Sansović Ivona, Meašić Ana-Maria, Bobinec Adriana, Morožin Pohovski Leona, Odak Ljubica, Vulin Katarina, Lozić Bernarda, Kero Mijana, Huljev Frković Sanda, Pušeljić Silvija
Ivona Sansović, Children's Hospital Zagreb, University of Zagreb, School of Medicine, Department of Medical and Laboratory Genetics, Endocrinology and Diabetology, Klaićeva 16, 10000 Zagreb, Croatia,
Croat Med J. 2024 Jun 13;65(3):198-208. doi: 10.3325/cmj.2024.65.198.
To determine the spectrum and frequency of disease-causing variants in patients with non-syndromic hearing loss (NSHL) and to investigate the diagnostic yield of the applied genetic methods.
The study enrolled 306 unrelated patients with childhood-onset, mild-to-profound NSHL referred to Children's Hospital Zagreb for genetic testing between March 2006 and October 2023. The GJB2 variants were analyzed with the multiplex ligation-dependent probe amplification method and Sanger sequencing of the coding region of the GJB2 gene. In 21 patients negative for GJB2 biallelic variants, clinical exome sequencing (CES) was performed.
Among 234 disease-associated GJB2 alleles detected, 19 were clinically relevant, of which 18 were reported as pathogenic/likely pathogenic. The c.35delG variant accounted for 73.5% of the mutated alleles. More than half of the patients with biallelic GJB2 variants (64/110, 58.2%) were 35delG homozygotes. Seventeen non-GJB2 variants were found in 10 genes (TECTA, NOG, SLC26A4, PCDH15, TMPRSS3, USH2A, GATA3, MYO15A, SOX10, COL2A1) in 11 participants, and 5 variants (in TECTA, NOG, PCDH15, and SOX10) were novel (29.4%).
We were able to elucidate the genetic cause of hearing loss in 121 patients, with an overall diagnostic rate of 39.5%. The c.35delG was the most common variant. CES allowed us to diagnose almost half of the patients with HL; to distinguish NSHL from the syndromic form of HL in cases where the phenotype was unclear or where symptoms were absent from an early age; and to discover novel variants.
确定非综合征性听力损失(NSHL)患者致病变异的谱型和频率,并研究应用的基因检测方法的诊断效率。
该研究纳入了2006年3月至2023年10月期间转诊至萨格勒布儿童医院进行基因检测的306例非亲缘关系的儿童期起病、轻至重度NSHL患者。采用多重连接依赖探针扩增法和GJB2基因编码区的桑格测序法分析GJB2变异。对21例GJB2双等位基因变异阴性的患者进行了临床外显子组测序(CES)。
在检测到的234个与疾病相关的GJB2等位基因中,19个具有临床相关性,其中18个被报告为致病/可能致病。c.35delG变异占突变等位基因的73.5%。双等位基因GJB2变异患者中超过一半(64/110,58.2%)为35delG纯合子。在11名参与者的10个基因(TECTA、NOG、SLC26A4、PCDH15、TMPRSS3、USH2A、GATA3、MYO15A、SOX10、COL2A1)中发现了17个非GJB2变异,其中5个变异(TECTA、NOG、PCDH15和SOX10中的变异)是新发现的(29.4%)。
我们能够阐明121例患者听力损失的遗传原因,总体诊断率为39.5%。c.35delG是最常见的变异。CES使我们能够诊断近一半的HL患者;在表型不明确或早年无症状的情况下,将NSHL与综合征型HL区分开来;并发现新的变异。
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