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全外显子组测序和功能分析鉴定一个与中国人先天性白内障相关的新型 MIP 移码突变。

Identification of a novel MIP frameshift mutation associated with congenital cataract in a Chinese family by whole-exome sequencing and functional analysis.

机构信息

Center for Medical Genetics, School of Life Sciences, Central South University, 110 Xiangya Road, Changsha, 410078, Hunan, PR China.

Hunan Jiahui Genetics Hospital, 110 Xiangya Road, Changsha, 410078, Hunan, PR China.

出版信息

Eye (Lond). 2018 Aug;32(8):1359-1364. doi: 10.1038/s41433-018-0084-5. Epub 2018 Apr 26.

DOI:10.1038/s41433-018-0084-5
PMID:29695758
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6085365/
Abstract

PURPOSE

To detect the underlying pathogenesis of congenital cataract in a four-generation Chinese family.

METHODS

Whole-exome sequencing (WES) of family members (III:4, IV:4, and IV:6) was performed. Sanger sequencing and bioinformatics analysis were subsequently conducted. Full-length WT-MIP or K228fs-MIP fused to HA markers at the N-terminal was transfected into HeLa cells. Next, quantitative real-time PCR, western blotting and immunofluorescence confocal laser scanning were performed.

RESULTS

The age of onset for nonsyndromic cataracts in male patients was by 1-year old, earlier than for female patients, who exhibited onset at adulthood. A novel c.682_683delAA (p.K228fs230X) mutation in main intrinsic protein (MIP) cosegregated with the cataract phenotype. The instability index and unfolded states for truncated MIP were predicted to increase by bioinformatics analysis. The mRNA transcription level of K228fs-MIP was reduced compared with that of WT-MIP, and K228fs-MIP protein expression was also lower than that of WT-MIP. Immunofluorescence images showed that WT-MIP principally localized to the plasma membrane, whereas the mutant protein was trapped in the cytoplasm.

CONCLUSIONS

Our study generated genetic and primary functional evidence for a novel c.682_683delAA mutation in MIP that expands the variant spectrum of MIP and help us better understand the molecular basis of cataract.

摘要

目的

检测一个四代中国家族先天性白内障的潜在发病机制。

方法

对家庭成员(III:4、IV:4 和 IV:6)进行全外显子组测序(WES)。随后进行 Sanger 测序和生物信息学分析。将全长 WT-MIP 或 K228fs-MIP 与 HA 标记融合到 N 端转染到 HeLa 细胞中。接下来进行定量实时 PCR、western blot 和免疫荧光共聚焦激光扫描。

结果

男性非综合征性白内障患者的发病年龄为 1 岁,早于成年发病的女性患者。主要内在蛋白(MIP)中的一个新的 c.682_683delAA(p.K228fs230X)突变与白内障表型共分离。生物信息学分析预测截短 MIP 的不稳定性指数和未折叠状态增加。与 WT-MIP 相比,K228fs-MIP 的 mRNA 转录水平降低,并且 K228fs-MIP 蛋白表达也低于 WT-MIP。免疫荧光图像显示 WT-MIP 主要定位于质膜,而突变蛋白则滞留在细胞质中。

结论

本研究为 MIP 中的一个新的 c.682_683delAA 突变提供了遗传和初步功能证据,扩展了 MIP 的变异谱,并帮助我们更好地理解白内障的分子基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7dc9/6085365/ee767c9dd3f5/41433_2018_84_Fig2_HTML.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7dc9/6085365/68465d0edbb3/41433_2018_84_Fig1_HTML.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7dc9/6085365/ee767c9dd3f5/41433_2018_84_Fig2_HTML.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7dc9/6085365/68465d0edbb3/41433_2018_84_Fig1_HTML.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7dc9/6085365/ee767c9dd3f5/41433_2018_84_Fig2_HTML.jpg

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2
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Sporadic and Familial Congenital Cataracts: Mutational Spectrum and New Diagnoses Using Next-Generation Sequencing.
阳性预测值从 22 万份临床基因组记录分析中突出了四个新的可进行基因筛查的候选基因。
Genet Med. 2021 Dec;23(12):2300-2308. doi: 10.1038/s41436-021-01293-9. Epub 2021 Aug 13.
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A novel missense mutation in the gene encoding major intrinsic protein (MIP) in a Giant panda with unilateral cataract formation.大熊猫单侧白内障形成相关基因编码主要内在蛋白的新型错义突变。
BMC Genomics. 2021 Feb 2;22(1):100. doi: 10.1186/s12864-021-07386-8.
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Genetic modifiers of rodent animal models: the role in cataractogenesis.鼠类动物模型的遗传修饰物:在白内障发生中的作用。
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