Institute for Neurosciences of Montpellier U1051, University of Montpellier-University Hospital, Genetics of Sensory Diseases, Montpellier, France.
Center for structural biochemistry Montpellier, INSERM U1054-CNRS UMR5048, Montpellier, France.
Sci Rep. 2016 Sep 7;6:32544. doi: 10.1038/srep32544.
To revisit the autosomal dominant Sorsby fundus dystrophy (SFD) as a syndromic condition including late-onset pulmonary disease. We report clinical and imaging data of ten affected individuals from 2 unrelated families with SFD and carrying heterozygous TIMP3 mutations (c.572A > G, p.Y191C, exon 5, in family 1 and c.113C > G, p.S38C, exon 1, in family 2). In family 1, all SFD patients older than 50 (two generations) had also a severe emphysema, despite no history of smoking or asthma. In the preceding generation, the mother died of pulmonary emphysema and she was blind after the age of 50. Her two great-grandsons (<20 years), had abnormal Bruch Membrane thickness, a sign of eye disease. In family 2, eye and lung diseases were also associated in two generations, both occurred later, and lung disease was moderate (bronchiectasis). This is the first report of a syndromic SFD in line with the mouse model uncovering the role of TIMP3 in human lung morphogenesis and functions. The TIMP3 gene should be screened in familial pulmonary diseases with bronchiectasis, associated with a medical history of visual loss. In addition, SFD patients should be advised to avoid tobacco consumption, to practice sports, and to undergo regular pulmonary examinations.
重新审视常染色体显性 Sorsby 眼底营养不良 (SFD),将其视为一种包括迟发性肺部疾病的综合征。我们报告了来自 2 个无关联家族的 10 名受影响个体的临床和影像学数据,这些个体携带有 TIMP3 突变的杂合子 (c.572A>G,p.Y191C,外显子 5,家族 1 和 c.113C>G,p.S38C,外显子 1,家族 2)。在家族 1 中,所有年龄大于 50 岁(两代人)的 SFD 患者都患有严重的肺气肿,尽管没有吸烟或哮喘病史。在前一代中,母亲死于肺气肿,并且在 50 岁以后失明。她的两个曾孙(<20 岁)的布鲁赫膜厚度异常,这是眼部疾病的一个标志。在家族 2 中,眼部和肺部疾病也在两代人之间相关,且发生较晚,肺部疾病为中度(支气管扩张症)。这是首次报道与小鼠模型一致的综合征性 SFD,揭示了 TIMP3 在人类肺部形态发生和功能中的作用。在伴有关联的支气管扩张症的家族性肺部疾病中,应筛选 TIMP3 基因,这些疾病伴有视力丧失的病史。此外,应建议 SFD 患者避免吸烟,进行体育锻炼,并定期进行肺部检查。
