Department of Pediatrics, New York University School of Medicine, New York, New York 10016, USA.
Pediatr Res. 2011 Nov;70(5):480-3. doi: 10.1203/PDR.0b013e31822e1825.
Familial dysautonomia (FD) is caused by an intronic splice mutation in the IKBKAP gene that leads to partial skipping of exon 20 and tissue-specific reduction in I-κ-B kinase complex-associated protein/elongation protein 1 (IKAP/ELP-1) expression. Kinetin (6-furfurylaminopurine) has been shown to improve splicing and increase WT IKBKAP mRNA and IKAP protein expression in FD cell lines and carriers. To determine whether oral kinetin treatment could alter mRNA splicing in FD subjects and was tolerable, we administered kinetin to eight FD individuals homozygous for the splice mutation. Subjects received 23.5 mg/Kg/d for 28 d. An increase in WT IKBKAP mRNA expression in leukocytes was noted after 8 d in six of eight individuals; after 28 d, the mean increase compared with baseline was significant (p = 0.002). We have demonstrated that kinetin is tolerable in this medically fragile population. Not only did kinetin produce the desired effect on splicing in FD patients but also that effect seems to improve with time despite lack of dose change. This is the first report of a drug that produces in vivo mRNA splicing changes in individuals with FD and supports future long-term trials to determine whether kinetin will prove therapeutic in FD patients.
家族性自主神经异常症(FD)是由 IKBKAP 基因内含子剪接突变引起的,导致外显子 20 的部分跳跃和组织特异性 IκB 激酶复合物相关蛋白/延伸蛋白 1(IKAP/ELP-1)表达减少。已表明激动素(6-糠基氨基嘌呤)可改善剪接,并增加 FD 细胞系和携带者中的 WT IKBKAP mRNA 和 IKAP 蛋白表达。为了确定口服激动素治疗是否能改变 FD 患者的 mRNA 剪接并具有耐受性,我们对 8 名纯合剪接突变的 FD 个体进行了激动素治疗。受试者接受 23.5mg/Kg/d 的治疗,持续 28 天。在 8 名个体中有 6 名在 8 天后观察到白细胞中 WT IKBKAP mRNA 表达增加;28 天后,与基线相比,平均增加具有显著意义(p=0.002)。我们已经证明,激动素在这个医疗脆弱的人群中是耐受的。激动素不仅在 FD 患者中产生了所需的剪接效果,而且这种效果似乎随着时间的推移而改善,尽管没有改变剂量。这是第一个报告在 FD 个体中产生体内 mRNA 剪接变化的药物的报告,并支持未来的长期试验,以确定激动素是否对 FD 患者具有治疗作用。
