综合分析图尔基耶东部地区生物素酶缺乏症患者的基因型和表型特征。

Kısmet Çıkı, Ceren Alavanda, Emine İpek Ceylan, Tijen Tanyalçın, Sebile Kılavuz
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引用次数: 0

摘要

背景:生物素是一种水溶性维生素,在羧化过程中起着关键作用。生物素缺乏症(BD)患者体内游离生物素的形成受阻,导致生物素依赖性羧化酶功能受损。根据残留血清酶活性的百分比,BD 可分为部分和深度两类:方法:在土耳其东部地区的一个中心对确诊为生物素酶缺乏症的患者进行回顾性数据评估,包括性别、年龄、父母血缘关系、家族史、生物素酶活性分析、缺乏症类型(部分-深度)、体格检查、治疗和基因型。生物素酶活性低于 30% 且 BTD 基因存在双倍变异的患者被诊断为生物素酶缺乏症:研究共纳入 302 名患者。其中 135 人(44.7%)的父母为近亲。其中 286 例(94.7%)通过新生儿筛查确诊,14 例(4.6%)通过家族筛查确诊,2 例(0.06%)通过临床症状确诊。有 92 名(30.5%)患者在随访中被诊断为严重缺乏症,210 名(69.5%)患者被诊断为部分缺乏症。共检测到 306 个变异体。其中检测到 20 个不同的变体(3 个新变体 - 3 个罕见变体)和 31 个不同的基因型。最常检测到的 3 个变异是 c.410G>A(p.Arg137His;47.3%)、c.1270G>C(p.Asp424His;29.7%)和 c.38_44delGCGGCTGinsTCC(p.Cys13Phefs*36;15.3%)。最常见的三种基因型是 c.410G>A (p.Arg137His) / c.1270G>C (p.Asp424His) 复合杂合型(32.4%)、c.410G>A(p.Arg137His)同基因杂合子(24.8%),以及 c.38_44delGCGGCTGinsTCC (p.Cys13Phefs*36) / c.1270G>C (p.Asp424His) 复合杂合子(12.2%)。据统计,c.410G>A(p.Arg137His)同源变异、c.38_44delGCGGCTGinsTCC(p.Cys13Phefs*36)同源变异和c.38_44delGCGGCTGinsTCC(p.Cys13Phefs*36)/c.410G>A(p.Arg137His)复合杂合变异患者与深度缺乏症有显著相关性。c.410G>A(p.Arg137His)/c.1270G>C(p.Asp424His)变异的复合杂合子与部分缺乏症明显相关:结论:BTD 基因型与生化表型之间的关联并不总是一致的。我们的研究提供了有价值的数据,在文献中增加了基因型与表型相关的变异,并增加了三个新的变异,这些变异可为临床随访提供重要指导。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Comprehensive analysis of genotypic and phenotypic characteristics of biotinidase deficiency patients in the eastern region of Türkiye.

Background: Biotin is a water-soluble vitamin that plays a key role in carboxylation. The formation of free biotin is impaired in biotinidase deficiency (BD), resulting in impaired biotin-dependent carboxylase functions. Based on the percentage of residual serum enzyme activity, BD is classified as partial and profound.

Methods: Retrospective data including gender, age, parental consanguinity, family history, biotinidase activity analyses, type of deficiency (partial-profound), physical examination, treatment, and genotypes were evaluated in patients diagnosed with biotinidase deficiency in a single center in the eastern region of Türkiye. Patients whose biotinidase enzyme activity was below 30% with biallelic variants in the BTD gene were diagnosed as BD.

Results: A total of 302 patients were included in the study. Parental consanguinity was present in 135 (44.7%) of them. Two hundred eighty-six (94.7%) were diagnosed by neonatal screening, 14 (4.6%) by family screening and two (0.06%) by clinical symptoms. Ninety-two (30.5%) of the patients were followed-up with profound deficiency and 210 (69.5%) with partial deficiency. A total of 306 variants were detected. Twenty different variants (3 novel - 3 rare) and 31 different genotypes were detected. The 3 most frequently detected variants were c.410G>A (p.Arg137His; 47.3%), c.1270G>C (p.Asp424His; 29.7%), and c.38_44delGCGGCTGinsTCC (p.Cys13Phefs*36; 15.3%). The 3 most frequently identified genotypes were c.410G>A (p.Arg137His) / c.1270G>C (p.Asp424His) compound heterozygous (32.4%), c.410G>A (p.Arg137His) homozygous (24.8%), and c.38_44delGCGGCTGinsTCC (p.Cys13Phefs*36) / c.1270G>C (p.Asp424His) compound heterozygous (12.2%). Patients with c.410G>A (p.Arg137His) homozygous variant, c.38_44delGCGGCTGinsTCC (p.Cys13Phefs*36) homozygous variant and c.38_44delGCGGCTGinsTCC (p.Cys13Phefs*36) / c.410G>A (p.Arg137His) compound heterozygous variant were statistically significantly associated with profound deficiency. Compound heterozygosity of c.410G>A (p.Arg137His) / c.1270G>C (p.Asp424His) variants were significantly associated with partial deficiency.

Conclusions: The association between the BTD genotype and biochemical phenotype is not always consistent. Our study provides valuable data by adding variants with genotype-phenotype correlations to the literature and three novel variants, which can provide significant guidance in clinical follow-up.

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