A phase Ib/IIa study of Enoxacin in patients with ALS

Iddo Magen, Hannah Marlene Kaneb, Maria Masnata, Nisha Pulimood, Anna Emde, Angela Genge, Eran Hornstein
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Abstract

The RNAse III DICER is essential for miRNA biogenesis. DICER activity is downregulated in sporadic and genetic forms of ALS. Accordingly, hundreds of miRNAs are broadly downregulated, and their mRNA targets are de-repressed. Enoxacin is a fluoroquinolone, which increases DICER activity and miRNA biogenesis. In an investigator-initiated, first-in-patient phase Ib/IIa study we tested Enoxacin safety and tolerability in patients with ALS and explored pharmacodynamic biomarkers for Enoxacin target engagement. Six patients with sporadic ALS were dosed with oral Enoxacin twice daily for 30 days. Patients did not experience any serious adverse events and completed the dosing period. Molecular analysis of cell-free miRNA in plasma and CSF revealed a global increase in plasma and CSF miRNA levels in all post-treatment time points, compared to baseline. Therefore, our study demonstrates that Enoxacin is tolerable and provides important evidence for in-patient target engagement. These results encourage testing Enoxacin efficacy in larger trials.
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肌萎缩侧索硬化症患者的依诺沙星 Ib/IIa 期研究
RNAse III DICER 对 miRNA 的生物发生至关重要。在渐冻症的散发性和遗传性形式中,DICER 活性下调。因此,数百种 miRNA 被广泛下调,其 mRNA 靶标被抑制。依诺沙星是一种氟喹诺酮类药物,可提高 DICER 的活性和 miRNA 的生物生成。在一项由研究者发起的首例患者 Ib/IIa 期研究中,我们测试了依诺沙星在 ALS 患者中的安全性和耐受性,并探索了依诺沙星靶点参与的药效学生物标志物。六名散发性肌萎缩性脊髓侧索硬化症患者每天口服两次依诺沙星,持续30天。患者未出现任何严重不良反应,并完成了服药期。对血浆和脑脊液中游离的细胞 miRNA 进行的分子分析表明,与基线相比,治疗后所有时间点的血浆和脑脊液 miRNA 水平均有全面提高。因此,我们的研究表明依诺沙星是可耐受的,并为住院患者的目标参与提供了重要证据。这些结果鼓励在更大规模的试验中测试依诺沙星的疗效。
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