Inhibition of neovascularization but not fibrosis with the fluocinolone acetonide implant in autosomal dominant neovascular inflammatory vitreoretinopathy.

Paul S Tlucek, James C Folk, Jason A Orien, Edwin M Stone, Vinit B Mahajan
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引用次数: 17

Abstract

OBJECTIVE To review the effect of the fluocinolone acetonide implant in subjects with autosomal dominant neovascular inflammatory vitreoretinopathy (ADNIV), an inherited autoimmune uveitis. METHODS A retrospective case series was assembled from patients with ADNIV who received fluocinolone acetonide implants. Visual acuity and features of ADNIV, including inflammatory cells, neovascularization, fibrosis, and cystoid macular edema, were reviewed. RESULTS Nine eyes of 5 related patients with ADNIV with uncontrolled inflammation were reviewed. Follow-up ranged from 21.7 to 56.7 months. Visual acuity at implantation ranged from 20/40 to hand motion. Preoperatively, 8 eyes had vitreous cells (a ninth had diffuse vitreous hemorrhage). Eight eyes had cystoid macular edema, 7 had an epiretinal membrane, and 3 had retinal neovascularization. Following implantation, vitreous cells resolved in all eyes and neovascularization regressed or failed to develop. Central macular thickness improved in 4 eyes. During the postoperative course, however, visual acuity continued to deteriorate, with visual acuity at the most recent examination ranging from 20/60 to no light perception. There was also progressive intraocular fibrosis and phthisis in 1 case. Four eyes underwent cataract surgery. Six of the 7 eyes without previous glaucoma surgery had elevated intraocular pressure at some point, and 3 of these required glaucoma surgery. CONCLUSIONS The fluocinolone acetonide implant may inhibit specific features of ADNIV such as inflammatory cells and neovascularization but does not stabilize long-term vision, retinal thickening, or fibrosis. All eyes in this series required cataract extraction, and more than half required surgical intervention for glaucoma. Further studies may identify additional therapies and any benefit of earlier implantation.

醋酸氟西诺酮在常染色体显性遗传的新血管炎性玻璃体视网膜病变中的抑制新生血管形成而非纤维化作用
目的探讨氟西诺酮植入治疗常染色体显性遗传性新血管性炎症性玻璃体视网膜病变(ADNIV)的疗效。方法回顾性收集了接受氟西诺酮植入的ADNIV患者的病例系列。我们回顾了ADNIV的视力和特征,包括炎症细胞、新生血管、纤维化和囊样黄斑水肿。结果对5例伴有炎症控制的相关ADNIV患者9只眼进行回顾性分析。随访时间为21.7 - 56.7个月。植入时视力从20/40到手部运动。术前8只眼有玻璃体细胞(1 / 9有弥漫性玻璃体出血)。8只眼出现囊样黄斑水肿,7只眼出现视网膜前膜,3只眼出现视网膜新生血管。植入术后,所有眼的玻璃体细胞溶解,新生血管退化或未形成。4眼中央黄斑厚度改善。然而,在术后过程中,视力继续恶化,最近一次检查的视力从20/60到无光感。1例并发进行性眼内纤维化及肺结核。其中四只眼睛接受了白内障手术。未做过青光眼手术的7只眼睛中,有6只在某一时刻眼压升高,其中3只需要青光眼手术。结论氟西诺酮植入物可能抑制ADNIV的特异性特征,如炎症细胞和新生血管形成,但不能稳定长期视力、视网膜增厚或纤维化。所有的眼睛都需要白内障摘除,超过一半的人需要青光眼手术治疗。进一步的研究可能会确定额外的治疗方法和早期植入的任何益处。
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来源期刊
Archives of ophthalmology
Archives of ophthalmology 医学-眼科学
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3-8 weeks
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