光感受器祖细胞 mRNA 分析揭示 ABCA4 c.5461-10T→C 突变导致斯塔加特病中外显子跳跃。

Photoreceptor Progenitor mRNA Analysis Reveals Exon Skipping Resulting from the ABCA4 c.5461-10T→C Mutation in Stargardt Disease.

机构信息

Department of Human Genetics, Radboud University Medical Center, Nijmegen, The Netherlands; Radboud Institute of Molecular Life Sciences, Nijmegen, The Netherlands.

Department of Ophthalmology, Radboud University Medical Center, Nijmegen, The Netherlands.

出版信息

Ophthalmology. 2016 Jun;123(6):1375-85. doi: 10.1016/j.ophtha.2016.01.053. Epub 2016 Mar 12.

DOI:10.1016/j.ophtha.2016.01.053

PMID:26976702

Abstract

PURPOSE

To elucidate the functional effect of the ABCA4 variant c.5461-10T→C, one of the most frequent variants associated with Stargardt disease (STGD1).

DESIGN

Case series.

PARTICIPANTS

Seventeen persons with STGD1 carrying ABCA4 variants and 1 control participant.

METHODS

Haplotype analysis of 4 homozygotes and 11 heterozygotes for c.5461-10T→C and sequence analysis of the ABCA4 gene for a homozygous proband. Fibroblasts were reprogrammed from 3 persons with STGD1 into induced pluripotent stem cells, which were differentiated into photoreceptor progenitor cells (PPCs). The effect of the c.5461-10T→C variant on RNA splicing by reverse-transcription polymerase chain reaction was analyzed using PPC mRNA. In vitro assays were performed with minigene constructs containing ABCA4 exon 39. We analyzed the natural history and ophthalmologic characteristics of 4 persons homozygous for c.5461-10T→C.

MAIN OUTCOME MEASURES

Haplotype and rare variant data for ABCA4, RNA splice defects, age at diagnosis, visual acuity, fundus appearance, visual field, electroretinography (ERG) results, fluorescein angiography results, and fundus autofluorescence findings.

RESULTS

The frequent ABCA4 variant c.5461-10T→C has a subtle effect on splicing based on prediction programs. A founder haplotype containing c.5461-10T→C was found to span approximately 96 kb of ABCA4 and did not contain other rare sequence variants. Patient-derived PPCs showed skipping of exon 39 or exons 39 and 40 in the mRNA. HEK293T cell transduction with minigenes carrying exon 39 showed that the splice defects were the result of the c.5461-10T→C variant. All 4 subjects carrying the c.5461-10T→C variant in a homozygous state showed a young age of STGD1 onset, with low visual acuity at presentation and abnormal cone ERG results. All 4 demonstrated severe cone-rod dystrophy before 20 years of age and were legally blind by 25 years of age.

CONCLUSIONS

The ABCA4 variant c.5461-10T→C is located on a founder haplotype lacking other disease-causing rare sequence variants. In vitro studies revealed that it leads to mRNA exon skipping and ABCA4 protein truncation. Given the severe phenotype in persons homozygous for this variant, we conclude that this variant results in the absence of ABCA4 activity.

摘要

目的

阐明与斯塔加特病（STGD1）相关的最常见变异之一 ABCA4 变体 c.5461-10T→C 的功能影响。

设计

病例系列。

参与者

17 名携带 ABCA4 变异体的 STGD1 患者和 1 名对照参与者。

方法

对 4 名纯合子和 11 名杂合子的 c.5461-10T→C 进行单体型分析，并对纯合子先证者的 ABCA4 基因进行序列分析。从 3 名 STGD1 患者中重编程成纤维细胞为诱导多能干细胞，然后分化为光感受器祖细胞（PPC）。使用 PPC mRNA 通过逆转录聚合酶链反应分析 c.5461-10T→C 变体对 RNA 剪接的影响。使用包含 ABCA4 外显子 39 的小基因构建体进行体外测定。我们分析了 4 名纯合子 c.5461-10T→C 的自然病史和眼科特征。

主要观察指标

ABCA4 的单体型和稀有变异数据、RNA 剪接缺陷、诊断年龄、视力、眼底外观、视野、视网膜电图（ERG）结果、荧光素血管造影结果和眼底自发荧光发现。

结果

基于预测程序，常见的 ABCA4 变体 c.5461-10T→C 对剪接有细微影响。发现包含 c.5461-10T→C 的常见 ABCA4 单体型跨越大约 96 kb 的 ABCA4，并且不包含其他稀有序列变异。源自患者的 PPC 在 mRNA 中显示外显子 39 或外显子 39 和 40 的跳过。用携带外显子 39 的小基因转导 HEK293T 细胞表明，剪接缺陷是由 c.5461-10T→C 变体引起的。所有 4 名携带 c.5461-10T→C 变体的纯合子患者均表现出 STGD1 发病年龄较轻，发病时视力较低，视锥细胞 ERG 结果异常。所有 4 名患者在 20 岁之前均表现出严重的锥杆营养不良，并在 25 岁之前失明。