Department of Human Neurosciences, Rare Neuromuscular Diseases Centre, Sapienza University, Viale Dell'Università 30, 00185, Rome, Italy.
R & I Genetics, C.So Stati Uniti 4int.F, 35127, Padua, Italy.
J Neurol. 2024 Apr;271(4):1921-1936. doi: 10.1007/s00415-023-12142-x. Epub 2023 Dec 19.
Amyotrophic Lateral Sclerosis (ALS) is a neurodegenerative disease with an elusive etiology. While environmental factors have been considered, familial ALS cases have raised the possibility of genetic involvement. This genetic connection is increasingly evident, even in patients with sporadic ALS. We allowed access to the genetic test to all patients attending our clinic to identify the prevalence and the role of genetic variants in the development of the disease and to identify patients with potentially treatable forms of the disease.
194 patients with probable or definite ALS, were enrolled. A comprehensive genetic testing was performed, including sequencing all exons of the SOD1 gene and testing for hexanucleotide intronic repeat expansions (G4C2) in the C9orf72 gene using fluorescent repeat-primed PCR (RP-PCR). Whole Exome NGS Sequencing (WES) was performed, followed by an in silico multigene panel targeting neuromuscular diseases, spastic paraplegia, and motor distal neuropathies. We conducted statistical analyses to compare different patient groups.
Clinically significant pathogenetic variants were detected in 14.43% of cases. The highest prevalence of pathogenetic variants was observed in fALS patients, but a substantial proportion of sALS patients also displayed at least one variant, either pathogenetic or of uncertain significance (VUS). The most observed pathogenetic variant was the expansion of the C9orf72 gene, which was associated with a shorter survival. SOD1 variants were found in 1.6% of fALS and 2.5% of sALS patients.
The study reveals a significant number of ALS patients carrying pathogenic or likely pathogenic variants, with a higher prevalence in familial ALS cases. The expansion of the C9orf72 gene emerges as the most common genetic cause of ALS, affecting familial and sporadic cases. Additionally, SOD1 variants are detected at an unexpectedly higher rate, even in patients without a familial history of ALS, underscoring the crucial role of genetic testing in treatment decisions and potential participation in clinical trials. We also investigated variants in genes such as TARDBP, FUS, NEK1, TBK1, and DNAJC7, shedding light on their potential involvement in ALS. These findings underscore the complexity of interpreting variants of uncertain significance (VUS) and their ethical implications in patient communication and genetic counseling for patients' relatives.
This study emphasizes the diverse genetic basis of ALS and advocates for integrating comprehensive genetic testing into diagnostic protocols. The evolving landscape of genetic therapies requires identifying all eligible patients transcending traditional familial boundaries. The presence of VUS highlights the multifaceted nature of ALS genetics, prompting further exploration of complex interactions among genetic variants, environmental factors, and disease development.
肌萎缩侧索硬化症(ALS)是一种病因不明的神经退行性疾病。虽然已经考虑了环境因素,但家族性 ALS 病例提出了遗传参与的可能性。这种遗传联系越来越明显,即使是在散发性 ALS 患者中也是如此。我们允许我们诊所的所有患者进行基因检测,以确定遗传变异在疾病发展中的普遍性和作用,并确定具有潜在可治疗形式的疾病的患者。
共纳入 194 例疑似或明确的 ALS 患者。我们进行了全面的基因检测,包括对 SOD1 基因的所有外显子进行测序,并使用荧光重复引物 PCR(RP-PCR)检测 C9orf72 基因中的六核苷酸内含子重复扩增(G4C2)。进行全外显子组 NGS 测序(WES),然后进行针对神经肌肉疾病、痉挛性截瘫和运动远端神经病的多基因面板的计算机分析。我们进行了统计分析以比较不同的患者组。
在 14.43%的病例中检测到具有临床意义的致病性变异。致病性变异的最高患病率见于 fALS 患者,但相当一部分 sALS 患者也显示出至少一种变异,无论是致病性的还是意义不明的(VUS)。最常见的致病性变异是 C9orf72 基因的扩增,这与生存时间较短有关。在 1.6%的 fALS 和 2.5%的 sALS 患者中发现了 SOD1 变异。
该研究揭示了相当数量的 ALS 患者携带致病性或可能致病性的变异,家族性 ALS 病例中的患病率更高。C9orf72 基因的扩增成为 ALS 最常见的遗传原因,影响家族性和散发性病例。此外,即使在没有 ALS 家族史的患者中,SOD1 变异的检出率也出人意料地高,这突显了基因检测在治疗决策和潜在参与临床试验中的关键作用。我们还研究了 TARDBP、FUS、NEK1、TBK1 和 DNAJC7 等基因中的变异,揭示了它们在 ALS 中的潜在作用。这些发现强调了不确定意义的变异(VUS)的复杂性及其在患者沟通和遗传咨询中对患者亲属的伦理影响。
本研究强调了 ALS 的多种遗传基础,并主张将全面的基因检测纳入诊断方案。不断发展的基因治疗领域需要确定所有符合条件的患者,超越传统的家族界限。VUS 的存在突出了 ALS 遗传学的多面性,促使进一步探索遗传变异、环境因素和疾病发展之间的复杂相互作用。
