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[增殖性视网膜疾病玻璃体及视网膜前膜中凝血因子 XIII 的检测]

[Detection of coagulation factor XIII in the vitreous body and periretinal membranes in proliferative retinal diseases].

作者信息

Bresgen M, Weller M, Heimann K, Wiedemann P

机构信息

Abteilung für Netzhaut- und Glaskörperchirurgie, Universitäts Augenklinik, Köln.

出版信息

Fortschr Ophthalmol. 1990;87(3):279-82.

PMID:2198204
Abstract

The human blood coagulation factor catalyses the cross-linking of fibrin monomers at the end of the coagulation cascade. Additional functions are the coupling of fibronectin and collagen to each other and fibrin. Therefore we tried to investigate the significance of factor XIII in the development of intraocular membranes. Using gel electrophoresis and western blotting, both subunits (A and B) of factor XIII could be detected in vitreous aspirates from patients with "idiopathic" proliferative vitreoretinopathy (PVR) (n = 5), traumatic PVR (n = 5), and proliferative diabetic retinopathy (n = 5). In contrast the vitreous of five human "normal" post mortem eyes did not contain the subunits of factor XIII. Furthermore, we observed immunofluorescence staining for both subunits of factor XIII in 20 surgically obtained periretinal membranes. In early cellular as opposed to late hypocellular membranes we observed stronger labeling for both subunits of factor XIII. With double label staining techniques, the fibroblastic cells recognized by vimentin staining did not contain factor XIII. About 50% of the macrophages stained positive for the A-subunit of factor XIII. We observed no labeling for the B-subunit in macrophages. Therefore, we hypothesize that factor XIII in proliferative vitreoretinal disorders (PVR, PDR) is derived from the exudation of plasma and platelets through disrupted blood-retinal barriers.

摘要

人凝血因子在凝血级联反应结束时催化纤维蛋白单体的交联。其他功能包括纤连蛋白与胶原蛋白之间以及它们与纤维蛋白的偶联。因此,我们试图研究因子 XIII 在眼内膜形成过程中的意义。通过凝胶电泳和蛋白质印迹法,在患有“特发性”增生性玻璃体视网膜病变(PVR)(n = 5)、外伤性 PVR(n = 5)和增生性糖尿病视网膜病变(n = 5)患者的玻璃体抽吸物中均检测到了因子 XIII 的两个亚基(A 和 B)。相比之下,五只人类“正常”死后眼睛的玻璃体中未含有因子 XIII 的亚基。此外,我们在 20 个手术获取的视网膜周膜中观察到了因子 XIII 两个亚基的免疫荧光染色。在早期细胞性而非晚期低细胞性膜中,我们观察到因子 XIII 两个亚基的标记更强。采用双重标记染色技术,波形蛋白染色识别出的成纤维细胞不含因子 XIII。约 50%的巨噬细胞因子 XIII 的 A 亚基染色呈阳性。我们未观察到巨噬细胞中 B 亚基的标记。因此,我们推测增生性玻璃体视网膜疾病(PVR、PDR)中的因子 XIII 源自血浆和血小板通过受损血视网膜屏障的渗出。

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