Department of Thoracic Medicine and Surgery, Lewis Katz School of Medicine, Temple University, Philadelphia, PA, USA.
Molecular Therapeutics Program, Institute for Cancer Research, Fox Chase Cancer Center, Philadelphia, Pennsylvania, USA.
BMC Med Genet. 2019 Jul 15;20(1):125. doi: 10.1186/s12881-019-0852-5.
Alpha 1 Antitrypsin (AAT) is a key serum proteinase inhibitor encoded by SERPINA1. Sequence variants of the gene can cause Alpha 1 Antitrypsin Deficiency (AATD), a condition associated with lung and liver disease. The majority of AATD cases are caused by the 'Z' and 'S' variants - single-nucleotide variations (SNVs) that result in amino acid substitutions of E342K and E264V. However, SERPINA1 is highly polymorphic, with numerous potentially clinically relevant variants reported. Novel variants continue to be discovered, and without reports of pathogenicity, it can be difficult for clinicians to determine the best course of treatment.
We assessed the utility of next-generation sequencing (NGS) and predictive computational analysis to guide the diagnosis of patients suspected of having AATD. Blood samples on serum separator cards were submitted to the DNA Advanced Screening Program (Biocerna LLC, Fulton, Maryland, USA) by physicians whose patients were suspected of having AATD. Laboratory analyses included quantification of serum AAT levels, qualitative analysis by isoelectric focusing, and targeted genotyping and NGS of the SERPINA1 gene. Molecular modeling software UCSF Chimera (University College of San Francisco, CA) was used to visualize the positions of amino acid changes as a result of rare/novel SNVs. Predictive software was used to assess the potential pathogenicity of these variants; methods included a support vector machine (SVM) program, PolyPhen-2 (Harvard University, Cambridge, MA), and FoldX (Centre for Genomic Regulation, Barcelona, Spain).
Samples from 23 patients were analyzed; 21 rare/novel sequence variants were identified by NGS, including splice variants (n = 2), base pair deletions (n = 1), stop codon insertions (n = 2), and SNVs (n = 16). Computational modeling of protein structures caused by the novel SNVs showed that 8 were probably deleterious, and two were possibly deleterious. For the majority of probably/possibly deleterious SNVs (I50N, P289S, M385T, M221T, D341V, V210E, P369H, V333M and A142D), the mechanism is probably via disruption of the packed hydrophobic core of AAT. Several deleterious variants occurred in combination with more common deficiency alleles, resulting in very low AAT levels.
NGS and computational modeling are useful tools that can facilitate earlier, more precise diagnosis, and consideration for AAT therapy in AATD.
α1 抗胰蛋白酶(AAT)是一种由 SERPINA1 编码的关键血清蛋白酶抑制剂。该基因的序列变异可导致 α1 抗胰蛋白酶缺乏症(AATD),这是一种与肺部和肝脏疾病相关的疾病。大多数 AATD 病例是由“Z”和“S”变异引起的-单核苷酸变异(SNV),导致 E342K 和 E264V 的氨基酸取代。然而,SERPINA1 高度多态性,有许多潜在的临床相关变异报道。新的变异仍在不断发现,如果没有致病性的报告,临床医生很难确定最佳的治疗方案。
我们评估了下一代测序(NGS)和预测性计算分析在指导疑似 AATD 患者诊断中的应用。疑似 AATD 患者的医生将血清分离卡上的血液样本提交给 DNA 高级筛查计划(Biocerna LLC,马里兰州富尔顿)。实验室分析包括血清 AAT 水平的定量、等电聚焦的定性分析,以及 SERPINA1 基因的靶向基因分型和 NGS。使用 UCSF Chimera(旧金山加利福尼亚大学)分子建模软件可视化由于罕见/新 SNV 导致的氨基酸变化的位置。使用预测软件评估这些变异的潜在致病性;方法包括支持向量机(SVM)程序、PolyPhen-2(哈佛大学,马萨诸塞州剑桥)和 FoldX(巴塞罗那基因组调控中心,西班牙)。
分析了 23 名患者的样本;通过 NGS 鉴定了 21 种罕见/新的序列变异,包括剪接变异(n=2)、碱基对缺失(n=1)、终止密码子插入(n=2)和 SNV(n=16)。新型 SNV 引起的蛋白质结构的计算建模表明,8 个可能是有害的,2 个可能是有害的。对于大多数可能/可能有害的 SNV(I50N、P289S、M385T、M221T、D341V、V210E、P369H、V333M 和 A142D),其机制可能是通过破坏 AAT 的包装疏水核心。一些有害的变异与更常见的缺陷等位基因结合,导致 AAT 水平非常低。
NGS 和计算建模是有用的工具,可以促进更早、更准确的诊断,并考虑 AATD 中的 AAT 治疗。
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