全面的遗传分析揭示了中国小眼症患者大样本中 MFRP 的突变谱及其基因型-表型相关性。
Comprehensive genetic analysis uncovers the mutational spectrum of MFRP and its genotype-phenotype correlation in a large cohort of Chinese microphthalmia patients.
机构信息
Beijing Tongren Eye Center, Beijing Tongren Hospital, Capital Medical University, Beijing Key Laboratory of Ophthalmology and Visual Sciences, Beijing 100730, China.
State Key Laboratory of Ophthalmology, Guangdong Provincial Key Laboratory of Ophthalmology and Visual Science, Zhongshan Ophthalmic Center, Sun Yat-sen University, Guangzhou, Guangdong 510000, China.
出版信息
Gene. 2024 Oct 30;926:148647. doi: 10.1016/j.gene.2024.148647. Epub 2024 Jun 5.
PURPOSE
Microphthalmia is a severe congenital ocular disease featured by abnormal ocular development. The aim of this study was to detail the genetic and clinical characteristics of a large cohort of Chinese patients with microphthalmia related to MFRP variants, focusing on uncovering genotype-phenotype correlations.
METHODS
Fifty microphthalmia patients from 44 unrelated Chinese families were recruited. Whole-exome sequencing (WES) was conducted to analyze the coding regions and adjacent intronic regions of MFRP. Axial lengths (AL) were measured for all probands and available family members. Protein structures of mutations with high frequency in our cohort were predicted. The genotype-phenotype correlations were explored by statistical analysis.
RESULTS
Sixteen MFRP variants were detected in 17 families, accounting for 38.64 % of all microphthalmia families. There were 9 novel mutations (c.427+1G>C, c.428-2A>C, c.561_575del:p.A188_E192del, c.836G>A:p.C279Y, c.1010_1021del:p.H337_E340del:p.Y479*, c.1516_1517del:p.S506Pfs*66, c.1561T>G:p.C521G, c.1616G>A:p.R539H, and c.1735C>T:p.P579S) and six previously reported variants in MFRP, with p.E496K and p.H337_E340del being highly frequent, found in eight (47.06 %) and two families (11.76 %), respectively. Seven variants (43.75 %) were located in the C-terminal cysteine-rich frizzled-related domain (CRD) (7/16, 43.75 %). Protein prediction implicated p.E496K and p.H337_E340del mutations might lead to a destabilization of the MFRP protein. The average AL of all 42 eyes was 16.02 ± 1.05 mm, and 78.36 % of eyes with AL < 16 mm harbored p.E496K variant. Twenty-six eyes with variant variant had shorter AL than that of the other 16 eyes without this variant (p = 0.006), highlighting a novel genotype-phenotype correlation.
CONCLUSIONS
In this largest cohort of Chinese patients with microphthalmia, the 9 novel variants, high frequency of p.E496W, and mutation hotspots in CRD reveals unique insights into the MFRP mutation spectrum among Chinese patients, indicating ethnic variability. A new genotype-phenotype correlation that p.E496K variant associated with a shorter AL is unveiled. Our findings enhance the current knowledge of MFRP-associated microphthalmia and provide valuable information for prenatal diagnosis as well as future therapy.
目的
小眼症是一种严重的先天性眼部疾病,其特征为眼部发育异常。本研究旨在详细描述与 MFRP 变异相关的中国小眼症患者的遗传和临床特征,重点揭示基因型-表型相关性。
方法
招募了来自 44 个无关中国家庭的 50 名小眼症患者。进行全外显子组测序(WES)以分析 MFRP 的编码区域和相邻的内含子区域。对所有先证者和可获得的家族成员进行眼轴长度(AL)测量。预测我们队列中高频突变的蛋白质结构。通过统计分析探讨基因型-表型相关性。
结果
在 17 个家庭中检测到 16 个 MFRP 变异,占所有小眼症家庭的 38.64%。有 9 个新突变(c.427+1G>C、c.428-2A>C、c.561_575del:p.A188_E192del、c.836G>A:p.C279Y、c.1010_1021del:p.H337_E340del:p.Y479*、c.1516_1517del:p.S506Pfs*66、c.1561T>G:p.C521G、c.1616G>A:p.R539H 和 c.1735C>T:p.P579S)和 MFRP 中的 6 个先前报道的变异,p.E496K 和 p.H337_E340del 高度频繁,分别在 8 个(47.06%)和 2 个家庭(11.76%)中发现。7 个变异(43.75%)位于 C 末端富含半胱氨酸的卷曲螺旋受体(CRD)中(7/16,43.75%)。蛋白质预测提示 p.E496K 和 p.H337_E340del 突变可能导致 MFRP 蛋白不稳定。所有 42 只眼中的平均 AL 为 16.02±1.05mm,78.36%的 AL<16mm 的眼中存在 p.E496K 变异。26 只携带变异的眼中的 AL 短于其他 16 只不携带这种变异的眼中的 AL(p=0.006),突出了一种新的基因型-表型相关性。
结论
在这个最大的中国小眼症患者队列中,9 个新突变、p.E496K 的高频出现以及 CRD 中的突变热点揭示了中国患者中 MFRP 突变谱的独特见解,表明存在种族差异。揭示了与较短的 AL 相关的新的基因型-表型相关性 p.E496K 变异。我们的发现增强了对 MFRP 相关小眼症的现有认识,并为产前诊断以及未来的治疗提供了有价值的信息。
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