SLC26A2/DTDST Spectrum: A Cohort of 12 Patients Associated with a Comprehensive Review of the Genotype-Phenotype Correlation.

IF 0.9 4区医学 Q4 GENETICS & HEREDITY Molecular Syndromology Pub Date : 2023-01-01 DOI:10.1159/000525020

Cynthia Silveira, Karina da Costa Silveira, Maria D Lacarrubba-Flores, Maurício T Sakata, Silvia N Carbognani, Juan Llerena, Carolina A Moreno, Denise P Cavalcanti

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引用次数: 1

Abstract

Introduction: Pathogenic variants in the SLC26A2/DTDST gene cause the following spectrum of phenotypes: achondrogenesis 1B (ACG1B), atelosteogenesis 2 (AO2), diastrophic dysplasia (DTD), and recessive-multiple epiphyseal dysplasia (rMED), the first 2 being lethal. Here, we report a cohort and a comprehensive literature review on a genotype-phenotype correlation of SLC26A2/DTDST-related disorders.

Methods: The local patients were genotyped by Sanger sequencing or next-generation sequencing (NGS). We reviewed data from the literature regarding phenotype, zygosity, and genotype in parallel.

Results: The local cohort enrolled 12 patients, including one with a Desbuquois-like phenotype. All but one showed biallelic mutations, however, only one allele mutated in a fetus presenting ACG1B was identified. The literature review identified 42 articles and the analyses of genotype and zygosity included the 12 local patients.

Discussion: The R279W variant was the most prevalent among the local patients. It was in homozygosity (hmz) in 2 patients with rMED and in compound heterozygosity (chtz) in 9 patients. The genotype and zygosity review of all patients led to the following conclusions: DTD is the most common phenotype in Finland due to a Finnish mutation (c.727-1G>C). Outside of Finland, rMED is the most prevalent phenotype, usually associated with R279W in hmz. In contrast, DTD's genotype is usually in chtz. Despite a large number of variants (38), just 8 are recurrent (R279W, C653S, c.-26+2T>C, R178*, K575Sfs*10, V340del, G663R, T512K). The last 3 in hmz lead to lethal phenotypes. The Finnish mutation is found only in chtz outside of Finland, being associated with all 4 classical phenotypes. The p.R178* and p.K575Sfs*10 variants should be viewed as lethal mutations since both were mainly described with lethal phenotypes and were never reported in hmz. The existence of 9 patients with only one mutated allele suggests that other mutations in the other allele of these patients still need to be unveiled.

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SLC26A2/DTDST谱:一项与基因型-表型相关性相关的12例患者队列研究

SLC26A2/DTDST基因的致病变异可导致以下表型谱:软骨发育不全1B (ACG1B)、骨不全2 (AO2)、异位性发育不良(DTD)和隐性多发性骨骺发育不良(rMED)，其中前2种是致命的。在这里，我们报告了SLC26A2/ dtdst相关疾病的基因型-表型相关性的队列和全面的文献综述。方法:采用Sanger测序或下一代测序(NGS)对局部患者进行基因分型。我们回顾了文献中关于表型、合子性和基因型的数据。结果:当地队列纳入了12例患者，其中1例具有desbuquois样表型。除一例外，其余均显示双等位基因突变，然而，在出现ACG1B的胎儿中只发现了一个等位基因突变。文献复习42篇，对12例本地患者进行基因型和合子分析。讨论:R279W变异在当地患者中最为普遍。2例为纯合性(hmz)， 9例为复合杂合性(chtz)。所有患者的基因型和合子性回顾得出以下结论:由于芬兰突变(C .727- 1g >C)， DTD是芬兰最常见的表型。在芬兰以外，rMED是最普遍的表型，通常与hmz的R279W相关。相反，DTD的基因型通常为chtz。尽管有大量的变体(38个)，只有8个是反复出现的(R279W、C653S、C -26+2T>C、R178*、K575Sfs*10、V340del、G663R、T512K)。最后3兆赫兹导致致命表型。芬兰突变仅在芬兰以外的chtz中发现，与所有4种经典表型相关。p.R178*和p.K575Sfs*10变异应被视为致死突变，因为这两种变异主要描述为致死表型，而在hmz中从未报道过。只有一个等位基因突变的9例患者的存在表明，这些患者的其他等位基因的其他突变仍然需要揭示。

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来源期刊

Molecular Syndromology Biochemistry, Genetics and Molecular Biology-Genetics

CiteScore

1.70

自引率

9.10%

发文量

期刊介绍： ''Molecular Syndromology'' publishes high-quality research articles, short reports and reviews on common and rare genetic syndromes, aiming to increase clinical understanding through molecular insights. Topics of particular interest are the molecular basis of genetic syndromes, genotype-phenotype correlation, natural history, strategies in disease management and novel therapeutic approaches based on molecular findings. Research on model systems is also welcome, especially when it is obviously relevant to human genetics. With high-quality reviews on current topics the journal aims to facilitate translation of research findings to a clinical setting while also stimulating further research on clinically relevant questions. The journal targets not only medical geneticists and basic biomedical researchers, but also clinicians dealing with genetic syndromes. With four Associate Editors from three continents and a broad international Editorial Board the journal welcomes submissions covering the latest research from around the world.