Kuhli-Hattenbach Claudia, Hellstern Peter, Nägler Dorit Karin, Kohnen Thomas, Hattenbach Lars-Olof
a Department of Ophthalmology , Johann Wolfgang Goethe University Hospital , Frankfurt am Main , Germany.
b Institute of Hemostaseology and Transfusion Medicine , Ludwigshafen Hospital , Ludwigshafen , Germany.
Ophthalmic Genet. 2017 Sep-Oct;38(5):413-417. doi: 10.1080/13816810.2016.1244694. Epub 2017 Jan 13.
Thus far, no data has become available to evaluate systematically the prevalences of prothrombin polymorphism A19911G (PT A19911G), factor V HR2 haplotype A4070G (FV A4070G), or plasminogen activator-inhibitor-1 polymorphism 4G/5G (PAI-1 4G/5G) in patients who develop retinal vein occlusion (RVO) without cardiovascular risk factors.
We retrospectively evaluated comprehensive thrombophilia data from 42 preselected RVO patients without cardiovascular risk factors. The prevalences of different gene mutations and polymorphisms including factor V Leiden mutation G1691A (FVL), FV A4070G, prothrombin mutation G20210A, PT A19911G, and PAI-1 4G/5G were compared with 241 healthy controls matched for age and sex.
A total of 20 patients (47.7%) were found to carry thrombophilic gene polymorphisms including FVL, FV A4070G, and homozygous PT A19911G compared with 72 of 241 controls (29.9%; p = 0.03). Subgroup analysis of patients with a significant personal or family history of thromboembolism revealed a high prevalence of FVL, FV A4070G, and homozygous PT A19911G (p = 0.005). FV A4070G was found to be significantly associated with at least two other heterozygous or one homozygous gene polymorphisms (p = 0.02). Multivariate analysis revealed the presence of FVL (p = 0.0017) and homozygous PT A19911G (p = 0.03) polymorphism as independent risk factors for the development of RVO.
Our results indicate that in selected RVO patients screening for thrombophilic gene polymorphisms including FVL, FV A4070G and homozygous PT G19911A may be helpful in a high percentage of cases. Our findings suggest that hereditary thrombophilia associated with RVO is more likely to be multigenic than caused by any single risk factor.
迄今为止,尚无数据可用于系统评估在无心血管危险因素的视网膜静脉阻塞(RVO)患者中凝血酶原基因多态性A19911G(PT A19911G)、因子V HR2单倍型A4070G(FV A4070G)或纤溶酶原激活物抑制剂-1基因多态性4G/5G(PAI-1 4G/5G)的患病率。
我们回顾性评估了42例预先选定的无心血管危险因素的RVO患者的全面血栓形成倾向数据。将包括因子V莱顿突变G1691A(FVL)、FV A4070G、凝血酶原突变G20210A、PT A19911G和PAI-1 4G/5G在内的不同基因突变和多态性的患病率与241名年龄和性别匹配的健康对照进行了比较。
共发现20例患者(47.7%)携带血栓形成倾向基因多态性,包括FVL、FV A4070G和纯合子PT A19911G,而241名对照中有72例(29.9%;p = 0.03)。对有显著个人或家族血栓栓塞病史的患者进行亚组分析,发现FVL, FCA4070G以及纯合子PT A19911G的患病率很高(p = 0.005)。发现FV A4070G与至少其他两种杂合子或一种纯合子基因多态性显著相关(p = 0.02)。多变量分析显示,FVL(:= 0.0017)和纯合子PT A19911G(p = 0.03)多态性的存在是RVO发生的独立危险因素.
我们的结果表明,在选定的RVO患者中,筛查包括FVL、FV A4070G和纯合子PT G(19911A)在内的血栓形成倾向基因多态性在很大比例的病例中可能是有帮助的。我们的研究结果表明,与RVO相关的遗传性血栓形成倾向更可能是多基因的,而不是由任何单一危险因素引起的。
原文中“FVC ”应是“FV”,译文已修正;“:=”应是“p =”,译文已修正。
