Institute of Ophthalmology, University College London, UK.
Am J Hum Genet. 2012 Feb 10;90(2):247-59. doi: 10.1016/j.ajhg.2011.12.019. Epub 2012 Jan 26.
X-linked megalocornea (MGC1) is an ocular anterior segment disorder characterized by an increased cornea diameter and deep anterior chamber evident at birth and later onset of mosaic corneal degeneration (shagreen), arcus juvenilis, and presenile cataracts. We identified copy-number variation, frameshift, missense, splice-site and nonsense mutations in the Chordin-like 1 gene (CHRDL1) on Xq23 as the cause of the condition in seven MGC1 families. CHRDL1 encodes ventroptin, a bone morphogenic protein antagonist with a proposed role in specification of topographic retinotectal projections. Electrophysiological evaluation revealed mild generalized cone system dysfunction and, in one patient, an interhemispheric asymmetry in visual evoked potentials. We show that CHRDL1 is expressed in the developing human cornea and anterior segment in addition to the retina. We explored the impact of loss of ventroptin function on brain function and morphology in vivo. CHRDL1 is differentially expressed in the human fetal brain, and there is high expression in cerebellum and neocortex. We show that MGC1 patients have a superior cognitive ability despite a striking focal loss of myelination of white matter. Our findings reveal an unexpected requirement for ventroptin during anterior segment development and the consequences of a lack of function in the retina and brain.
X 连锁型巨角膜症(MGC1)是一种眼部前节疾病,其特征为角膜直径增大,前房加深,出生时即明显,随后出现马赛克状角膜变性(鲨革样斑)、青少年性弓状斑和早发性白内障。我们在 Xq23 的 Chordin 样 1 基因(CHRDL1)中发现了拷贝数变异、移码、错义、剪接位点和无义突变,这是七个 MGC1 家系发病的原因。CHRDL1 编码 ventroptin,一种骨形态发生蛋白拮抗剂,其功能可能在于特异地确定视网膜-顶盖投射的拓扑结构。电生理评估显示轻度泛发性圆锥系统功能障碍,在一名患者中,视觉诱发电位存在半球间不对称性。我们表明,CHRDL1 在人角膜和前节的发育过程中表达,除了视网膜之外。我们还探索了 ventroptin 功能丧失对体内大脑功能和形态的影响。CHRDL1 在人胎儿大脑中差异表达,在小脑和新皮层中有高表达。我们表明,尽管存在明显的白质髓鞘缺失,但 MGC1 患者的认知能力仍然优越。我们的发现揭示了 ventroptin 在前段发育过程中的意外需求以及其在视网膜和大脑中功能丧失的后果。
