Department of Life Sciences and Biotechnology and LTTA Center, University of Ferrara, Ferrara.
Transfusion Service, Haemophilia Centre and Haematology, Castelfranco Veneto Hospital, Castelfranco Veneto.
Haematologica. 2023 Feb 1;108(2):472-482. doi: 10.3324/haematol.2022.281279.
In hemophilia A, F8 nonsense variants, and particularly those affecting the large factor VIII (FVIII) B domain that is dispensable for coagulant activity, display lower association with replacement therapy-related anti-FVIII inhibitory antibodies as retrieved from multiple international databases. Since null genetic conditions favor inhibitor development, we hypothesized that translational readthrough over premature termination codons (PTC) may contribute to immune tolerance by producing full-length proteins through the insertion of amino acid subset(s). To quantitatively evaluate the readthrough output in vitro, we developed a very sensitive luciferase-based system to detect very low full-length FVIII synthesis from a wide panel (n=45; ~60% patients with PTC) of F8 nonsense variants. PTC not associated with inhibitors displayed higher readthrough-driven expression levels than inhibitor-associated PTC, a novel observation. Particularly, higher levels were detected for B-domain variants (n=20) than for variants in other domains (n=25). Studies on plasma from six hemophilia A patients with PTC, integrated by expression of the corresponding nonsense and readthrough-deriving missense variants, consistently revealed higher FVIII levels for B-domain variants. Only one B-domain PTC (Arg814*) was found among the highly represented PTC not sporadically associated with inhibitors, but with the lowest proportion of inhibitor cases (4 out of 57). These original insights into the molecular genetics of hemophilia A, and particularly into genotype-phenotype relationships related with disease treatment, demonstrate that B-domain features favor PTC readthrough output. This provides a potential molecular mechanism contributing to differential PTC-associated inhibitor occurrence, with translational implications for a novel, experimentally based classification of F8 nonsense variants.
在血友病 A 中,F8 无义变异体,特别是那些影响对凝血活性非必需的大因子 VIII(FVIII)B 结构域的变异体,与从多个国际数据库中检索到的与替代治疗相关的抗 FVIII 抑制性抗体的关联较低。由于缺失的遗传条件有利于抑制剂的发展,我们假设翻译通读越过终止密码子(PTC)可能通过插入氨基酸子集来产生全长蛋白,从而有助于免疫耐受。为了在体外定量评估通读产物,我们开发了一种非常灵敏的基于荧光素酶的系统,以从广泛的 F8 无义变异体面板(n=45;约 60%的 PTC 患者)中检测非常低的全长 FVIII 合成。与抑制剂无关的 PTC 显示出比与抑制剂相关的 PTC 更高的通读驱动表达水平,这是一个新的观察结果。特别是,在 B 结构域变异体(n=20)中检测到更高的水平,而在其他结构域(n=25)的变异体中检测到更高的水平。对来自六个具有 PTC 的血友病 A 患者的血浆进行的研究,通过表达相应的无义和通读衍生的错义变异体进行整合,一致显示出 B 结构域变异体的 FVIII 水平更高。在与抑制剂不随机相关但与抑制剂病例比例最低(57 例中的 4 例)的高度代表性 PTC 中,仅发现一个 B 结构域 PTC(Arg814*)。这些对血友病 A 的分子遗传学的原始见解,特别是与疾病治疗相关的基因型-表型关系的见解,表明 B 结构域特征有利于 PTC 通读产物。这为 PTC 相关抑制剂发生的差异提供了潜在的分子机制,对基于实验的 F8 无义变异体的新型分类具有翻译意义。
