾擦拭以引起荧光素染色。对侧眼睛未进行处理。在疾病检测后 24 小时,将隐形眼镜转移到未感染的大鼠身上,或在进行匀浆以量化活菌之前通过共聚焦显微镜进行检查。移除隐形眼镜后,用角膜冲洗液收集非黏附细菌,并通过免疫组织化学进行分析。
结果:所有用未经佩戴的污染隐形眼镜进行挑战的眼睛在大约 7 至 10 天后均发展为角膜炎。接种物参数或组织擦拭对疾病的延迟和严重程度没有影响,但从感染眼睛转移的隐形眼镜会更早发生(大约 2 天)。佩戴的隐形眼镜和角膜冲洗液中含有感染细菌。后表面,而不是前表面,隐形眼镜表面存在穿透隐形眼镜基质的绿脓杆菌生物膜。患病的角膜显示出吞噬细胞和 T 淋巴细胞的浸润。
结论:在单次接种后,这种佩戴隐形眼镜的模型中绿脓杆菌会引起角膜炎。考虑到延长佩戴时间会增加角膜炎的风险,疾病的延迟发作很有趣。在佩戴隐形眼镜之前,感染并不需要破坏角膜屏障功能,并且在没有接触隐形眼镜护理溶液的情况下发生。这些数据表明角膜炎涉及生物膜形成或其他细菌在体内的适应。
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