Pekeles Heather, Berrahmoune Saoussen, Dassi Christelle, Cheung Anthony C T, Gagnon Tommy, Waters Paula J, Eberhard Ralf, Buhas Daniela, Myers Kenneth A
Division of Neurology, Department of Pediatrics, Montreal Children's Hospital, McGill University Health Centre, 1001 Décarie Boulevard, Montreal, Quebec, H4A 3J1, Canada.
Research Institute of the McGill University Health Centre, 2155 Guy Street, Suite 500, Montreal, Quebec, H3H 2R9, Canada.
EClinicalMedicine. 2024 Jul 18;74:102740. doi: 10.1016/j.eclinm.2024.102740. eCollection 2024 Aug.
DNA polymerase gamma (POLG)-related disorders are a group of rare neurodegenerative mitochondrial diseases caused by pathogenic variants in , the gene encoding POLG. Patients may experience a range of signs and symptoms, including seizures, vision loss, myopathy, neuropathy, developmental impairment or regression, and liver failure. The diseases follow a progressive, degenerative course, with most affected individuals dying within 3 months-12 years of diagnosis. At present, there are no effective treatments for POLG-related disorders.
In this study we report the interim 6-month data from a long term open-label, single arm phase 2 trial, in which we assessed the safety and efficacy of combination therapy with deoxycytidine and deoxythymidine (dC/dT) in children with POLG-related disorders. dC/dT was given enterally in powder form, dissolved in water. The primary outcome measures included Newcastle Mitochondrial Disease Scale (NMDS) score, serum growth differentiation factor 15 (GDF-15; a biomarker of mitochondrial dysfunction), electroencephalography (EEG), seizure diary, and blood and urine tests to assess end organ and mitochondrial function. Secondary outcome measures included recording of all adverse events to evaluate the safety of the intervention. The trial is registered with ClinicalTrials.gov, NCT04802707 (https://clinicaltrials.gov/ct2/show/NCT04802707). Data were collected from 14 October, 2021 to 13 December, 2023.
We present 6-month interim data from the first ten people with POLG-related disorders enrolled in the trial, six with Alpers-Huttenlocher syndrome, two with ataxia-neuropathy spectrum, and two who do not fit into a classical POLG-related phenotype. During the 6 months of treatment, NMDS score improved from a mean of 27.3 at baseline to 20.7 at 6 months (estimated difference 6.0; 95% CI 2.5-∞). GDF-15 values remained stable or decreased in all patients; the mean decreased from 1031 pg/ml to 729 pg/ml (estimated difference 200; 95% CI 12-∞). 8/10 patients had abnormal baseline EEG; improvement in EEG was seen in 5 of these 8. There were no significant changes in other blood and urine testing. Regarding adverse events, two patients experienced diarrhea that spontaneously resolved.
dC/dT is a promising treatment option for people with POLG-related disorders. Further research is needed to assess the long-term safety and efficacy in POLG-related disorders, as well as safety and efficacy in other mitochondrial DNA depletion disorders.
This study was primarily funded by the Liam Foundation, with additional funding from the Savoy Foundation, Grand Défi Pierre Lavoie Foundation, and Fonds de Recherche du Québec - Santé.
DNA聚合酶γ(POLG)相关疾病是由编码POLG的基因中的致病变异引起的一组罕见的神经退行性线粒体疾病。患者可能会出现一系列体征和症状,包括癫痫发作、视力丧失、肌病、神经病变、发育障碍或倒退以及肝功能衰竭。这些疾病呈进行性、退行性病程,大多数受影响个体在诊断后的3个月至12年内死亡。目前,对于POLG相关疾病尚无有效的治疗方法。
在本研究中,我们报告了一项长期开放标签、单臂2期试验的6个月中期数据,在该试验中,我们评估了脱氧胞苷和脱氧胸苷(dC/dT)联合治疗对POLG相关疾病儿童的安全性和有效性。dC/dT以粉末形式经肠道给药,溶于水中。主要结局指标包括纽卡斯尔线粒体疾病量表(NMDS)评分、血清生长分化因子15(GDF-15;线粒体功能障碍的生物标志物)、脑电图(EEG)、癫痫日记以及评估终末器官和线粒体功能的血液和尿液检查。次要结局指标包括记录所有不良事件以评估干预措施的安全性。该试验已在ClinicalTrials.gov注册,注册号为NCT04802707(https://clinicaltrials.gov/ct2/show/NCT04802707)。数据收集时间为2021年10月14日至2023年12月13日。
我们展示了该试验中首批入组的10例POLG相关疾病患者的6个月中期数据,其中6例患有阿尔珀斯-许滕洛赫尔综合征,2例患有共济失调-神经病变谱系,2例不符合经典的POLG相关表型。在6个月的治疗期间,NMDS评分从基线时的平均27.3分提高到6个月时的20.7分(估计差异为6.0;95%置信区间为2.5至无穷大)。所有患者的GDF-15值保持稳定或下降;平均值从1031 pg/ml降至729 pg/ml(估计差异为200;95%置信区间为12至无穷大)。10例患者中有8例基线脑电图异常;这8例中的5例脑电图有所改善。其他血液和尿液检查无显著变化。关于不良事件,2例患者出现腹泻,随后自行缓解。
dC/dT对于POLG相关疾病患者是一种有前景的治疗选择。需要进一步研究来评估其在POLG相关疾病中的长期安全性和有效性,以及在其他线粒体DNA耗竭性疾病中的安全性和有效性。
本研究主要由利亚姆基金会资助,此外还获得了萨沃伊基金会、皮埃尔·拉沃伊大挑战基金会和魁北克卫生研究基金会的额外资助。
