Ophthalmology Service, CUB Hopital Erasme, Brussels, Belgium.
Neuropediatric Service, University Hospital Lille, Lille, France.
Ophthalmic Genet. 2021 Jun;42(3):296-299. doi: 10.1080/13816810.2021.1897846. Epub 2021 Mar 10.
The complete form of congenital stationary night blindness (cCSNB) represents a non-progressive retinal disorder characterized by night vision problems and often congenital nystagmus, reduced vision, high myopia, strabismus and normal fundus appearance. Clinically this form of CSNB can be diagnosed by full-field electroretinogram. The mode of inheritance can be X-linked and autosomal recessive with mutations in genes coding for proteins mainly present at the dendritic tips of ON-bipolar cells. Mutations in NYX, GRM6, GPR179, LRIT3 and TRPM1 lead to this condition. The latter gene defect represents the major form underlying cCSNBC. It codes for the melastatin-related transient receptor 1 expressed in the inner nuclear layer of the retina, with the protein localized in ON-bipolar cells. To date, various homozygous or compound heterozygous mutations in TRPM1 have been reported. Small chromosomal rearrangements are frequent cause of mental retardation. In rare cases deletions can overlap with a mutation on the remaining chromosome and lead to a recessive disorder. Here, we describe a patient with mild neurological deficiencies and cCSNB caused by a microdeletion on 15q32 overlapping with a TRPM1 variant.
先天性静止性夜盲症(cCSNB)的完全形式代表了一种非进行性视网膜疾病,其特征是夜视问题,通常伴有先天性眼球震颤、视力下降、高度近视、斜视和正常眼底外观。临床上,这种 CSNB 形式可以通过全视野视网膜电图进行诊断。遗传方式可以是 X 连锁和常染色体隐性遗传,突变发生在主要存在于 ON-双极细胞树突末端的蛋白质编码基因中。NYX、GRM6、GPR179、LRIT3 和 TRPM1 的突变导致这种情况。后者的基因缺陷是 cCSNBC 的主要形式。它编码在视网膜内核层表达的黑色素瘤相关瞬时受体 1,该蛋白定位于 ON-双极细胞中。迄今为止,已经报道了 TRPM1 的各种纯合子或复合杂合子突变。小染色体重排是智力障碍的常见原因。在罕见情况下,缺失可能与剩余染色体上的突变重叠,导致隐性疾病。在这里,我们描述了一名患者,其轻度神经功能缺陷和 cCSNB 是由 15q32 上的微缺失引起的,该缺失与 TRPM1 变异重叠。
