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增殖性玻璃体视网膜病变的病理生理学及其治疗

The pathophysiology of proliferative vitreoretinopathy in its management.

作者信息

Ryan S J

出版信息

Am J Ophthalmol. 1985 Jul 15;100(1):188-93. doi: 10.1016/s0002-9394(14)75004-4.

Abstract

Cellular proliferation following retinal reattachment surgery frequently results in contraction and subsequent recurrent detachment of the retina, negating an initial successful reattachment. This process has been called by a variety of names, such as massive vitreous retraction, massive preretinal retraction, and, more recently, proliferative vitreoretinopathy. Although a good start has been made by the Retina Society to classify the various types of proliferative vitreoretinopathy, some modifications in the classification are required. The fundamental problem in the treatment of proliferative vitreoretinopathy is a lack of knowledge regarding the factors that stimulate the proliferation of cells. The vitreoretinal surgeon should recognize in the life cycle of this process that stage which an eye with retinal detachment has reached. If there is no active cellular proliferation, then a scleral buckle will usually suffice. If there is traction from epiretinal membranes which cannot be relieved by a buckle, then vitrectomy and adjunct procedures are necessary. If there is active cellular proliferation and epiretinal membranes, then the arguments related to proper timing of vitrectomy must be considered. In cases where the retinal holes can be identified and closed, scleral buckling may be performed with subsequent delayed vitrectomy. In most cases, in my experience, a combination of revision of the scleral buckle is required at the time of vitrectomy and membrane segmentation for proliferative vitreoretinopathy. Until such time as drugs are available to inhibit cellular proliferation or until our basic understanding of the cell biology of this process allows other means of pharmacologic intervention, mechanical approaches will remain necessary for the treatment of the most advanced cases.

摘要

视网膜复位手术后的细胞增殖常常导致视网膜收缩以及随后的复发性脱离,使最初的成功复位化为泡影。这个过程有多种叫法,如大量玻璃体后脱离、大量视网膜前膜收缩,以及最近的增殖性玻璃体视网膜病变。尽管视网膜协会在对增殖性玻璃体视网膜病变的各种类型进行分类方面已经有了良好开端,但仍需对分类进行一些修改。增殖性玻璃体视网膜病变治疗中的根本问题是缺乏对刺激细胞增殖因素的了解。玻璃体视网膜外科医生应该在这个过程的生命周期中识别出视网膜脱离的眼睛所处的阶段。如果没有活跃的细胞增殖,那么巩膜扣带术通常就足够了。如果存在视网膜前膜的牵拉,而扣带术无法缓解这种牵拉,那么玻璃体切除术及辅助手术就是必要的。如果存在活跃的细胞增殖和视网膜前膜,那么就必须考虑与玻璃体切除术恰当时机相关的争论。在能够识别并封闭视网膜裂孔的情况下,可以先进行巩膜扣带术,随后延迟进行玻璃体切除术。以我的经验来看,在大多数情况下,对于增殖性玻璃体视网膜病变,在进行玻璃体切除术和膜分割时需要联合修正巩膜扣带术。在有药物可抑制细胞增殖之前,或者在我们对这个过程的细胞生物学有了基本了解从而能够采用其他药物干预方法之前,对于最严重的病例,机械方法仍是必要的治疗手段。

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