Brogidirsen的I/II期试验:双靶向反义寡核苷酸用于杜氏肌营养不良症的第 44 号外显子跳接治疗

Hirofumi Komaki, Eri Takeshita, Katsuhiko Kunitake, Takami Ishizuka, Yuko Shimizu-Motohashi, Akihiko Ishiyama, Masayuki Sasaki, Chihiro Yonee, Shinsuke Maruyama, Eisuke Hida, Yoshitsugu Aoki
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引用次数: 0

摘要

杜氏肌营养不良症(DMD)是一种严重的肌肉疾病,由 DMD 基因突变引起,导致肌营养不良蛋白缺失。使用反义寡核苷酸(ASO)进行外显子跳接是一种很有前景的方法,它可以通过纠正前 mRNA 剪接过程中的帧移位来部分恢复肌营养不良蛋白。然而,目前这种方法的一个弱点是它具有突变特异性,而且疗效不佳。为了解决这些问题,我们旨在开发一种新型双靶向 ASO--brogidirsen,它利用磷酸二酰胺吗啉寡聚体靶向 DMD 第 44 号外显子中的两个序列。在此,我们进行了一项开放标签、剂量递增的 I/II 期试验,以评估 Brogidirsen 的安全性、药代动力学和活性,并对六名适合跳过 44 号外显子的 DMD 患者进行静脉给药。研究包括剂量递增部分,以确定最佳剂量,然后延长治疗时间,每周剂量为 40 毫克/千克或 80 毫克/千克,持续 24 周。没有出现与博吉德森有关的严重不良事件。研究结果表明,肌营养不良蛋白水平呈剂量依赖性增长,在两组患者中分别达到正常水平的10.27%和15.79%。运动功能测试表明,运动功能有保持或略有改善的趋势。Cmax和AUC0-t的增加呈剂量依赖性。高通量蛋白质组检测显示,PADI2、TTN、MYOM2 和 MYLPF 等血清蛋白减少,表明它们是治疗效果的生物标志物。值得注意的是,使用来自 DMD 患者的尿源细胞进行的体外试验证明,在首次人体试验中,溴吉森具有很高的疗效。这些令人鼓舞的结果证明了随后针对 DMD 的多国试验是有必要的。
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Phase I/II Trial of Brogidirsen: Dual-Targeting Antisense Oligonucleotides for Exon 44 Skipping in Duchenne Muscular Dystrophy
Duchenne muscular dystrophy (DMD) is a severe muscle disorder caused by mutations in the DMD gene, resulting in dystrophin loss. Exon-skipping using antisense oligonucleotides (ASO) is a promising approach that partially restores dystrophin by correcting the frameshift during pre-mRNA splicing. However, a weakness of the current approach is that it is mutation-specific and has poor efficacy. To address these, we aim to develop brogidirsen, a new dual-targeting ASO that targets two sequences in exon 44 of the DMD using phosphorodiamidate morpholino oligomer. Here, we conducted an open-label, dose-escalation, Phase I/II trial to evaluate the safety, pharmacokinetics, and activity of brogidirsen, administered intravenously to six ambulant patients with DMD amenable to exon 44 skipping. The study consisted of a dose-escalation part to determine the optimal doses, followed by extended treatment with 40 mg/kg or 80 mg/kg weekly dose for 24 weeks. There were no serious adverse events related to brogidirsen. The results indicated a dose-dependent increase in dystrophin levels, reaching 10.27% and 15.79% of the normal level in the two cohorts. Motor functional tests suggested a trend toward maintaining or slightly improving motor function. There was a dose-dependent increase in Cmax and AUC0–t. High-throughput proteomic assays revealed that serum proteins such as PADI2, TTN, MYOM2, and MYLPF were observed to reduce, suggesting them as biomarkers for therapeutic effects. Notably, in vitro assays using urine-derived cells from patients with DMD support brogidirsen’s high efficacy in the first-in-human studies. These promising results warrant a subsequent multinational trial for DMD.
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