IWK Health Centre Eye Care Team, Halifax, Nova Scotia, Canada2Department of Ophthalmology and Visual Sciences, Dalhousie University, Halifax, Nova Scotia, Canada3Department of Pathology, Dalhousie University, Halifax, Nova Scotia, Canada.
Department of Pathology, Dalhousie University, Halifax, Nova Scotia, Canada.
JAMA Ophthalmol. 2014 Dec;132(12):1393-9. doi: 10.1001/jamaophthalmol.2014.2814.
Retinal detachment with avascularity of the peripheral retina, typically associated with familial exudative vitreoretinopathy (FEVR), can result from mutations in KIF11, a gene recently identified to cause microcephaly, lymphedema, and chorioretinal dysplasia (MLCRD) as well as chorioretinal dysplasia, microcephaly, and mental retardation (CDMMR). Ophthalmologists should be aware of the range of presentations for mutations in KIF11 because the phenotypic distinction between FEVR and MLCRD/CDMMR portends management implications in patients with these conditions.
To identify gene mutations in patients who present with a FEVR phenotype and explore the spectrum of ocular and systemic abnormalities caused by KIF11 mutations in a cohort of patients with FEVR or microcephaly in conjunction with chorioretinopathy or FEVR.
DESIGN, SETTING, AND PARTICIPANTS: Clinical data and DNA were collected from each participant between 1998 and 2013 from the clinical practices of ophthalmologists and clinical geneticists internationally. Twenty-eight FEVR probands with diagnoses made by the referring physician and without a known FEVR gene mutation, and 3 with microcephaly and chorioretinopathy, were included. At least 1 patient in each pedigree manifested 1 or more of the following: macular dragging, partial retinal detachment, falciform folds, or total retinal detachment.
Whole-exome sequencing was conducted on affected members in multiplex pedigrees, and Sanger sequencing of the 22 exons of the KIF11 gene was performed on singletons. Clinical data and history were collected and reviewed.
Identification of mutations in KIF11.
Four novel heterozygous KIF11 mutations and 1 previously published mutation were identified in probands with FEVR: p.A218Gfs*15, p.E470X, p.R221G, c.790-1G>T, and the previously described heterozygous p.R47X. Documentation of peripheral avascular areas on intravenous fluorescein angiography was possible in 2 probands with fibrovascular proliferation demonstrating phenotypic overlap with FEVR.
Mutations in KIF11 cause a broader spectrum of ocular disease than previously reported, including retinal detachment. The KIF11 gene likely plays a role in retinal vascular development and mutations in this gene can lead to clinical overlap with FEVR. Cases of FEVR should be carefully inspected for the presence of microcephaly as a marker for KIF11-related disease to enhance the accuracy of the prognosis and genetic counseling.
与家族渗出性玻璃体视网膜病变(FEVR)相关的视网膜脱离伴周边视网膜无血管,通常可归因于 KIF11 基因突变,该基因最近被发现可导致小头畸形、淋巴水肿和脉络膜视网膜发育不良(MLCRD)以及脉络膜视网膜发育不良、小头畸形和智力障碍(CDMMR)。眼科医生应该了解 KIF11 基因突变的各种表现,因为 FEVR 和 MLCRD/CDMMR 之间的表型差异预示着这些情况下患者的管理意义。
在 FEVR 表型的患者中鉴定基因突变,并在 FEVR 或小眼合并脉络膜视网膜病变或 FEVR 的患者队列中,探索 KIF11 突变引起的眼部和全身异常的范围。
设计、地点和参与者:临床数据和 DNA 于 1998 年至 2013 年从国际眼科医生和临床遗传学家的临床实践中收集。纳入 28 名 FEVR 先证者,其诊断由主治医生做出且无已知 FEVR 基因突变,其中 3 名伴有小眼和脉络膜视网膜病变。每个家系中至少有 1 名患者表现出以下 1 种或多种情况:黄斑牵拉、部分视网膜脱离、镰状褶皱或完全视网膜脱离。
对多态性家系中的受累成员进行全外显子组测序,并对单体进行 KIF11 基因的 22 个外显子的 Sanger 测序。收集和回顾临床数据和病史。
鉴定 KIF11 突变。
在 FEVR 先证者中鉴定出 4 种新的杂合 KIF11 突变和 1 种先前发表的突变:p.A218Gfs*15、p.E470X、p.R221G、c.790-1G>T 和先前描述的杂合 p.R47X。在 2 名表现出纤维血管增生的患者中可以对静脉内荧光素血管造影上的周边无血管区域进行记录,这些患者表现出与 FEVR 的表型重叠。
KIF11 突变导致比以前报道的更广泛的眼部疾病,包括视网膜脱离。KIF11 基因可能在视网膜血管发育中起作用,该基因的突变可导致与 FEVR 的临床重叠。FEVR 病例应仔细检查是否存在小头畸形作为与 KIF11 相关疾病的标志物,以提高预后和遗传咨询的准确性。
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