Inherited Variants in the COL11A, COL1A, COL5A1, COMP, GSTM1 Genes and the Risk of Carpal Tunnel Syndrome.

IF 0.4 4区 医学 Q4 SURGERY Handchirurgie Mikrochirurgie Plastische Chirurgie Pub Date : 2024-09-01 Epub Date: 2024-09-27 DOI:10.1055/a-2375-3737
Andrzej Zyluk, Tadeusz Debniak, Filip Flicinski, Helena Rudnicka
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Abstract

The pathogenesis of most cases of carpal tunnel syndrome is not clearly defined. There are some aspects of the disease that suggest a potential effect of genetic predispositions. Mutations (variants) within the genes encoding various subtypes of collagen synthesis, oligomerisation in the endoplasmic reticulum and inactivation of reactive oxygen species may be involved in the development of carpal tunnel syndrome. The objective of this study was to determine the role of DNA alterations within the COL11A, COL1A, COL5A1, COMP and GSTM1 genes in the pathogenesis of carpal tunnel syndrome based on a Polish population.

Study design: In the discovery phase, a total of 96 patients with familial aggregation of CTS were genotyped using a Next Generation Sequencing panel in order to find possible mutations within the studied genes. The potential pathogenicity of the detected variants was investigated using the predictions of several in-silico algorithms and the TaqMan technology. In the association phase of the study, a group of 345 CTS patients and 1035 healthy controls were genotyped.

Results: A total of 35 splice-site or exonic non-synonymous variants were detected by NGS. We did not identify any clearly pathogenic or likely pathogenic alternations. The 30 variants were identified as benign or likely benign. Five missense changes were predicted as VUS and selected for association study. The COL5A1 c.1595 C>T (p.Ala532Val) was detected in one out of 345 cases and three out of 1035 controls (P=1, OR=1); this indicates that the variant is a neutral alteration. Four remaining variants - c.2840 C>A, c.5395 G>A, c.1331 C>G, c.1590 C>A - were present in none out of the 345 CTS patients and none out of 1035 controls.

Conclusion: The main finding of this study was that there was no independent association between the variants of five examined genes and carpal tunnel syndrome. Four uncertain variants were identified that seem to be extremely rare in the Polish population.

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COL11A、COL1A、COL5A1、COMP、GSTM1 基因的遗传变异与腕管综合征的风险。
大多数腕管综合征病例的发病机制尚不明确。该病的某些方面表明可能受到遗传倾向的影响。编码胶原合成、内质网寡聚化和活性氧失活的各种亚型基因的突变(变体)可能与腕管综合征的发病有关。本研究的目的是以波兰人群为基础,确定 COL11A、COL1A、COL5A1、COMP 和 GSTM1 基因中的 DNA 改变在腕管综合征发病机制中的作用:研究设计:在发现阶段,使用新一代测序面板对 96 名家族聚集性 CTS 患者进行基因分型,以发现所研究基因中可能存在的突变。研究人员利用几种内部算法和 TaqMan 技术的预测结果,对检测到的变异基因的潜在致病性进行了研究。在研究的关联阶段,对 345 名 CTS 患者和 1035 名健康对照者进行了基因分型:结果:通过 NGS 共检测到 35 个剪接位点或外显子非同义变异。我们没有发现任何明显致病或可能致病的变异。30个变异被鉴定为良性或可能良性。五个错义变异被预测为 VUS,并被选中进行关联研究。COL5A1 c.1595 C>T(p.Ala532Val)在 345 例病例中检测到一个,在 1035 例对照中检测到三个(P=1,OR=1);这表明该变异为中性变异。其余四个变异--c.2840 C>A、c.5395 G>A、c.1331 C>G、c.1590 C>A--在 345 例 CTS 患者和 1035 例对照中均未出现:本研究的主要发现是,五个受检基因的变异与腕管综合征之间没有独立关联。研究发现了四种不确定的变异基因,它们在波兰人群中似乎极为罕见。
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来源期刊
CiteScore
1.00
自引率
16.70%
发文量
85
审稿时长
6-12 weeks
期刊介绍: In Originalarbeiten und Fallberichten finden Sie die neuesten Informationen über: Diagnostik Verfahrenswahl state of the art / neueste Techniken rekonstruktive Verfahren Behandlung infolge von Traumata oder OP Bewertung der Ergebnisse Klinische Forschung Interessante Darstellung der neuesten Erkenntnisse in Originalarbeiten und Fallberichten. Exzellent veranschaulicht durch ein klares Layout und reiche Bebilderung. Überzeugen Sie sich selbst! Organschaften Organ der Deutschsprachigen Arbeitsgemeinschaft für Handchirurgie, Deutschen Gesellschaft für Handchirurgie und Österreichischen Gesellschaft für Handchirurgie Organ der Deutschsprachigen Arbeitsgemeinschaft für Mikrochirurgie der peripheren Nerven und Gefäße Organ der Deutschen Gesellschaft der Plastischen, Rekonstruktiven und Ästhetischen Chirurgen
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