Monoallelic missense variants in MAB21L1 cause a novel autosomal dominant microphthalmia.

IF 1.2 4区 医学 Q4 GENETICS & HEREDITY Ophthalmic Genetics Pub Date : 2024-12-01 Epub Date: 2024-07-17 DOI:10.1080/13816810.2024.2378029
Jinli Li, Qin Wang, Aijun Yang, Junyu Zhang
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引用次数: 0

Abstract

Purpose: The biallelic variant of MAB21L1 has previously been documented in conjunction with the autosomal recessive cerebellar, ocular, craniofacial, and genital syndrome (COFG). The purpose of this study was to investigate the gene-disease association of MAB21L1 and the newly discovered autosomal dominant (AD) microphthalmia.

Methods: We report the presence of an exceptionally rare missense variant in a single allele of the Arg51 codon of MAB21L1 among four individuals from a single family diagnosed with microphthalmia, which suggesting an autosomal dominant inheritance pattern. Subsequently, based on comprehensive literature review, we identified another 13 families that have reported cases of autosomal dominant microphthalmos.

Results: Genotype-phenotype analysis revealed that patients with a single allele missense variant in MAB21L1 exhibited solely eye abnormalities. This starkly diverged from the clinical presentation of COFG, typified by the concurrent occurrence of ocular and extraocular symptoms stemming from the biallelic variant in MAB21L1. Our findings revealed that the heterozygous pathogenic variant in MAB21L1 resulted in the emergence of autosomal dominant microphthalmia. By combining these genetic and experimental evidence, the clinical validity of MAB21L1 and the emerging autosomal dominant microphthalmia can be regarded as moderate.

Conclusion: In summary, there is sufficient convincing evidence to prove that MAB21L1 is a novel pathogenic gene responsible for autosomal dominant microphthalmia, thus offering valuable insights for precise diagnosis and targeted therapeutic interventions in cases of microphthalmia.

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MAB21L1 的单倍错义变体会导致一种新型常染色体显性小眼症。
目的:MAB21L1的双倍拷贝变体曾被证实与常染色体隐性遗传的小脑、眼、颅面和生殖器综合征(COFG)有关。本研究的目的是调查 MAB21L1 与新发现的常染色体显性(AD)小眼球症的基因-疾病关联:方法:我们报告了在一个小眼球症家族的四名确诊患者中,MAB21L1 的 Arg51 密码子的单等位基因中存在异常罕见的错义变异,这表明该基因具有常染色体显性遗传模式。随后,我们在全面查阅文献的基础上,确定了另外 13 个报告过常染色体显性小眼症病例的家族:结果:基因型-表型分析表明,MAB21L1 单等位基因错义变异患者仅表现出眼部异常。这与 COFG 的临床表现截然不同,COFG 的典型表现是同时出现由 MAB21L1 双等位基因变异引起的眼部和眼外症状。我们的研究发现,MAB21L1 的杂合致病变体导致了常染色体显性小眼症的出现。综合这些遗传和实验证据,MAB21L1 和新出现的常染色体显性小眼球症的临床有效性可被视为中等:总之,有足够令人信服的证据证明MAB21L1是导致常染色体显性小眼症的新型致病基因,从而为小眼症病例的精确诊断和有针对性的治疗干预提供了有价值的见解。
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来源期刊
Ophthalmic Genetics
Ophthalmic Genetics 医学-眼科学
CiteScore
2.40
自引率
8.30%
发文量
126
审稿时长
>12 weeks
期刊介绍: Ophthalmic Genetics accepts original papers, review articles and short communications on the clinical and molecular genetic aspects of ocular diseases.
期刊最新文献
A novel frameshift variant in BCOR causes congenital nuclear cataract. Single-cell somatic copy number alteration profiling of vitreous humor seeds in retinoblastoma. Usher syndrome in the United Arab Emirates. Monoallelic missense variants in MAB21L1 cause a novel autosomal dominant microphthalmia. The landscape of clinical trials research in inherited ophthalmic disease.
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