Leber's Congenital Amaurosis: Current Concepts of Genotype-Phenotype Correlations

Leber's congenital amaurosis (LCA), one of the most severe inherited retinal dystrophies, is typically associated with extremely early onset of visual loss, nystagmus, and amaurotic pupils, and is responsible for 20% of childhood blindness. With advances in molecular diagnostic technology, the knowledge about the genetic background of LCA has expanded widely, while disease-causing variants have been identified in 38 genes. Different pathogenetic mechanisms have been found among these varieties of genetic mutations, all of which result in the dysfunction or absence of their encoded proteins participating in the visual cycle. Hence, the clinical phenotypes also exhibit extensive heterogenicity, including the course of visual impairment, involvement of the macular area, alteration in retinal structure, and residual function of the diseased photoreceptor. By reviewing the clinical course, fundoscopic images, optical coherent tomography examination, and electroretinogram, genotype-phenotype correlations could be established for common genetic mutations in LCA, which would benefit the timing of the diagnosis and thus promote early intervention. Gene therapy is promising in the management of LCA, while several clinical trials are ongoing and preliminary success has been announced, focusing on RPE65 and other common disease-causing genes. This review provides an update on the genetics, clinical examination findings, and genotype-phenotype correlations in the most well-established causative genetic mutations of LCA.

Automated summary

Leber's congenital amaurosis (LCA) is a severe genetic retinal disease responsible for 20% of childhood blindness, with its genetic background widely understood and disease-causing variants identified in 38 genes. Different pathogenetic mechanisms result in dysfunction or absence of encoded proteins in the visual cycle, leading to extensive heterogeneity in clinical phenotypes. Gene therapy shows promise in managing LCA, with ongoing clinical trials focusing on common disease-causing genes such as RPE65.