在酵母中研究与线粒体疾病相关的线粒体氨基酰-tRNA合成酶 WARS2、NARS2 和 RARS2 基因的新型变体。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-09-03 DOI:10.1093/hmg/ddae104
Sonia Figuccia, Rossella Izzo, Andrea Legati, Alessia Nasca, Paola Goffrini, Daniele Ghezzi, Camilla Ceccatelli Berti
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引用次数: 0

摘要

氨基酰转移核糖核酸合成酶(ARSs)是一种重要的酶,可催化每种氨基酸与其同源 tRNA 的连接。确保线粒体内蛋白质合成的线粒体 ARSs(mtARSs)由核基因编码,在细胞质中翻译后输入细胞器。随着新一代测序技术(NGS)的广泛应用,越来越多的 mtARS 基因变异被发现并与线粒体疾病相关。酵母和人类线粒体翻译机制的相似性使酵母成为快速有效评估 mtARS 基因变异影响的良好模型。通过对已知疾病基因(包括所有编码 mtARS 的基因)的定制基因面板对临床怀疑患有线粒体疾病的患者进行基因筛查,发现了 WARS2、NARS2 和 RARS2 中的错义变体。其中大部分变异被归类为意义不明的变异。我们利用酵母模型来评估在这些分别编码线粒体色氨酰-tRNA、天冬酰胺酰-tRNA 和精氨酰-tRNA 合成酶的基因中发现的变体的功能性后果。研究人员分析了缺失 MSW1、SLM5 和 MSR1(分别是 WARS2、NARS2 和 RARS2 的酵母直向同源物)、表达野生型或突变等位基因的酵母菌株的线粒体表型,如氧化生长、耗氧量、Cox2 稳态水平和线粒体蛋白质合成。大多数变体的致病性得到证实,因此被重新归类为 "可能致病"。此外,在生长培养基中补充天冬酰胺和精氨酸后观察到的有益效果表明,它们是一种潜在的治疗方法。
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Investigation in yeast of novel variants in mitochondrial aminoacyl-tRNA synthetases WARS2, NARS2, and RARS2 genes associated with mitochondrial diseases.

Aminoacyl-transfer RiboNucleic Acid synthetases (ARSs) are essential enzymes that catalyze the attachment of each amino acid to their cognate tRNAs. Mitochondrial ARSs (mtARSs), which ensure protein synthesis within the mitochondria, are encoded by nuclear genes and imported into the organelle after translation in the cytosol. The extensive use of next generation sequencing (NGS) has resulted in an increasing number of variants in mtARS genes being identified and associated with mitochondrial diseases. The similarities between yeast and human mitochondrial translation machineries make yeast a good model to quickly and efficiently evaluate the effect of variants in mtARS genes. Genetic screening of patients with a clinical suspicion of mitochondrial disorders through a customized gene panel of known disease-genes, including all genes encoding mtARSs, led to the identification of missense variants in WARS2, NARS2 and RARS2. Most of them were classified as Variant of Uncertain Significance. We exploited yeast models to assess the functional consequences of the variants found in these genes encoding mitochondrial tryptophanyl-tRNA, asparaginyl-tRNA, and arginyl-tRNA synthetases, respectively. Mitochondrial phenotypes such as oxidative growth, oxygen consumption rate, Cox2 steady-state level and mitochondrial protein synthesis were analyzed in yeast strains deleted in MSW1, SLM5, and MSR1 (the yeast orthologues of WARS2, NARS2 and RARS2, respectively), and expressing the wild type or the mutant alleles. Pathogenicity was confirmed for most variants, leading to their reclassification as Likely Pathogenic. Moreover, the beneficial effects observed after asparagine and arginine supplementation in the growth medium suggest them as a potential therapeutic approach.

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