Astuti Galuh D N, Sun Vincent, Bauwens Miriam, Zobor Ditta, Leroy Bart P, Omar Amer, Jurklies Bernhard, Lopez Irma, Ren Huanan, Yazar Volkan, Hamel Christian, Kellner Ulrich, Wissinger Bernd, Kohl Susanne, De Baere Elfride, Collin Rob W J, Koenekoop Robert K
Department of Human Genetics, Radboud University Medical Centre Nijmegen, The Netherlands ; Radboud Institute for Molecular Life Sciences, Radboud University Medical Centre Nijmegen, The Netherlands ; Division of Human Genetics, Center for Biomedical Research, Faculty of Medicine, Diponegoro University Semarang, Indonesia.
McGill Ocular Genetics Laboratory, Departments of Paediatric Surgery, Human Genetics and Ophthalmology, Montreal Children's Hospital, McGill University Health Centre Montreal, Quebec, Canada.
Mol Genet Genomic Med. 2015 Jan;3(1):14-29. doi: 10.1002/mgg3.109. Epub 2014 Sep 15.
Bietti's crystalline dystrophy (BCD) is a rare, autosomal recessive retinal degenerative disease associated with mutations in CYP4V2. In this study, we describe the genetic and clinical findings in 19 unrelated BCD patients recruited from five international retinal dystrophy clinics. Patients underwent ophthalmic examinations and were screened for CYP4V2 mutations by Sanger sequencing and quantitative polymerase chain reaction (qPCR) copy number variation screening. Eight CYP4V2 mutations were found in 10/19 patients, including three patients in whom only monoallelic mutations were detected. Four novel mutations were identified: c.604G>A; p.(Glu202Lys), c.242C>G; p.(Thr81Arg), c.604+4A>G; p.(?), and c.1249dup; p.(Thr417Asnfs*2). In addition, we identified a heterozygous paternally inherited genomic deletion of at least 3.8 Mb, encompassing the complete CYP4V2 gene and several other genes, which is novel. Clinically, patients demonstrated phenotypic variability, predominantly showing choroidal sclerosis, attenuated vessels, and crystalline deposits of varying degrees of severity. To our knowledge, our study reports the first heterozygous CYP4V2 deletion and hence a novel mutational mechanism underlying BCD. Our results emphasize the importance of copy number screening in BCD. Finally, the identification of CYP4V2-negative patients with indistinguishable phenotypes from CYP4V2-positive patients might suggest the presence of mutations outside the coding regions of CYP4V2, or locus heterogeneity, which is unreported so far.
比耶蒂结晶性视网膜营养不良(BCD)是一种罕见的常染色体隐性视网膜退行性疾病,与CYP4V2基因突变有关。在本研究中,我们描述了从五个国际视网膜营养不良诊所招募的19例无亲缘关系的BCD患者的基因和临床研究结果。患者接受了眼科检查,并通过桑格测序和定量聚合酶链反应(qPCR)拷贝数变异筛查对CYP4V2突变进行了检测。在19例患者中的10例中发现了8种CYP4V2突变,其中3例仅检测到单等位基因突变。鉴定出4种新突变:c.604G>A;p.(Glu202Lys),c.242C>G;p.(Thr81Arg),c.604+4A>G;p.(?),以及c.1249dup;p.(Thr417Asnfs*2)。此外,我们还发现了一种杂合的父系遗传基因组缺失,至少为3.8 Mb,涵盖了整个CYP4V2基因和其他几个基因,这是前所未有的。临床上,患者表现出表型变异性,主要表现为脉络膜硬化、血管变细以及不同严重程度的结晶沉积物。据我们所知,我们的研究首次报道了杂合性CYP4V2缺失,因此也是BCD潜在的一种新突变机制。我们的结果强调了在BCD中进行拷贝数筛查的重要性。最后,鉴定出与CYP4V2阳性患者具有难以区分表型的CYP4V2阴性患者,这可能表明在CYP4V2编码区之外存在突变,或者存在基因座异质性,而这在目前尚未见报道。
